TRIMERIC ACTIVATABLE CYTOKINE CONSTRUCTS AND RELATED COMPOSITIONS AND METHODS

REFERENCE TO AN ELECTRONIC SEQUENCE LISTING

The contents of the electronic sequence listing (CYTX088.xml; Size: 741,530 bytes; and Date of Creation: Oct. 3, 2022) is herein incorporated by reference in its entirety.

TECHNICAL FIELD

The present disclosure relates to the field of biotechnology, and more specifically, to activatable cytokine constructs.

BACKGROUND

Cytokines are a family of naturally-occurring small proteins and glycoproteins produced and secreted by most nucleated cells in response to viral infection and/or other antigenic stimuli. LIGHT (lymphotoxin-like inducible protein that competes with glycoprotein D for herpes virus entry on T cells) is a cytokine in the tumor necrosis factor (TNF) ligand superfamily that is expressed on activated T cells, monocytes, granulocytes and immature dendritic cells. LIGHT is also known as tumor necrosis factor superfamily member 14 (TNFSF14). LIGHT is a homotrimer and binds as a trimer to two known cellular receptors: the herpesvirus entry mediator (HVEM) and lymphotoxin-beta receptor (LTbetaR). Through the activation of the HVEM pathway and LT-beta-Receptor, LIGHT can activate T cells and stimulate the production of chemokines, to ultimately recruit T cells. It has been shown to trigger apoptosis of various tumor cells. (Rooney, I A, et. Al., J. Biol. Chem. 275(19):14307-15 (2000)). If expressed in the tumor micro-environment, LIGHT can recruit and activate T-cells in the tumor micro-environment. LIGHT thus has been considered as a therapeutic agent for cancer. However, constitutive LIGHT activity in the peripherial system can lead to lymphocyte activation, inflammation, and tissue destruction. Significant side effects and off-target toxicity have hampered the development of LIGHT as a therapeutic agent.

The need and desire for improved specificity and selectivity of cytokine therapy to the desired target is of great interest. Increased targeting of cytokine therapeutics to the disease site could reduce systemic mechanism-based toxicities and lead to broader therapeutic utility.

SUMMARY

The present disclosure provides trimeric activatable cytokine constructs and methods of using and making thereof. In one aspect, the present disclosure provides an activatable cytokine construct (ACC) comprising: a first monomer construct comprising a first cytokine protein (CP1), a first cleavable moiety (CM1), and a first steric masking moiety (SMM1), wherein the CM1 is positioned between the CP1 and the SMM1; a second monomer construct comprising a second cytokine protein (CP2), a second cleavable moiety (CM2), and a second steric masking moiety (SMM2), wherein the CM2 is positioned between the CP2 and the SMM2; and a third monomer construct comprising a third cytokine protein (CP3), a third cleavable moiety (CM3), and a third steric masking moiety (SMM3), wherein the CM3 is positioned between the CP3 and the SMM3, wherein: the CP1, the CP2, and the CP3 bind to one another thereby forming a trimer of the first, the second, and the third monomer constructs; and the SMM1, the SMM2, and the SMM3 are globular molecules.

In some embodiments, the CP1, the CP2, and the CP3 are the same cytokine. In some embodiments, the cytokine is a member of tumor necrosis factor or tumor necrosis factor super family. In some embodiments, the CP1, the CP2 and the CP3 are tumor necrosis factor superfamily member 14 (TNFSF14 also known as LIGHT). In some embodiments, each of the CP1, the CP2, and the CP3 comprises a sequence that is at least 80%, 90%, 95%, or 99% identical to SEQ ID NO: 54.

In some embodiments, the SMM1, the SMM2, and the SMM3 are the same globular molecule. In some embodiments, the globular molecule is an albumin. In some embodiments, the albumin is a human serum albumin. In some embodiments, the albumin comprises a sequence that is at least 80%, 90%, 95%, or 99% identical to a human serum albumin.

In some embodiments, the first monomer construct comprises at least one linker. In some embodiments, the at least one linker comprises a linker L1 disposed between the CP1 and the CM1, and/or a linker L2 between the CM1 and the SMM1. In some embodiments, the second monomer construct comprises at least one linker. In some embodiments, the at least one linker comprises a linker L3 disposed between the CP2 and the CM2, and/or a linker L4 between the CM2 and the SMM2. In some embodiments, the third monomer construct comprises at least one linker. In some embodiments, the at least one linker comprises a linker L5 disposed between the CP3 and the CM3, and/or a linker L6 between the CM3 and the SMM3.

In some embodiments, the first monomer construct further comprises a first affinity masking moiety (AMM1) and optionally a fourth cleavable moiety (CM4) positioned between the AMM1 and the CP1, the second monomer construct further comprises a second affinity masking moiety (AMM2) and optionally a fifth cleavable moiety (CM5) positioned between the AMM2 and the CP2, and the third monomer construct further comprises a third affinity masking moiety (AMM3) and optionally a sixth cleavable moiety (CM6) positioned between the AMM3 and the CP3. In some embodiments, the AMM1, the AMM2, and the AMM3 are the same. In some embodiments, each of the AMM1, the AMM2, and the AMM3 comprises a sequence of SEQ ID NO: 61. In some embodiments, each of the AMM1, the AMM2, and the AMM3 comprises a sequence that at least 80%, 90%, 95%, or 99% identical to SEQ ID NO: 61. In some embodiments, the CM1, the CM2, and the CM3 comprise a substrate of the same protease. In some embodiments, the CM1, the CM2, and the CM3 comprise substrates of different proteases. In some embodiments, each of the CM1, the CM2, and the CM3 comprises a sequence that is at least 95% identical to SEQ ID NO: 62 or 63. In some embodiments, the CM4, the CM5, and the CM6 comprise a substrate of the same protease. In some embodiments, the CM4, the CM5, and the CM6 comprise substrates of different proteases. In some embodiments, each of the CM4, the CM5, and the CM6 comprises a sequence that is at least 95% identical to SEQ ID NO: 62 or 63.

In some embodiments, the protease(s) is/are produced by a tumor in a subject. In some embodiments, the protease(s) is/are selected from the group consisting of: ADAM8, ADAM9, ADAM10, ADAM12, ADAM15, ADAM17/TACE, ADAMDEC1, ADAMTS1, ADAMTS4, ADAMTS5, BACE, Renin, Cathepsin D, Cathepsin E, Caspase 1, Caspase 2, Caspase 3, Caspase 4, Caspase 5, Caspase 6, Caspase 7, Caspase 8, Caspase 9, Caspase 10, Caspase 14, Cathepsin B, Cathepsin C, Cathepsin K, Cathespin L, Cathepsin S, Cathepsin V/L2, Cathepsin X/Z/P, Cruzipain, Legumain, Otubain-2, KLK4, KLK5, KLK6, KLK7, KLK8, KLK10, KLK11, KLK13, KLK14, Meprin, Neprilysin, PSMA, BMP-1, MMP-1, MMP-2, MMP-3, MMP-7, MMP-9, MMP-10, MMP-11, MMP-12, MMP-13, MMP-14, MMP-15, MMP-16, MMP-17, MMP-19, MMP-20, MMP-23, MMP-24, MMP-26, MMP-27, activated protein C, cathepsin A, cathepsin G, Chymase, FVIIa, FIXa, FXa, FXIa, FXIIa, Elastase, Granzyme B, Guanidinobenzoatase, HtrA1, human neutrophil lyase, lactoferrin, marapsin, NS3/4A, PACE4, Plasmin, PSA, tPA, thrombin, tryptase, uPA, DESC1, DPP-4, FAP, Hepsin, Matriptase-2, MT-SP1/Matripase, TMPRSS2, TMPRSS3, and TMPRSS4.

In some embodiments, the first monomer construct further comprises a linker L7 between the AMM1 and the CM4 and/or a linker L8 between the CM4 and the CP1. In some embodiments, the second monomer construct further comprises a linker L9 between the AMM2 and the CM5 and/or a linker L10 between the CM5 and the CP2. In some embodiments, the third monomer construct further comprises a linker L11 between the AMM3 and the CM6 and/or a linker L12 between the CM6 and the CP3. In some embodiments, each of the linkers L1-L12 has a total length of 2 to 30 amino acids. In some embodiments, each of the linkers L1-L12 independently comprises a sequence of any one of SEQ ID NO: 64-69, 75-77, GGS, SGG, GSG, GS, or G.

In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises the CP1, the CM1, and the SMM1, the second monomer construct comprises the CP2, the CM2, and the SMM2, and the third monomer construct comprises the CP3, the CM3, and the SMM3. In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises the SMM1, the CM1, and the CP1, the second monomer construct comprises the SMM2, the CM2, and the CP2, and the third monomer construct comprises the SMM3, the CM3, and the CP3. In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises the AMM1, the CM4, the CP1, the CM1, and the SMM1, the second monomer construct comprises the AMM2, the CM5, the CP2, the CM2, and the SMM2, and the third monomer construct comprises the AMM3, the CM6, the CP3, the CM3, and the SMM3. In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises the SMM1, the AMM1, the CM1, and the CP1; the second monomer construct comprises the SMM2, the AMM2, the CM2, and the CP2, and the third monomer construct comprises the SMM3, the AMM3, the CM3, and the CP3. In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises, the AMM1, the SMM1, the CM1, and the CP1; the second monomer construct comprises the AMM2, the SMM2, the CM2, and the CP2, and the third monomer construct comprises the AMM3, the SMM3, the CM3, and the CP3. In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises the SMM1, the CM1, the CP1, the CM4, and AMM1, the second monomer construct comprises the SMM2, the CM2, the CP2, the CM5, and AMM2, and the third monomer construct comprises the SMM3, the CM3, the CP3, the CM6, and the AMM3. In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises the CP1, the CM1, the AMM1, and the SMM1; the second monomer construct comprises the CP2, the CM2, the AMM2, and the SMM2; and the third monomer construct comprises the CP3, the CM3, the AMM3, and the SMM3. In some embodiments, in a N- to C-terminal direction: the first monomer construct comprises the CP1, the CM1, the SMM1, and the AMM1; the second monomer construct comprises the CP2, the CM2, the SMM2, and the AMM2; and the third monomer construct comprises the CP3, the CM3, the SMM3, and the AMM3.

In some embodiments, in an inactive state, the ACC is characterized by having a reduced level of an activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof as compared to a control level of the activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof. In some embodiments, the ACC is characterized by at least a 2-fold, 5-fold, 10-fold, 500-fold, 10³-fold, 10⁴-fold, 10⁵-fold, or 10⁶-fold reduction in the activity of the trimer of CP1, CP2, and CP3 as compared to the activity of a control trimer of CP1, CP2, and CP3 that does not comprise a steric masking moiety or an affinity masking moiety. In some embodiments, the activity is activation of herpes virus entry mediator (HVEM). In some embodiments, the activity is activation of lymphotoxin beta receptor. In some embodiments, the activity is activation of herpes virus entry mediator (HVEM) and activation of lymphotoxin beta receptor. In some embodiments, the control trimer of CP1, CP2, and CP3 results from activation of the ACC.

In some embodiments, the first monomer construct, the second monomer construct, and the third monomer construct are identical. In some embodiments, the ACC does not comprise any domain that facilitates formation of a trimer other than CP1, CP2, and CP3. In some embodiments, the ACC does not comprise any domain other than the CP1, the CP2, and the CP3 that covalently links the first, the second, and the third monomer constructs. In some embodiments, the ACC does not comprise a coil-coiled domain, an Fc domain, or a domain other than the CP1, the CP2, or the CP3 that is capable forming a disulfide bond. In some embodiments, the ACC does not comprise a tumor-directing molecule (e.g., the ACC does not comprise an Fab or scFv fragment that recognizes an antigen found on cancer cells). In some embodiments, the CP1, CP2, and CP3 are identical and each comprises the amino acid sequence of SEQ ID NO: 54. In some embodiments, the first monomer construct, the second monomer construct, and the third monomer construct are identical and each monomer comprises: the amino acid sequence of SEQ ID NO: 54; and an AMM comprising an amino acid sequence that is at least 95% identical to that of SEQ ID NO: 61; and an SMM comprising an albumin.

In another aspect, the present disclosure provides an activatable cytokine construct (ACC) comprising: a first monomer construct comprising a first cytokine protein (CP1), a first cleavable moiety (CM1), and a first affinity masking moiety (AMM1), wherein the CM1 is positioned between the CP1 and the AMM1; a second monomer construct comprising a second cytokine protein (CP2), a second cleavable moiety (CM2), and a second affinity masking moiety (AMM2), wherein the CM2 is positioned between the CP2 and the AMM2; and a third monomer construct comprising a third cytokine protein (CP3), a third cleavable moiety (CM3), and a third affinity steric masking moiety (AMM3), wherein the CM3 is positioned between the CP3 and the AMM3, wherein the CP1, the CP2, and the CP3 bind to one another thereby forming a trimer of the first, the second, and the third monomer constructs.

In another aspect, the present disclosure provides a composition comprising the ACC herein. In some embodiments, the composition is a pharmaceutical composition.

In another aspect, the present disclosure provides a container, vial, syringe, injector pen, or kit comprising at least one dose of the composition herein.

In another aspect, the present disclosure provides a nucleic acid encoding a polypeptide that comprises at least one of the first monomer construct, the second monomer construct, or the third monomer construct of the ACC herein. In some embodiments, the nucleic acid comprises a sequence of any one of SEQ ID NOs: 9, 11, 13, 25, 31, 41, 43, 45, or 47.

In another aspect, the present disclosure provides a set of nucleic acids that together encode polypeptides that comprise the first monomer construct, the second monomer construct, and the third monomer construct in the ACC herein.

In another aspect, the present disclosure provides a vector comprising the nucleic acid or a set of nucleic acids herein.

In another aspect, the present disclosure provides a cell comprising the nucleic acid or the vector herein. In some aspects, the cell is a mammalian cell.

In another aspect, the present disclosure provides a method of treating a subject in need thereof comprising administering to the subject a therapeutically effective amount of the ACC or the composition herein. In some embodiments, the subject has been identified or diagnosed as having a cancer. In some embodiments, the method further comprises administering an immune checkpoint inhibitor. In some embodiments, the immune checkpoint inhibitor is an anti-PD-1 antibody or anti-PD-L1 antibody.

In another aspect, the present disclosure provides a method of producing an ACC comprising: culturing a cell of claim 61 in a liquid culture medium under conditions sufficient to produce the ACC; and recovering the ACC from the cell or the liquid culture medium. In some embodiments, the method further comprises purifying the recovered ACC using affinity chromatography. In some embodiments, the method further comprises formulating the recovered ACC into a pharmaceutical composition.

BRIEF DESCRIPTION OF DRAWINGS

FIGS. 1A-1H show exemplary activatable cytokine constructs according to some embodiments of the present disclosure. FIGS. 1A-1B illustrate exemplary cytokine constructs that utilize human serum albumin (HSA) as a steric masking moiety. FIGS. 1C-1D illustrate exemplary cytokine constructs that utilize a peptide masking moiety. FIGS. 1E-1H illustrate exemplary cytokine constructs that utilize both a steric masking moiety and a peptide masking moiety. FIGS. 1E-1F illustrate exemplary cytokine constructs that have a steric masking moiety and an affinity masking moiety coupled to different sides of the cytokine component. FIGS. 1G-1H illustrate exemplary cytokine constructs that have a steric masking moiety and an affinity masking moiety coupled to the same side of the cytokine component.

FIGS. 2A-2B show that the addition of HSA steric masking moiety to LIGHT reduces LIGHT signaling activity in both the herpes virus entry mediator (HVEM) reporter assay and Lymphotoxin beta receptor cell-based assay (A375 IL-8 ELISA).

FIGS. 3A-3B show that the addition of cleavable peptide mask to LIGHTreduces LIGHT signaling activity in both the HVEM reporter assay and A375 IL-8 ELISA.

FIGS. 4A-4C show that the addition of a cleavable peptide mask to the N-terminus of LIGHT-HSA further reduces LIGHT signaling activity in both the HVEM reporter assay and A375 IL-8 ELISA.

FIGS. 5A-5B show in vitro activity of single and dual masked LIGHT activatable cytokine constructs in the HVEM reporter assay and A375 IL-8 ELISA.

FIGS. 6A and 6B show in vitro activity of additional ACCs.

FIGS. 7A-7D show in vitro activity of mouse-human cross-reactive LIGHT activatable cytokine constructs.

FIGS. 8A-8B show the activity of ProC1486, ProC1487 and ProC2076 determined by HVEM assays.

FIG. 9 shows tumor growth inhibition profiles of human LIGHT ACC ProC1491 engineered with a cleavable HSA domain at the C-terminal extremity of LIGHT and human LIGHT ProC1 189 engineered with a His tag at the C-terminal extremity of LIGHT.

FIGS. 10A-10B show antitumor activity of ProC1486 and ProC1487 in the MC38 syngeneic mouse model.

FIGS. 11A-11B show that at day 6 post treatment initiation in the MC38 syngeneic mice model, ProC1487, dosed as a single agent or in combination with an anti-PD-1 antibody, was able to increase the level of CD8+ T cells in the tumor micro-environment (FIG. 11A) as well as to promote the production of Th1 cytokines (IFNγ, TNFα) by CD8+ T cells (FIG. 11B).

DETAILED DESCRIPTION

Provided herein are trimeric activatable cytokine constructs (ACCs) that include trimers of three monomer constructs. Each of the monomer constructs includes a cytokine, which can bind to one another and form a trimer (e.g., homotrimer or heterotrimer). Upon activation, the active cytokine products remain in a trimeric form.

Each of the monomer constructs may further comprise one or more masking moieties, coupled with the cytokine via one or more cleavable moieties. In some embodiments, the masking moieties may be steric masking moieties that do not bind to the cytokine, but, in an inactive state, reduce, inhibit, or interfere with binding between the cytokine and its binding partner (e.g., a ligand or receptor) via steric hindrance. In some embodiments, the masking moieties may be affinity masking moieties that specifically bind to the cytokine and reduce, inhibit, or interfere with binding between the cytokine and its binding partner in an inactivate state. In some embodiments, each monomer construct of the trimeric ACC comprises a steric masking moiety. In some examples, each monomer construct may be dual masked and include both a steric masking moiety and an affinity masking moiety. In such monomer constructs, the steric masking moiety and the affinity masking moiety may be coupled to different sides of the cytokine, with each masking moiety coupled to the cytokine with its own cleavable moiety. Alternatively, the steric masking moiety and the affinity masking moiety may be on the same side of the cytokine in the monomer construct. In such cases, the masking moieties may be coupled with the cytokine via one cleavable moiety (e.g., positioned between the cytokine and the masking moiety closer to the cytokine).

In an active state (e.g., when the ACC is exposed to a protease that cleaves the cleavable moieties), the one or more masking moieties may be released from the cytokines, yielding a cytokine product with substantially restored activity. In the active state, the cytokines may be in a trimeric form. The ACC may be designed to selectively activate upon exposure to diseased tissue, and not in normal tissue. For example, the ACC may be designed with one or more cleavable moieties (CMs) that are cleaved by a protease. The protease(s) that cleave the one or more CMs may be over-expressed in diseased tissue (e.g., tumor tissue) relative to healthy tissue. The ACC may be activated upon cleavage of the CM(s) so that the cytokine may exert its activity in the diseased tissue (e.g., in a tumor microenvironment) while the cytokine activity is attenuated in the context of healthy tissue. Thus, the ACCs provided herein may provide reduced toxicity relative to traditional cytokine therapeutics, enable higher effective dosages of cytokine, and/or increase the therapeutic window for the cytokine. As such, these compounds have the potential for conferring the benefit of a cytokine-based therapy, with potentially less of the toxicity associated with certain cytokine-based therapies.

Also provided herein are related intermediates, compositions, kits, nucleic acids, vectors, and recombinant cells, as well as related methods, including methods of using and methods of producing any of the activatable cytokine constructs described herein. Provided herein are ACCs produced by any one of the methods described herein. Also provided herein are compositions comprising any one the ACCs described herein. Also provided herein are compositions of any one of the compositions described herein, wherein the composition is a pharmaceutical composition. Also provided herein are kits comprising at least one dose of any one of the compositions described herein.

Definitions

Unless otherwise defined, all technical and scientific terms used herein have the same meaning as commonly understood by one of ordinary skill in the art to which this invention belongs. Methods and materials are described herein for use in the present invention; other, suitable methods and materials known in the art can also be used. The materials, methods, and examples are illustrative only and not intended to be limiting. All publications, patent applications, patents, sequences, database entries, and other references mentioned herein are incorporated by reference in their entirety. In case of conflict, the present specification, including definitions, will control.

Other features and advantages of the invention will be apparent from the following detailed description and figures, and from the claims.

The term “a” and “an” refers to one or more (i.e., at least one) of the grammatical object of the article. By way of example, “a cell” encompasses one or more cells.

As used herein, the terms “about” and “approximately,” when used to modify an amount specified in a numeric value or range, indicate that the numeric value as well as reasonable deviations from the value known to the skilled person in the art. For example ±20%, ±10%, or ±5%, are within the intended meaning of the recited value where appropriate.

Concentrations, amounts, and other numerical data may be expressed or presented herein in a range format. It is to be understood that such a range format is used merely for convenience and brevity and thus should be interpreted flexibly to include not only the numerical values explicitly recited as the limits of the range, but also to include all the individual numerical values or sub-ranges encompassed within that range as if each numerical value and sub-range is explicitly recited. As an illustration, a numerical range of “about 0.01 to 2.0” should be interpreted to include not only the explicitly recited values of about 0.01 to about 2.0, but also include individual values and sub-ranges within the indicated range. Thus, included in this numerical range are individual values such as 0.5, 0.7, and 1.5, and sub-ranges such as from 0.5 to 1.7, 0.7 to 1.5, and from 1.0 to 1.5, etc. Furthermore, such an interpretation should apply regardless of the breadth of the range or the characteristics being described. Additionally, it is noted that all percentages are in weight, unless specified otherwise.

In understanding the scope of the present disclosure, the terms “including” or “comprising” and their derivatives, as used herein, are intended to be open ended terms that specify the presence of the stated features, elements, components, groups, integers, and/or steps, but do not exclude the presence of other unstated features, elements, components, groups, integers and/or steps. The foregoing also applies to words having similar meanings such as the terms “including”, “having” and their derivatives. The term “consisting” and its derivatives, as used herein, are intended to be closed terms that specify the presence of the stated features, elements, components, groups, integers, and/or steps, but exclude the presence of other unstated features, elements, components, groups, integers and/or steps. The term “consisting essentially of,” as used herein, is intended to specify the presence of the stated features, elements, components, groups, integers, and/or steps as well as those that do not materially affect the basic and novel characteristic(s) of features, elements, components, groups, integers, and/or steps. It is understood that reference to any one of these transition terms (i.e. “comprising,” “consisting,” or “consisting essentially”) provides direct support for replacement to any of the other transition term not specifically used. For example, amending a term from “comprising” to “consisting essentially of” or “consisting of” would find direct support due to this definition for any elements disclosed throughout this disclosure. Based on this definition, any element disclosed herein or incorporated by reference may be included in or excluded from the claimed invention.

As used herein, a plurality of compounds, elements, or steps may be presented in a common list for convenience. However, these lists should be construed as though each member of the list is individually identified as a separate and unique member. Thus, no individual member of such list should be construed as a de facto equivalent of any other member of the same list solely based on their presentation in a common group without indications to the contrary.

Furthermore, certain molecules, constructs, compositions, elements, moieties, excipients, disorders, conditions, properties, steps, or the like may be discussed in the context of one specific embodiment or aspect or in a separate paragraph or section of this disclosure. It is understood that this is merely for convenience and brevity, and any such disclosure is equally applicable to and intended to be combined with any other embodiments or aspects found anywhere in the present disclosure and claims, which all form the application and claimed invention at the filing date. For example, a list of constructs, molecules, method steps, kits, or compositions described with respect to a construct, composition, or method is intended to and does find direct support for embodiments related to constructs, compositions, formulations, and methods described in any other part of this disclosure, even if those method steps, active agents, kits, or compositions are not re-listed in the context or section of that embodiment or aspect.

Unless otherwise specified, a “nucleic acid sequence encoding a protein” includes all nucleotide sequences that are degenerate versions of each other and thus encode the same amino acid sequence.

The term “N-terminally positioned” when referring to a position of a first domain or sequence relative to a second domain or sequence in a polypeptide primary amino acid sequence means that the first domain or sequence is located closer to the N-terminus of the polypeptide primary amino acid sequence than the second domain or sequence. In some embodiments, there may be additional sequences and/or domains between the first domain or sequence and the second domain or sequence.

The term “C-terminally positioned” when referring to a position of a first domain or sequence relative to a second domain or sequence in a polypeptide primary amino acid sequence means that the first domain or sequence is located closer to the C-terminus of the polypeptide primary amino acid sequence than the second domain or sequence. In some embodiments, there may be additional sequences and/or domains between the first domain or sequence and the second domain or sequence.

The term “exogenous” refers to any material introduced from or originating from outside a cell, a tissue, or an organism that is not produced by or does not originate from the same cell, tissue, or organism in which it is being introduced.

The term “transduced,” “transfected,” or “transformed” refers to a process by which an exogenous nucleic acid is introduced or transferred into a cell. A “transduced,” “transfected,” or “transformed” cell (e.g., mammalian cell) is one that has been transduced, transfected, or transformed with exogenous nucleic acid (e.g., a vector) that includes an exogenous nucleic acid encoding any of the activatable cytokine constructs described herein.

The term “nucleic acid” refers to a deoxyribonucleic acid (DNA) or ribonucleic acid (RNA), or a combination thereof, in either a single- or double-stranded form. Unless specifically limited, the term encompasses nucleic acids containing known analogues of natural nucleotides that have similar binding properties as the reference nucleotides. Unless otherwise indicated, a particular nucleic acid sequence also implicitly encompasses complementary sequences as well as the sequence explicitly indicated. In some embodiments of any of the nucleic acids described herein, the nucleic acid is DNA. In some embodiments of any of the nucleic acids described herein, the nucleic acid is RNA.

Modifications can be introduced into a nucleotide sequence by standard techniques known in the art, such as site-directed mutagenesis and polymerase chain reaction (PCR)-mediated mutagenesis. Conservative amino acid substitutions are ones in which the amino acid residue is replaced with an amino acid residue having a similar side chain. Families of amino acid residues having similar side chains have been defined in the art. These families include: amino acids with acidic side chains (e.g., aspartate and glutamate), amino acids with basic side chains (e.g., lysine, arginine, and histidine), non-polar amino acids (e.g., alanine, valine, leucine, isoleucine, proline, phenylalanine, methionine, and tryptophan), uncharged polar amino acids (e.g., glycine, asparagine, glutamine, cysteine, serine, threonine and tyrosine), hydrophilic amino acids (e.g., arginine, asparagine, aspartate, glutamine, glutamate, histidine, lysine, serine, and threonine), hydrophobic amino acids (e.g., alanine, cysteine, isoleucine, leucine, methionine, phenylalanine, proline, tryptophan, tyrosine, and valine). Other families of amino acids include: aliphatic-hydroxy amino acids (e.g., serine and threonine), amide family (e.g., asparagine and glutamine), alphatic family (e.g., alanine, valine, leucine and isoleucine), aromatic family (e.g., phenylalanine, tryptophan, and tyrosine).

As used herein the phrase “specifically binds,” or “immunoreacts with” means that a protein or protein complex reacts with one or more binding partners and does not react with other polypeptides, or binds at much lower affinity, e.g., about or greater than 10⁻⁶M.

The term “treatment” refers to ameliorating at least one symptom of a disorder. In some embodiments, the disorder being treated is a cancer and to ameliorate at least one symptom of a cancer.

Activatable Cytokine Constructs

In one aspect, the present disclosure provides activatable cytokine constructs (ACCs) that include three monomer constructs forming a trimer through their cytokine components. Each of the monomer construct may comprise a cytokine protein (CP), one or more masking moieties (MMs), and one or more cleavable moieties (CMs) positioned between the MMs and the CP. In some embodiments, the MMs may be steric masking moieties (SMMs). In some embodiments, the MMs may be affinity masking moieties (AMMs). In some embodiments, the MMs may include both SMMs and AMMs. In some embodiments, the ACC does not include any covalent bonds between the monomeric units that form the trimer. In some embodiments, the ACC does not include any domain, other than the cytokine itself, that promotes formation of trimers. In some embodiments, the ACC does not include any domain, other than the cytokine itself, that reinforces the formation of trimers. For example, in some embodiments, the ACC may not comprise any domain other than the CP1, the CP2, and the CP3 that covalently links the first, the second, and the third monomer constructs. In some examples, the ACC does not comprise a coil-coiled domain, an Fc domain, or a domain other than the CP1, the CP2, or the CP3 that is capable forming a disulfide bond across separate monomers.

Upon activation, the CMs may be cleaved and the MMs may be released from the ACC, resulting in an active cytokine product. The active cytokine product may remain in a trimeric form, e.g., comprising a trimer formed by the three CPs.

In a specific embodiment, provided herein is an activatable cytokine construct (ACC) that includes a first monomer construct, a second monomer construct, and a third monomer construct, wherein:

- the first monomer construct comprises a first cytokine protein (CP1), a first cleavable moiety (CM1), and a first steric masking moiety (SMM1), wherein the CM1 is positioned between the CP1 and the SMM1;
- the second monomer construct comprising a second cytokine protein (CP2), a second cleavable moiety (CM2), and a second steric masking moiety (SMM2), wherein the CM2 is positioned between the CP2 and the SMM2; and
- the a third monomer construct comprising a third cytokine protein (CP3), a third cleavable moiety (CM3), and a third steric masking moiety (SMM3), wherein the CM3 is positioned between the CP3 and the SMM3.

The CP1, the CP2, and CP3 may bind to one another (e.g., by covalent or non-covalent bonding) thereby forming a trimer of the first, the second, and the third monomer constructs. In some embodiments, each of the SMM1, the SMM2, and the SMM3 is a globular molecule. In one example, the SMM1, the SMM2 and the SMM3 are the same globular molecule (e.g., human serum albumin). In some examples the CP1, the CP2, and the CP3 are tumor necrosis factor superfamily member 14 (TNFSF14, also known as LIGHT).

The ACC may comprise a linker between two of the components described herein. In some examples, the first monomer construct comprises at least one linker, e.g., a linker L1 disposed between the CP1 and the CM1, and/or a linker L2 between the CM1 and the SMM1. In some examples, the second monomer construct comprises at least one linker, e.g., a linker L3 disposed between the CP2 and the CM2, and/or a linker L4 between the CM2 and the SMM2. In some examples, the third monomer construct comprises at least one linker, e.g., a linker L5 disposed between the CP3 and the CM3, and/or a linker L6 between the CM3 and the SMM3.

In some embodiments, the first monomer construct may further comprise a first affinity masking moiety (AMM1) and a fourth cleavable moiety (CM4) positioned between the AMM1 and the CP1, the second monomer construct may further comprise a second affinity masking moiety (AMM2) and a fifth cleavable moiety (CM5) positioned between the AMM2 and the CP2, and the third monomer construct may further comprise a third affinity masking moiety (AMM3) and a sixth cleavable moiety (CM6) positioned between the AMM3 and the CP3.

In some examples, the first monomer construct may further comprise a linker L7 between the AMM1 and the CM4 and/or a linker L8 between the CM4 and the CP1. In some examples, the second monomer construct further comprise a linker L9 between the AMM2 and the CM5 and/or a linker L10 between the CM5 and the CP2. In some examples, the third monomer construct may further comprise a linker L11 between the AMM3 and the CM6 and/or a linker L12 between the CM6 and the CP3.

In another specific embodiment, provided herein is an activatable cytokine construct (ACC) that includes a first monomer construct, a second monomer construct, and a third monomer construct, wherein

- a first monomer construct comprising a first cytokine protein (CP1), a first cleavable moiety (CM1), and a first affinity masking moiety (AMM1), wherein the CM1 is positioned between the CP1 and the AMM1;
- a second monomer construct comprising a second cytokine protein (CP2), a second cleavable moiety (CM2), and a second affinity masking moiety (AMM2), wherein the CM2 is positioned between the CP2 and the AMM2; and
- a third monomer construct comprising a third cytokine protein (CP3), a third cleavable moiety (CM3), and a third affinity steric masking moiety (AMM3), wherein the CM3 is positioned between the CP3 and the AMM3.

The CP1, the CP2, and CP3 may bind to one another thereby forming a trimer of the first, the second, and the third monomer constructs.

The ACC may further comprise one or more spacers, which are an amino acid residue or a peptide incorporated at a free terminus of the mature ACC, for example between the signal peptide and the N-terminus of the mature ACC. In some aspects, a spacer (or “header”) may contain glutamine (Q) residues. In some aspects, residues in the spacer minimize aminopeptidase and/or exopeptidase action to prevent cleavage of N-terminal amino acids. Illustrative and non-limiting spacer amino acid sequences may comprise or consist of any of the following exemplary amino acid sequences: QGQSGS (SEQ ID NO: 76); GQSGS (SEQ ID NO: 1); QSGS (SEQ ID NO: 70); SGS; GS; S; QGQSGQG (SEQ ID NO: 71); GQSGQG (SEQ ID NO: 72); QSGQG (SEQ ID NO: 73); SGQG (SEQ ID NO: 74); GQG; QG; G; QGQSGQ (SEQ ID NO: 80); GQSGQ (SEQ ID NO: 136); QSGQ (SEQ ID NO: 137); QGQSG (SEQ ID NO: 138); QGQS (SEQ ID NO: 139); SGQ; GQ; and Q. In some embodiments, spacer sequences may be omitted.

The term “activatable” when used in reference to a cytokine construct, refers to a cytokine construct that exhibits a first level of one or more activities, whereupon exposure to a condition that causes cleavage of at least one cleavable moiety results in the generation of a cytokine construct that exhibits a second level of the one or more activities, where the second level of activity is greater than the first level of activity. Non-limiting examples of an activities include any of the exemplary activities of a cytokine (e.g., a TNF or TNF sumper family member) described herein or known in the art.

The terms “masking moiety” and “MM” are used interchangeably herein to refer to an amino acid sequence that reduces or inhibits one or more activities of a cytokine protein. In some embodiments, the MM may be a steric masking moiety (SMM), which does not specifically bind to the CP, but rather interferes with CP's binding to its binding partner through steric hindrance. For example, the SMM may be positioned in the uncleaved ACC such that the tertiary or quaternary structure of the ACC allows the SMM to mask the CP through positioning between the SMM and CP and/or charge-based interaction, thereby holding the SMM in place to interfere with binding partner access to the CP. In some embodiments, the MM may be an affinity masking moiety (AMM), which interacts with the CP, thus reducing, inhibiting, or interfering the interaction between the CP and its binding partner. In some embodiments, the AMM may be a peptide mask (“PM”).

The terms “peptide mask” and “PM” are used interchangeably herein to refer to an amino acid sequence of less than 50 amino acids that reduces or inhibits one or more activities of a cytokine protein. The PM may bind to the cytokine and limit the interaction of the cytokine with its receptor. In some embodiments, the PM is no more than 40 amino acids in length. In preferred embodiments, the PM is no more than 20 amino acids in length. In some embodiments, the PM is no more than 19, 18, 17, 16, or 15 amino acids in length.

As used herein, the term “masking efficiency” refers to the activity (e.g., EC50) of the uncleaved ACC divided by the activity of a control cytokine, wherein the control cytokine may be either cleavage product of the ACC or the cytokine used as the CP of the ACC. An ACC having a reduced level of at least one of the CP activity has a masking efficiency that is greater than 10. In some embodiments, the ACCs described herein have a masking efficiency that is greater than 10, greater than 100, greater than 1000, or greater than 5000. Illustrative assays for determining masking efficiency include those described in Example 1.

The terms “cleavable moiety” and “CM” are used interchangeably herein to refer to a peptide, the amino acid sequence of which comprises a substrate for a sequence-specific protease. Cleavable moieties that are suitable for use in the ACC herein include any of the protease substrates that are known the art. Exemplary cleavable moieties are described in more detail below.

As used herein, a polypeptide, such as a cytokine or the steric masking moiety (e.g., albumin such as human serum albumin), may be a wild-type polypeptide (e.g., a naturally-existing polypeptide) or a variant of the wild-type polypeptide. A variant may be a polypeptide modified by substitution, insertion, deletion and/or addition of one or more amino acids of the wild-type polypeptide, provided that the variant retains the basic function or activity of the wild-type polypeptide. In some examples, a variant may have altered (e.g., increased or decreased) function or activity comparing with the wild-type polypeptide. In some aspects, the variant may be a functional fragment of the wild-type polypeptide. The term “functional fragment” means that the sequence of the polypeptide (e.g., cytokine) may include fewer amino acids than the full-length polypeptide sequence, but sufficient polypeptide chain length to confer activity (e.g., cytokine activity).

As used herein, the term “linker” refers to a peptide, the amino acid sequence of which is not a substrate for a protease. A linker may comprise a stretch of amino acid sequence that links two components in the ACC. Exemplary linkers are described in more detail below.

The organization of the components in each of the first, the second, and the third monomer constructs may be arranged in the same order in each monomer construct. In some embodiments, the organization of the components in each of the first, the second, and the third monomer constructs may be arranged in different orders in each monomer construct. In some examples, the corresponding components in each monomer construct (e.g., CP1, CP2, and CP3; or SMM1, SMM2, and SMM3; CM1, CM2, and CM3; AMM1, AMM2, and AMM3; or CM4, CM5, CM6) may be the same in terms of, for example, molecular weights, sizes, amino acid sequences, and the like. In some examples, the corresponding components in each monomer construct (e.g., CP1, CP2, and CP3; or SMM1, SMM2, and SMM3; CM1, CM2, and CM3; AMM1, AMM2, and AMM3; or CM4, CM5, CM6) may be different in terms of, for example, molecular weights, sizes, amino acid sequences, and the like. Thus, the trimeric ACC may have symmetrical or asymmetrical monomer construct components.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the CP1, the CM1, and the SMM1, the second monomer construct comprises the CP2, the CM2, and the SMM2, and the third monomer construct comprises the CP3, the CM3, and the SMM3. An example of such ACCs is shown in FIG. 1A.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the SMM1, the CM1, and the CP1, the second monomer construct comprises the SMM2, the CM2, and the CP2, and the third monomer construct comprises the SMM3, the CM3, and the CP3. An example of such ACCs is shown in FIG. 1B.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the AMM1, the CM1, and the CP1, the second monomer construct comprises the AMM2, the CM2, and the CP2, and the third monomer construct comprises the AMM3, the CM3, and the CP3. An example of such ACCs is shown in FIG. 1C.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the CP1, the CM1, and the AMM1, the second monomer construct comprises the CP2, the CM2, and the AMM2, and the third monomer construct comprises the CP3, the CM3, and the AMM3. An example of such ACCs is shown in FIG. 1D.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the AMM1, the CM4, the CP1, the CM1, and the SMM1, the second monomer construct comprises the AMM2, the CM5, the CP2, the CM2, and the SMM2, and the third monomer construct comprises the AMM3, the CM6, the CP3, the CM3, and the SMM3. An example of such ACCs is shown in FIG. 1E.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the SMM1, the CM1, the CP1, the CM4, and AMM1, the second monomer construct comprises the SMM2, the CM2, the CP2, the CM5, and AMM2, and the third monomer construct comprises the SMM3, the CM3, the CP3, the CM6, and the AMM3. An example of such ACCs is shown in FIG. 1F.

In some embodiments, the AMM and SMM may be on the same side relative to the CP in the monomer construct. The AMM and the SMM may be coupled with the CP with a CM between the CP and the MM closer to the CP. The cleavage of the CM may release both the AMM and SMM from the CP, resulting in the active cytokine product.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the CP1, the CM1, the AMM1, and the SMM1; the second monomer construct comprises the CP2, the CM2, the AMM2, and the SMM2; and the third monomer construct comprises the CP3, the CM3, the AMM3, and the SMM3. An example of such ACCs is shown in FIG. 1H.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the CP1, the CM1, the SMM1, and the AMM1; the first monomer construct comprises the CP2, the CM2, the SMM2, and the AMM2; and the first monomer construct comprises the CP3, the CM3, the SMM3, and the AMM3.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises the SMM1, the AMM1, the CM1, and the CP1; the second monomer construct comprises the SMM2, the AMM2, the CM2, and the CP2, and the third monomer construct comprises the SMM3, the AMM3, the CM3, and the CP3. An example of such ACCs is shown in FIG. 1G.

In some embodiments, in an N- to C-terminal direction, the first monomer construct comprises, the AMM1, the SMM1, the CM1, and the CP1; the second monomer construct comprises the AMM2, the SMM2, the CM2, and the CP2, and the third monomer construct comprises the AMM3, the SMM3, the CM3, and the CP3.

In some embodiments, the ACC may be characterized by a reduction in an activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof, as compared to a control level of an activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof. In some embodiments, a control level can be the level of the activity for a recombinant CP1, CP2, CP3, or the trimer thereof (e.g., a commercially available recombinant CP1, CP2, CP3, or the trimer thereof, a recombinant wild type CP1, CP2, CP3, or the trimer thereof, and the like). In some embodiments, a control level can be the level of the activity of a cleaved (activated) form of the ACC.

In some embodiments, the binding affinity (K_D) of the CP1, CP2, CP3, or the trimer thereof for its binding partner (e.g., a cognate receptor) may be determined using surface plasmon resonance (e.g., performed in phosphate buffered saline at 25° C.). In certain embodiments, the activity may be the level of herpes virus entry mediator (HVEM) activation (e.g., as evaluated using HVEM cell-based assay described in the Example section below). In some embodiments, the activity may be the capability of stimulating the production of IL-5 when engaging the lymphotoxin beta receptor on the surface of the A375 human melanoma cell line (e.g., as evaluated using Lymphotoxin beta receptor cell-based assay as described in the Example section below). In some examples, the ACC shows a reduced activity in the activation of herpes virus entry mediator (HVEM) compared to a control trimer of the CP1, CP2, and CP3. In some examples, the ACC shows a reduced activity in the activation of lymphotoxin beta receptor compared to a control trimer of the CP1, CP2, and CP3. In some examples, the ACC shows a reduced activity in the activation of herpes virus entry mediator (HVEM) and the activation of lymphotoxin beta receptor compared to a control trimer of the CP1, CP2, and CP3. In some examples, the control trimer of CP1, CP2, and CP3 results from activation of the ACC.

In some embodiments, the ACC is characterized by at least a 2-fold, 5-fold, 10-fold, 20-fold, 30-fold, 40-fold, 50-fold, 60-fold, 70-fold, 80-fold, 90-fold, 100-fold, 200-fold, 300-fold, 400-fold, 500-fold, 600-fold, 700-fold, 800-fold, 900-fold, 1000-fold, 10⁴-fold, 10⁵-fold, 10⁶-fold, 10⁷-fold, or 10⁸-fold reduction in an activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof as compared to the control level.

In some embodiments, the ACC is characterized by a 1- to 20-fold reduction, a 200- to 500-fold reduction, a 300- to 500-fold reduction, a 400- to 500-fold reduction, a 500- to 600-fold reduction, a 600- to 700-fold reduction, a 150- to 1000-fold reduction, a 100- to 1500-fold reduction, a 200- to 1500-fold reduction, a 300- to 1500-fold reduction, a 400- to 1500-fold reduction, a 500- to 1500-fold reduction, a 1000- to 1500-fold reduction, a 100- to 1000-fold reduction, a 200- to 1000-fold reduction, a 300- to 1000-fold reduction, a 400- to 1000-fold reduction, a 500- to 1000-fold reduction, a 100- to 500-fold reduction, a 20- to 50-fold reduction, a 30- to 50-fold reduction, a 40- to 50-fold reduction, a 100- to 400-fold reduction, a 200- to 400-fold reduction, or a 300- to 400-fold reduction, a 100- to 300-fold reduction, a 200- to 300-fold reduction, or a 100- to 200-fold reduction in in an activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof as compared to the control level.

In some embodiments, the control level of the activity of the CP1, the CP2, the CP3, or the trimer thereof is the activity of the CP1, the CP2, the CP3, or the trimer thereof released from the ACC following cleavage of CMs by the protease(s) (the “cleavage product”). In some embodiments, the control level of the at least one activity of the CP1, the CP2, the CP3, or the trimer thereof is the activity of a corresponding wild type mature cytokine (e.g., recombinant wild type mature cytokine) or the trimer thereof.

In some embodiments, incubation of the ACC with the protease yields an activated cytokine product(s), where the activity of the CP1, the CP2, the CP3, or the trimer thereof is greater than the one or more activities of the CP1, the CP2, the CP3, or the trimer thereof of the intact ACC (uncleaved). In some embodiments, the activity of the CP1, the CP2, the CP3, or the trimer thereof is at least 1-fold, 2-fold, 3-fold, 4-fold, 5-fold, 10-fold, 20-fold, 30-fold, 40-fold, 50-fold, 60-fold, 70-fold, 80-fold, 90-fold, 100-fold, 200-fold, 300-fold, 400-fold, 500-fold, 600-fold, 700-fold, 800-fold, 900-fold, or 1000-fold, 10⁴-fold, 10⁵-fold, 10⁶-fold, 10⁷-fold, or 10⁸-fold greater than the activity of the CP1, the CP2, the CP3, or the trimer thereof of the ACC. In some embodiments, the activity of the CP1, the CP2, the CP3, or the trimer thereof is 1- to 20-fold greater, a 200- to 500-fold greater, a 300- to 500-fold greater, a 400- to 500-fold greater, a 500- to 600-fold greater, a 600- to 700-fold greater, a 150- to 1000-fold greater, a 100- to 1500-fold greater, a 200- to 1500-fold greater, a 300- to 1500-fold greater, a 400- to 1500-fold greater, a 500- to 1500-fold greater, a 1000- to 1500-fold greater, a 100- to 1000-fold greater, a 200- to 1000-fold greater, a 300- to 1000-fold greater, a 400- to 1000-fold greater, a 500- to 1000-fold greater, a 100- to 500-fold greater, a 20- to 50-fold greater, a 30- to 50-fold greater, a 40- to 50-fold greater, a 100- to 400-fold greater, a 200- to 400-fold greater, or a 300- to 400-fold greater, a 100- to 300-fold greater, a 200- to 300-fold greater, or a 100- to 200-fold greater than the activity of CP1, the CP2, the CP3, or the trimer thereof of the ACC.

In some embodiments, each of the first, the second, and/or the third monomer construct may independently comprise a total of about 150 amino acids to about 850 amino acids, about 150 amino acids to about 800 amino acids, about 150 amino acids to about 750 amino acids, about 150 amino acids to about 700 amino acids, about 150 amino acids to about 650 amino acids, about 150 amino acids to about 600 amino acids, about 150 amino acids to about 550 amino acids, about 150 amino acids to about 500 amino acids, about 150 amino acids to about 450 amino acids, about 150 amino acids to about 400 amino acids, about 150 amino acids to about 350 amino acids, about 150 amino acids to about 300 amino acids, about 150 amino acids to about 250 amino acids, about 150 amino acids to about 200 amino acids, about 200 amino acids to about 850 amino acids, about 200 amino acids to about 800 amino acids, about 200 amino acids to about 750 amino acids, about 200 amino acids to about 700 amino acids, about 200 amino acids to about 650 amino acids, about 200 amino acids to about 600 amino acids, about 200 amino acids to about 550 amino acids, about 200 amino acids to about 500 amino acids, about 200 amino acids to about 450 amino acids, about 200 amino acids to about 400 amino acids, about 200 amino acids to about 350 amino acids, about 200 amino acids to about 300 amino acids, about 200 amino acids to about 250 amino acids, about 250 amino acids to about 800 amino acids, about 250 amino acids to about 750 amino acids, about 250 amino acids to about 700 amino acids, about 250 amino acids to about 650 amino acids, about 250 amino acids to about 600 amino acids, about 250 amino acids to about 550 amino acids, about 250 amino acids to about 500 amino acids, about 250 amino acids to about 450 amino acids, about 250 amino acids to about 400 amino acids, about 250 amino acids to about 350 amino acids, about 250 amino acids to about 300 amino acids, about 300 amino acids to about 800 amino acids, about 300 amino acids to about 750 amino acids, about 300 amino acids to about 700 amino acids, about 300 amino acids to about 650 amino acids, about 300 amino acids to about 600 amino acids, about 300 amino acids to about 550 amino acids, about 300 amino acids to about 500 amino acids, about 300 amino acids to about 450 amino acids, about 300 amino acids to about 400 amino acids, about 300 amino acids to about 350 amino acids, about 350 amino acids to about 800 amino acids, about 350 amino acids to about 750 amino acids, about 350 amino acids to about 700 amino acids, about 350 amino acids to about 650 amino acids, about 350 amino acids to about 600 amino acids, about 350 amino acids to about 550 amino acids, about 350 amino acids to about 500 amino acids, about 350 amino acids to about 450 amino acids, about 350 amino acids to about 400 amino acids, about 400 amino acids to about 800 amino acids, about 400 amino acids to about 750 amino acids, about 400 amino acids to about 700 amino acids, about 400 amino acids to about 650 amino acids, about 400 amino acids to about 600 amino acids, about 400 amino acids to about 550 amino acids, about 400 amino acids to about 500 amino acids, about 400 amino acids to about 450 amino acids, about 450 amino acids to about 800 amino acids, about 450 amino acids to about 750 amino acids, about 450 amino acids to about 700 amino acids, about 450 amino acids to about 650 amino acids, about 450 amino acids to about 600 amino acids, about 450 amino acids to about 550 amino acids, about 450 amino acids to about 500 amino acids, about 500 amino acids to about 850 amino acids, about 500 amino acids to about 800 amino acids, about 500 amino acids to about 750 amino acids, about 500 amino acids to about 700 amino acids, about 500 amino acids to about 650 amino acids, about 500 amino acids to about 600 amino acids, about 500 amino acids to about 550 amino acids, about 550 amino acids to about 850 amino acids, about 550 amino acids to about 800 amino acids, about 550 amino acids to about 750 amino acids, about 550 amino acids to about 700 amino acids, about 550 amino acids to about 650 amino acids, about 550 amino acids to about 600 amino acids, about 600 amino acids to about 850 amino acids, about 600 amino acids to about 800 amino acids, about 600 amino acids to about 750 amino acids, about 600 amino acids to about 700 amino acids, about 600 amino acids to about 650 amino acids, about 650 amino acids to about 850 amino acids, about 650 amino acids to about 800 amino acids, about 650 amino acids to about 750 amino acids, about 650 amino acids to about 700 amino acids, about 700 amino acids to about 850 amino acids, about 700 amino acids to about 800 amino acids, about 700 amino acids to about 750 amino acids, about 750 amino acids to about 800 amino acids, or about 800 amino acids to about 850 amino acids.

In some embodiments, one or more monomer constructs in an ACC may comprise a sequence of any one of SEQ ID NOs: 8, 10, 12, 24, 30, 40, 42, 44, or 46. In some embodiments, one or more monomer constructs in an ACC may comprise a sequence that is at least 80% (e.g., at least 82%, at least 84%, at least 86%, at least 88%, at least 90%, at least 92%, at least 94%, at least 96%, at least 98%, at least 99%, or 100% identical to any one of SEQ ID NOs: 8, 10, 12, 24, 30, 40, 42, 44, or 46. In some embodiments, each of the three monomer constructs in the ACC is identical, and comprises a sequence that is at least 80% (e.g., at least 82%, at least 84%, at least 86%, at least 88%, at least 90%, at least 92%, at least 94%, at least 96%, at least 98%, at least 99%, or 100% identical to any one of SEQ ID NOs. 8, 10, 12, 24, 30, 40, 42, 44, or 46.

In some embodiments, one or more monomer constructs in an ACC may be encoded by a nucleic acid comprising a sequence of any one of SEQ ID NO: 9, 11, 13, 25, 31, 41, 43, 45, or 47.

In some embodiments, one or more monomer constructs in an ACC may be encoded by a nucleic acid comprising a sequence that is at least 80% (e.g., at least 82%, at least 84%, at least 86%, at least 88%, at least 90%, at least 92%, at least 94%, at least 96%, at least 98%, at least 99%, or 100%) identical to any one of SEQ ID NO: 9, 11, 13, 25, 31, 41, 43, 45, or 47.

In some aspects, the present disclosure provides nucleic acids comprising a sequence of any one of SEQ ID NO; 9, 11, 13, 25, 31, 41, 43, 45, or 47. In some aspects, the present disclosure provides nucleic acids comprising a sequence that is at least 80% (e.g., at least 82%, at least 84%, at least 86%, at least 88%, at least 90%, at least 92%, at least 94%, at least 96%, at least 98%, at least 99%, or 100%) identical to any one of SEQ ID NO: 9, 11, 13, 25, 31, 41, 43, 45, or 47. In some aspects, the present disclosure provides one or more vector comprising any of the nucleic acids described herein.

In some aspects, one or more monomer constructs in an ACC may include such sequences but either without the signal sequences of those sequences. Signal sequences are not particularly limited. Some examples of signal sequences include SEQ ID NO: 78.

Masking Moieties (MMs)

The ACCs herein may comprise one or more masking moieties (MMs) capable of interfering with the binding of the CP to its binding partner (e.g., ligand or receptor).

A MM may be a steric masking moiety (SMM) or an affinity masking moiety (AMM) as described herein. A MM may be coupled to a CP by a CM and optionally one or more linkers described herein. In some embodiments, when an ACC is not activated, the MM prevents the CP from target binding; but when the ACC is activated (when the CM is cleaved by a protease), the MMs does not substantially or significantly interfere with the CP's binding to the target.

In the ACC, a MM interfering with the target binding of a CP may be coupled to the CP. Alternatively, a MM interfering with the target binding of a CP may be coupled to a component of the ACC that is not the CP. For example, the MM may be coupled to a different CP. In either case, in the tertiary or quaternary structure of the activatable structure, the MM may be in a position (e.g., proximal to the CP to be masked) that allows the MM to mask the CP.

In some embodiments, a MM may interact with the CP, thus reducing or inhibiting the interaction between the CP and its binding partner. In some embodiments, the MM may comprise at least a partial or complete amino acid sequence of a naturally occurring binding partner of the CP. For example, the MM may be a fragment of a naturally occurring binding partner. The fragment may retain no more than 95%, 90%, 80%, 75%, 70%, 60%, 50%, 40%0, 30%, 25%, or 20% nucleic acid or amino acid sequence homology to the naturally occurring binding partner.

In some embodiments, the MM may not specifically bind to the CP, but still interfere with CP's binding to its binding partner through non-specific interactions such as steric hindrance. For example, the MM may be positioned in the ACC such that the tertiary or quaternary structure of the ACC allows the MM to mask the CP through charge-based interaction, thereby holding the MM in place to interfere with binding partner access to the CP.

In some embodiments, the masking moiety (e.g., the steric masking moiety such as albumin (e.g., HSA)) may stabilize the ACC in the inactivated state.

In some examples, a SMM may be a peptide whose size, structure, conformation, and/or position in the ACC prevents, inhibits, or interfere the binding of the CP to its binding partner. In some examples, the SMM may be a globular protein, e.g., an albumin such as ovalbumin, human serum albumin (HSA), and bovine serum albumin (BSA). In a particular example, the SMM may be a human serum albumin, e.g., SEQ ID NO: 56. In some examples, the SMM may comprise a sequence that is at least at least 80% (e.g., at least 82%, at least 84%, at least 86%, at least 88%, at least 90%, at least 92%, at least 94%, at least 96%, at least 98%, at least 99%, or 100%) identical to SEQ ID NO: 56.

In some embodiments, an AMM may be a cognate peptide of the CP. For example, the MM may comprise a sequence of the CP's epitope, ligand, or receptor, or a fragment thereof. In cases where the CP is a TNFSF14, an AMM may be a receptor or a portion thereof of the TNFSF14, e.g., SEQ ID NO: 61.

The term “naturally occurring” as used herein as applied to an object refers to the fact that an object can be found in nature. For example, a polypeptide or polynucleotide sequence that is present in an organism (including viruses) that can be isolated from a source in nature and that has not been intentionally modified by man in the laboratory or otherwise is naturally occurring.

In some embodiments, the MM may comprise an amino acid sequence that is not naturally occurring or does not contain the amino acid sequence of a naturally occurring binding partner or target protein. In certain embodiments, the MM is not a natural binding partner of the CP. The MM may be a modified binding partner for the CP which contains amino acid changes that decrease affinity and/or avidity of binding to the CP. In some embodiments the MM may contain no or substantially no nucleic acid or amino acid homology to the CP's natural binding partner. In other embodiments the MM is no more than 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or 80% similar to the natural binding partner of the CP.

In some embodiments, the MM may have a dissociation constant for binding to the CP that is no more than the dissociation constant of the CP to the target. In some embodiments, the MM may not interfere or compete with the CP for binding to the target in a cleaved state.

The structural properties of the MMs may be selected according to factors such as the minimum amino acid sequence required for interference with protein binding to target, the target protein-protein binding pair of interest, the size of the CP, the presence or absence of linkers, and the like.

In some embodiments, the MM may be unique for the coupled CP. Examples of MMs include MMs that were specifically screened to bind a binding domain of the CP or fragment thereof (e.g., affinity masks). Methods for screening MMs to obtain MMs unique for the CP and those that specifically and/or selectively bind a binding domain of a binding partner/target are provided herein and can include protein display methods.

As used herein, the term “masking efficiency” refers to the activity (e.g., EC₅₀) of the ACC in the inactivated state divided by the activity of a control antibody, wherein the control antibody may be either cleavage product of the ACC or the antibody or fragment thereof used as the CP of the activatable target-binding protein. An ACC having a reduced level of a CP activity may have a masking efficiency that is greater than 10. In some embodiments, the activatable target-binding proteins described herein may have a masking efficiency that is greater than 10, 100, 1000, or 5000.

In some embodiments, the MM may be a polypeptide of about 2 to 50 amino acids in length. For example, the MM may be a polypeptide of from 2 to 40, from 2 to 30, from 2 to 20, from 2 to 10, from 5 to 15, from 10 to 20, from 15 to 25, from 20 to 30, from 25 to 35, from 30 to 40, from 35 to 45, from 40 to 50 amino acids in length. For example, the MM may be a polypeptide with 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 31, 32, 33, 34, 35, 36, 37, 38, 39, 40, 41, 42, 43, 44, 45, 46, 47, 48, 49, or 50 amino acids in length. In some examples, the MM may be a polypeptide of more than 50 amino acids in length, e.g., 100, 200, 300, 400, 500, 600, 700, 800, or more amino acids.

In some embodiments, in an inactive state of the ACC with an CP and an interfering MM, in the presence of the target of an CP, there is no binding or substantially no binding of the CP to the target, or no more than 0.001%, 0.01%, 0.1%, 1%, 2%, 3%, 4%, 5%, 6%, 7%, 8%, 9%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, or 50% binding of the CP to its target, as compared to the binding of an counterpart antibody without the interfering MM, for at least 0.1, 0.5, 1, 2, 4, 6, 8, 12, 28, 24, 30, 36, 48, 60, 72, 84, 96 hours, or 5, 10, 15, 30, 45, 60, 90, 120, 150, 180 days, or 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, or 12 months when measured in vitro immunoabsorbant assay, e.g., as described in US20200308243A1.

The binding affinity of the CP towards the target or binding partner with an interfering MM may be at least 5, 10, 25, 50, 100, 250, 500, 1,000, 2,500, 5,000, 10,000, 50,000, 100,000, 500,000, 1,000,000, 5,000,000, 10,000,000, 50,000,000 times lower than the binding affinity of the CP towards its binding partner without an interfering MM, or between 5-10, 10-100, 10-1,000, 10-10,000, 10-100,000, 10-1,000,000, 10-10,000,000, 100-1,000, 100-10,000, 100-100,000, 100-1,000,000, 100-10,000,000, 1,000-10,000, 1,000-100,000, 1,000-1,000,000, 1000-10,000,000, 10,000-100,000, 10,000-1,000,000, 10,000-10,000,000, 100,000-1,000,000, or 100,000-10,000,000 times lower than the binding affinity of the CP towards its binding partner when there is no interfering MM.

The dissociation constant of the MM towards the CP it masks, may be greater than the dissociation constant of the CP towards the target. The dissociation constant of the MM towards the masked CP may be at least 5, 10, 25, 50, 100, 250, 500, 1,000, 2,500, 5,000, 10,000, 100,000, 1,000,000 or even 10,000,000 times greater than the dissociation constant of the CP towards the target. Conversely, the binding affinity of the MM towards the masked CP may be lower than the binding affinity of the CP towards the target. The binding affinity of MM towards the CP may be at least 5, 10, 25, 50, 100, 250, 500, 1,000, 2,500, 5,000, 10,000, 100,000, 1,000,000 or even 10,000,000 times lower than the binding affinity of the CP towards the target.

In some embodiments, the MMs may contain genetically encoded or genetically non-encoded amino acids. Examples of genetically non-encoded amino acids are but not limited to D-amino acids, β-amino acids, and γ-amino acids. In specific embodiments, the MMs contain no more than 50%, 40%, 30%, 20%, 15%, 10%, 5% or 1% of genetically non-encoded amino acids.

In some embodiments, once released from the ACC and in a free state, the MM may have a biological activity or a therapeutic effect, such as binding capability. For example, the free peptide may bind with the same or a different binding partner. In certain embodiments, the free MM may exert a therapeutic effect, providing a secondary function to the compositions disclosed herein. In some embodiments, once uncoupled from the ACC and in a free state, the MM may advantageously not exhibit biological activity. For example, in some embodiments the MM in a free state does not elicit an immune response in the subject.

Suitable MMs may be identified and/or further optimized through a screening procedure from a library of candidate activatable target-binding proteins having variable MMs. For example, a CP and a CM may be selected to provide for a desired enzyme/target combination, and the amino acid sequence of the MM can be identified by the screening procedure described below to identify a MM that provides for an activatable phenotype. For example, a random peptide library (e.g., of peptides comprising 2 to 40 amino acids or more) may be used in the screening methods disclosed herein to identify a suitable MM.

In some embodiments, MMs with specific binding affinity for a CP may be identified through a screening procedure that includes providing a library of peptide scaffolds comprising candidate MMs wherein each scaffold is made up of a transmembrane protein and the candidate MM. The library may then be contacted with an entire or portion of a protein such as a full length protein, a naturally occurring protein fragment, or a non-naturally occurring fragment containing a protein (also capable of binding the binding partner of interest), and identifying one or more candidate MMs having detectably bound protein. The screening may be performed by one more rounds of magnetic-activated sorting (MACS) or fluorescence-activated sorting (FACS), as well as determination of the binding affinity of MM towards the CP and subsequent determination of the masking efficiency, e.g., as described in WO2009025846 and US20200308243A1, which are incorporated herein by reference in their entireties.

Cytokine Proteins

The ACC may employ any of a variety of cytokine proteins that can form a trimer. Examples of such cytokine proteins include members of the tumor necrosis factor (TNF) ligand superfamily, such as a member of TNF or TNF superfamily member. Examples of the cytokine proteins include tumor necrosis factor superfamily member 14 (TNFSF14, also known as LIGHT), tumor necrosis factor TNF (e.g., TNF-alpha, -beta, or -C), TNFSF4, TNFSF5, TNFSF6, TNFSF7, TNFSF8, TNFSF9, TNFSF10, TNFSF1, TNFSF12, TNFSF13, TNFSF13B, TNFSF15, and TNFSF18. In one example, the cytokine proteins are LIGHT (also known as TNFSF14). In some examples, the ACC comprises a cytokine that is not TNF (e.g., a member of the TNF superfamily other than TNF).

In some embodiments, the cytokine proteins may be mature cytokine proteins. The term “mature cytokine protein” refers herein to a cytokine protein that lacks a signal sequence. A signal sequence is also referred to herein as a “signal peptide.” A mature cytokine protein may also lack intracellular and/or transmembrane domain(s). A cytokine protein (CP) may be a mature cytokine protein or a cytokine protein with a signal peptide, intracellular domain, transmembrane domain, or a portion thereof. In some embodiments, the cytokine proteins may comprise a signal peptide. In some examples, the ACCs of the present disclosure may include sequences disclosed herein, including or lacking the signal sequences recited herein.

For example, sequences of such proteins include those exemplified herein and additional sequences can be obtained from ncbi.nlm.nih.gov/protein. Truncation variants that are suitable for use in the ACCs of the present invention include any N- or C-terminally truncated cytokine that retains a cytokine activity. In some examples, the truncation variants may be cytokine polypeptides that are N- and/or C-terminally truncated by 1 to about 200 amino acids, 1 to about 150 amino acids, 1 to about 100 amino acids, 1 to about 95 amino acids, 1 to about 90 amino acids, 1 to about 85 amino acids, 1 to about 80 amino acids, 1 to about 75 amino acids, 1 to about 70 amino acids, 1 to about 65 amino acids, 1 to about 60 amino acids, 1 to about 55 amino acids, 1 to about 50 amino acids, 1 to about 45 amino acids, 1 to about 40 amino acids, 1 to about 35 amino acids, 1 to about 30 amino acids, 1 to about 25 amino acids, 1 to about 20 amino acids, 1 to about 15 amino acids, 1 to about 10 amino acids, 1 to about 8 amino acids, 1 to about 6 amino acids, 1 to about 4 amino acids, that retain a cytokine activity. In some of the foregoing embodiments, the truncated CP is an N-terminally truncated CP. In other embodiments, the truncated CP is a C-terminally truncated CP. In certain embodiments, the truncated CP is a C- and an N-terminally truncated CP. In some embodiments, the CP is truncated to remove a naturally-occurring protease recognition sequence (i.e., to remove a site that may be susceptible to cleavage by a protease).

In some examples, each of the CP1, the CP2, and the CP3 may independently comprise a cytokine (e.g., mutant of a wild type cytokine) that is cross-reactive among multiple species. The cross-reactive cytokine may bind to receptors in different species and activate the corresponding signaling pathways. In some examples, the cross-reactive cytokine is mouse-human cross-reactive, i.e., can bind to receptors in both human and mouse and activate the corresponding signaling pathway(s). In some examples, the cross-reactive cytokine is a mouse-human cross-reactive TNFSF14. The mouse-human cross-reactive TNFSF14 may comprise one or more mutations on human TNFSF14 protein. In one example, the mouse-human cross-reactive TNFSF14 comprises a sequence of SEQ ID NO: 55. Additional cross-reactive cytokines may be identified by screening a random error mutagenesis library of a cytokine (e.g., a wild type cytokine) using yeast surface display, e.g., as described in Tang et al. Cancer Cell. 2016 Mar. 14; 29(3):285-296, which is incorporated by reference in its entirety.

In some embodiments, each of the CP1, the CP2, and the CP3 may independently comprise an amino acid sequence that is at least 80% identical (e.g., at least 82%, at least 84%, at least 86%, at least 88%, at least 90%, at least 92%, at least 94%, at least 95%, at least 96%, at least 97%, at least 98%, at least 99%, or 100% identical) to a cytokine reference sequence of SEQ ID NO: 54 or 55.

The percentage of sequence identity refers to the level of amino acid sequence identity between two or more peptide sequences when aligned using a sequence alignment program, e.g., the suite of BLAST programs, publicly available on the Internet at the NCBI website. See also Altschul et al., J. Mol. Biol. 215:403-10, 1990.

In some embodiments, the CP1, CP2, and/or CP3 exhibit(s) an activity of a member of tumor necrosis factor or tumor necrosis factor super family (e.g., TNFSF14) and include(s) an amino acid sequence that is at least 80% identical, at least 82% identical, at least 84% identical, at least 86% identical, at least 88% identical, at least 90% identical, at least 92% identical, at least 94% identical, at least 96% identical, at least 98% identical, or at least 99% identical, or 100% identical to a sequence of SEQ ID NO: 54 or 55.

The number of amino acids in the sequence of the cytokine proteins employed may vary, depending on the specific cytokine protein employed. In some embodiments, the CP1, the CP2, and/or the CP3 includes a total of about 10 amino acids to about 700 amino acids, about 10 amino acids to about 650 amino acids, about 10 amino acids to about 600 amino acids, about 10 amino acids to about 550 amino acids, about 10 amino acids to about 500 amino acids, about 10 amino acids to about 450 amino acids, about 10 amino acids to about 400 amino acids, about 10 amino acids to about 350 amino acids, about 10 amino acids to about 300 amino acids, about 10 amino acids to about 250 amino acids, about 10 amino acids to about 200 amino acids, about 10 amino acids to about 150 amino acids, about 10 amino acids to about 100 amino acids, about 10 amino acids to about 80 amino acids, about 10 amino acids to about 60 amino acids, about 10 amino acids to about 40 amino acids, about 10 amino acids to about 20 amino acids, about 20 amino acids to about 700 amino acids, about 20 amino acids to about 650 amino acids, about 20 amino acids to about 600 amino acids, about 20 amino acids to about 550 amino acids, about 20 amino acids to about 500 amino acids, about 20 amino acids to about 450 amino acids, about 20 amino acids to about 400 amino acids, about 20 amino acids to about 350 amino acids, about 20 amino acids to about 300 amino acids, about 20 amino acids to about 250 amino acids, about 20 amino acids to about 200 amino acids, about 20 amino acids to about 150 amino acids, about 20 amino acids to about 100 amino acids, about 20 amino acids to about 80 amino acids, about 20 amino acids to about 60 amino acids, about 20 amino acids to about 40 amino acids, about 40 amino acids to about 700 amino acids, about 40 amino acids to about 650 amino acids, about 40 amino acids to about 600 amino acids, about 40 amino acids to about 550 amino acids, about 40 amino acids to about 500 amino acids, about 40 amino acids to about 450 amino acids, about 40 amino acids to about 400 amino acids, about 40 amino acids to about 350 amino acids, about 40 amino acids to about 300 amino acids, about 40 amino acids to about 250 amino acids, about 40 amino acids to about 200 amino acids, about 40 amino acids to about 150 amino acids, about 40 amino acids to about 100 amino acids, about 40 amino acids to about 80 amino acids, about 40 amino acids to about 60 amino acids, about 60 amino acids to about 700 amino acids, about 60 amino acids to about 650 amino acids, about 60 amino acids to about 600 amino acids, about 60 amino acids to about 550 amino acids, about 60 amino acids to about 500 amino acids, about 60 amino acids to about 450 amino acids, about 60 amino acids to about 400 amino acids, about 60 amino acids to about 350 amino acids, about 60 amino acids to about 300 amino acids, about 60 amino acids to about 250 amino acids, about 60 amino acids to about 200 amino acids, about 60 amino acids to about 150 amino acids, about 60 amino acids to about 100 amino acids, about 60 amino acids to about 80 amino acids, about 80 amino acids to about 700 amino acids, about 80 amino acids to about 650 amino acids, about 80 amino acids to about 600 amino acids, about 80 amino acids to about 550 amino acids, about 80 amino acids to about 500 amino acids, about 80 amino acids to about 450 amino acids, about 80 amino acids to about 400 amino acids, about 80 amino acids to about 350 amino acids, about 80 amino acids to about 300 amino acids, about 80 amino acids to about 250 amino acids, about 80 amino acids to about 200 amino acids, about 80 amino acids to about 150 amino acids, about 80 amino acids to about 100 amino acids, about 100 amino acids to about 700 amino acids, about 100 amino acids to about 650 amino acids, about 100 amino acids to about 600 amino acids, about 100 amino acids to about 550 amino acids, about 100 amino acids to about 500 amino acids, about 100 amino acids to about 450 amino acids, about 100 amino acids to about 400 amino acids, about 100 amino acids to about 350 amino acids, about 100 amino acids to about 300 amino acids, about 100 amino acids to about 250 amino acids, about 100 amino acids to about 200 amino acids, about 100 amino acids to about 150 amino acids, about 150 amino acids to about 700 amino acids, about 150 amino acids to about 650 amino acids, about 150 amino acids to about 600 amino acids, about 150 amino acids to about 550 amino acids, about 150 amino acids to about 500 amino acids, about 150 amino acids to about 450 amino acids, about 150 amino acids to about 400 amino acids, about 150 amino acids to about 350 amino acids, about 150 amino acids to about 300 amino acids, about 150 amino acids to about 250 amino acids, about 150 amino acids to about 200 amino acids, about 200 amino acids to about 700 amino acids, about 200 amino acids to about 650 amino acids, about 200 amino acids to about 600 amino acids, about 200 amino acids to about 550 amino acids, about 200 amino acids to about 500 amino acids, about 200 amino acids to about 450 amino acids, about 200 amino acids to about 400 amino acids, about 200 amino acids to about 350 amino acids, about 200 amino acids to about 300 amino acids, about 200 amino acids to about 250 amino acids, about 250 amino acids to about 700 amino acids, about 250 amino acids to about 650 amino acids, about 250 amino acids to about 600 amino acids, about 250 amino acids to about 550 amino acids, about 250 amino acids to about 500 amino acids, about 250 amino acids to about 450 amino acids, about 250 amino acids to about 400 amino acids, about 250 amino acids to about 350 amino acids, about 250 amino acids to about 300 amino acids, about 300 amino acids to about 700 amino acids, about 300 amino acids to about 650 amino acids, about 300 amino acids to about 600 amino acids, about 300 amino acids to about 550 amino acids, about 300 amino acids to about 500 amino acids, about 300 amino acids to about 450 amino acids, about 300 amino acids to about 400 amino acids, about 300 amino acids to about 350 amino acids, about 350 amino acids to about 700 amino acids, about 350 amino acids to about 650 amino acids, about 350 amino acids to about 600 amino acids, about 350 amino acids to about 550 amino acids, about 350 amino acids to about 500 amino acids, about 350 amino acids to about 450 amino acids, about 350 amino acids to about 400 amino acids, about 400 amino acids to about 700 amino acids, about 400 amino acids to about 650 amino acids, about 400 amino acids to about 600 amino acids, about 400 amino acids to about 550 amino acids, about 400 amino acids to about 500 amino acids, about 400 amino acids to about 450 amino acids, about 450 amino acids to about 700 amino acids, about 450 amino acids to about 650 amino acids, about 450 amino acids to about 600 amino acids, about 450 amino acids to about 550 amino acids, about 450 amino acids to about 500 amino acids, about 500 amino acids to about 700 amino acids, about 500 amino acids to about 650 amino acids, about 500 amino acids to about 600 amino acids, about 500 amino acids to about 550 amino acids, about 550 amino acids to about 700 amino acids, about 550 amino acids to about 650 amino acids, about 550 amino acids to about 600 amino acids, about 600 amino acids to about 700 amino acids, about 600 amino acids to about 650 amino acids, or about 650 amino acids to about 700 amino acids. In some embodiments, CP1, the CP2, and/or the CP3 is a mature wild type human cytokine protein.

Cleavable Moieties

In some aspects, positioned between a CP and an MM (e.g., SMM and/or AMM) components in an ACC, either directly or indirectly (e.g., via a linker), is a cleavable moiety (CM) that comprises a substrate for a protease. In some embodiments, each of the CMs in the ACC may independently comprise a substrate for a protease selected from the group consisting of ADAM8, ADAM9, ADAM10, ADAM12, ADAM15, ADAM17/TACE, ADEMDEC1, ADAMTS1, ADAMTS4, ADAMTS5, BACE, Renin, Cathepsin D, Cathepsin E, Caspase 1, Caspase 2, Caspase 3, Caspase 4, Caspase 5, Caspase 6, Caspase 7, Caspase 8, Caspase 9, Caspase 10, Caspase 14, Cathepsin A, Cathepsin B, Cathepsin C, Cathepsin G, Cathepsin K, Cathepsin L, Cathepsin S, Cathepsin V/L2, Cathepsin X/Z/P, Chymase, Cruzipain, DESC1, DPP-4, FAP, Legumain, Otubain-2, Elastase, FVIIa, FiXA, FXa, FXIa, FXIIa, Granzyme B, Guanidinobenzoatase, Hepsin, HtrA1, Human Neutrophil Elastase, KLK4, KLK5, KLK6, KLK7, KLK8, KLK10, KLK11, KLK13, KLK14, Lactoferrin, Marapsin, Matriptase-2, Meprin, MT-SP1/Matriptase, Neprilysin, NS3/4A, PACE4, Plasmin, PSMA, PSA, BMP-1, MMP1, MMP2, MMP3, MMP7, MMP8, MMP9, MMP10, MMP11, MMP12, MMPP13, MMP14, MMP15, MMP16, MMP17, MMPP19, MMP20, MMP23, MMP24, MMP26, MMP27, TMPRSS2, TMPRSS3, TMPRSS4, tPA, Thrombin, Tryptase, and uPA.

In some embodiments, the protease that cleaves any of the CMs described herein can be ADAM8, ADAM9, ADAM10, ADAM12, ADAM15, ADAM17/TACE, ADAMDEC1, ADAMTS1, ADAMTS4, ADAMTS5, BACE, Renin, Cathepsin D, Cathepsin E, Caspase 1, Caspase 2, Caspase 3, Caspase 4, Caspase 5, Caspase 6, Caspase 7, Caspase 8, Caspase 9, Caspase 10, Caspase 14, Cathepsin B, Cathepsin C, Cathepsin K, Cathespin L, Cathepsin S, Cathepsin V/L2, Cathepsin X/Z/P, Cruzipain, Legumain, Otubain-2, KLK4, KLK5, KLK6, KLK7, KLK8, KLK10, KLK11, KLK13, KLK14, Meprin, Neprilysin, PSMA, BMP-1, MMP-1, MMP-2, MMP-3, MMP-7, MMP-9, MMP-10, MMP-11, MMP-12, MMP-13, MMP-14, MMP-15, MMP-16, MMP-17, MMP-19, MMP-20, MMP-23, MMP-24, MMP-26, MMP-27, activated protein C, cathepsin A, cathepsin G, Chymase, FVIIa, FIXa, FXa, FXIa, FXIIa, Elastase, Granzyme B, Guanidinobenzoatase, HtrA1, human neutrophil lyase, lactoferrin, marapsin, NS3/4A, PACE4, Plasmin, PSA, tPA, thrombin, tryptase, uPA, DESC1, DPP-4, FAP, Hepsin, Matriptase-2, MT-SP1/Matripase, TMPRSS2, TMPRSS3, or TMPRSS4.

In some embodiments, the protease is selected from the group of: uPA, legumain, MT-SP1, ADAM17, BMP-1, TMPRSS3, TMPRSS4, MMP-2, MMP-9, MMP-12, MMP-13, and MMP-14.

In some embodiments, the CM is selected for use with a specific protease. The protease may be one produced by a tumor cell (e.g., the tumor cell may express greater amounts of the protease than healthy tissues). In some embodiments, the CM is a substrate for at least one protease selected from the group of an ADAM 17, a BMP-1, a cysteine protease such as a cathepsin, a HtrA1, a legumain, a matriptase (MT-SP1), a matrix metalloprotease (MMP), a neutrophil elastase, a TMPRSS, such as TMPRSS3 or TMPRSS4, a thrombin, and a u-type plasminogen activator (uPA, also referred to as urokinase).

In some embodiments, a CM is a substrate for at least one matrix metalloprotease (MMP). Examples of MMPs include MMP1, MMP2, MMP3, MMP7, MMP8, MMP9, MMP10, MMP11, MMPP12, MMP13, MMP14, MMP15, MMP16, MMPP17, MMP19, MMP20, MMP23, MMP24, MMP26, and MMP27. In some embodiments, the CM is a substrate for MMP9, MMP14, MMP1, MMP3, MMP13, MMP17, MMP11, and MMP19. In some embodiments, the CM is a substrate for MMP7. In some embodiments, the CM is a substrate for MMP9. In some embodiments, the CM is a substrate for MMP14. In some embodiments, the CM is a substrate for two or more MMPs. In some embodiments, the CM is a substrate for at least MMP9 and MMP14. In some embodiments, the CM includes two or more substrates for the same MMP. In some embodiments, the CM includes at least two or more MMP9 substrates. In some embodiments, the CM includes at least two or more MMP14 substrates.

Increased levels of proteases having known substrates have been reported in a number of cancers. See, e.g., La Roca et al., British J. Cancer 90(7):1414-1421, 2004. Substrates suitable for use in the CM components employed herein include those which are more prevalently found in cancerous cells and tissue. Thus, in certain embodiments, each of the CMs in the ACC may independently comprise a substrate for a protease that is more prevalently found in diseased tissue associated with a cancer. In some embodiments, the cancer is selected from the group of: gastric cancer, breast cancer, osteosarcoma, and esophageal cancer. In some embodiments, the cancer is breast cancer. In some embodiments, the cancer is a HER2-positive cancer. In some embodiments, the cancer is Kaposi sarcoma, hairy cell leukemia, chronic myeloid leukemia (CML), follicular lymphoma, renal cell cancer (RCC), melanoma, neuroblastoma, basal cell carcinoma, cutaneous T-cell lymphoma, nasopharyngeal adenocarcimoa, breast cancer, ovarian cancer, bladder cancer, BCG-resistant non-muscle invasive bladder cancer (NMIBC), endometrial cancer, pancreatic cancer, non-small cell lung cancer (NSCLC), colorectal cancer, esophageal cancer, gallbladder cancer, glioma, head and neck carcinoma, uterine cancer, cervical cancer, or testicular cancer, and the like. In some of the above-described embodiments, the CM components comprise substrates for protease(s) that is/are more prevalent in tumor tissue.

In some embodiments, the CM may be or comprise a sequence of encompassed by the consensus of sequence of any one of the sequences in Table 1 below and SEQ ID NOs: 62, 63, and 81. In some embodiments, the CM is at least 95%, 98% or 99% identical to a sequence selected from the group consisting of SEQ ID Nos: 62, 63, and 81.

TABLE 1

Exemplary CM sequences

SEQ

Sequences
ID NO

AANALAHGLF
140

AANL
141

AANLGSGGSS
142

AAPRS
143

AAPRSF
144

AARGPAIH
145

AAYHLVSQ
146

AFPDMRSVRS
147

AFQALRM
148

AFRHLR
149

AGLGISST
150

AGLGVVER
151

AGPR
152

AHGL
153

AHGLF
154

AHQALRM
155

AIPRVRLFDV
156

ALAHG
157

ALAHGL
158

ALAHGLF
159

ALAHGLFAPRSF
160

ALAHGLFSGRSA
161

N

ALAHGLPTFVHL
162

ALGLLRLP
163

ALPSVKMVSE
164

ALRAP
165

ANQALRM
166

ANQALRMA
167

APPLVKSMVV
168

APPSFKLVNA
169

APRS
170

APRSALAHGLF
171

APRSF
172

AQFVLTEG
173

AQNLLGMV
174

ARGP
175

ARGPS
176

ARGPSF
177

ARGPSFK
178

ASGLLRFP
179

ASPTMKTVGL
180

AVGLLAPP
181

AVGLLAPPGGLS
182

GRSANI

AVGLLAPPGGLS
183

GRSANP

AVGLLAPPGGLS
184

GRSDDH

AVGLLAPPGGLS
185

GRSDIH

AVGLLAPPGGLS
186

GRSDNH

AVGLLAPPGGLS
187

GRSDNI

AVGLLAPPGGLS
188

GRSDNP

AVGLLAPPGGLS
189

GRSDQH

AVGLLAPPGGLS
190

GRSDTH

AVGLLAPPGGLS
191

GRSDYH

AVGLLAPPGGLS
192

GRSNI

AVGLLAPPGGLS
193

GRSNIG

AVGLLAPPGGLS
194

GRSNIGS

AVGLLAPPGGTS
195

TSGRSANPRG

AVGLLAPPSGRS
196

ANPRG

AVGLLAPPTSGR
197

SANPRG

AVPKVRVVPE
198

CGPPLGR
199

CSPPLGR
200

DEVDGSGGSS
201

DEXXXC(A/S)
202

DISHWRRS
203

DLAHPLL
204

DLPLVKSLPS
205

DLXXT(A/S)
206

DRLSGRSANHK
207

K

DRLSGRSDNHK
208

K

DRPEMKSLSG
209

DRPKVKTMDF
210

DVAQFVLT
211

DVPPMKTLRP
212

DWLYWMGI
213

DWLYWMSI
214

DWLYWPGI
215

DWLYWPSI
216

EAPKVKALPK
217

EHPRVKVVSE
218

EKPRMKLFQG
219

EPQALAMS
220

EQPEVKMVKG
221

ERPGVKSLVL
222

ESLPVVAV
223

ESPVMKSMAL
224

ESRRW
225

ESRRWM
226

ESRRWMP
227

ETPSVKTMGR
228

ETPSVKTMGRSS
229

FPRPLGITGL
230

FRLLDWQW
231

GCGPPLGR
232

GCSPPLGR
233

GFPHMKTFQH
234

GFPHMKTFQHSS
235

GGGPPLGR
236

GGPPLGR
237

GGQPSGMWGW
238

GGSIDGR
239

GGSPPLGR
240

GGWHTGRN
241

GIAGQ
242

GLGTPRGLFA
243

GLPTFV
244

GLPTFVH
245

GLPTFVHL
246

GLPTFVHLPRQV
247

GLSGRSDNHGSS
248

GPEGLRVG
249

GPLGIAGI
250

GPLNGRSDNHK
251

A

GPLNGRSDNHK
252

K

GPLNGRSDNHK
253

R

GPLNGRSDNHQ
254

A

GPLNGRSDNHQ
255

K

GPLNGRSDNHQ
256

R

GPLNGRSDNHR
257

A

GPLNGRSDNHR
258

K

GPLNGRSDNHR
259

R

GPLSGRSDNHKA
260

GPLSGRSDNHKK
261

GPLSGRSDNHKR
262

GPLSGRSDNHQA
263

GPLSGRSDNHQK
264

GPLSGRSDNHQR
265

GPLSGRSDNHRA
266

GPLSGRSDNHRK
267

GPLSGRSDNHRR
268

GPPLGR
269

GPQGIAGQ
270

GPQGLLGA
271

GPRSFG
272

GPRSFGL
273

GPSHLVLT
274

GPTN
275

GPTNALAHGLF
276

GRSML
277

GRSMLL
278

GRSMLLG
279

GRSMLLGG
280

GRSMLLGP
281

GRSMLLGS
282

GRSMLLP
283

GRSMLLPG
284

GRSMLLPP
285

GRSMLLPS
286

GRSMLLS
287

GRSMLLSG
288

GRSMLLSP
289

GRSMLLSS
290

GRSMLM
291

GRSMLMG
292

GRSMLMGG
293

GRSMLMGP
294

GRSMLMGS
295

GRSMLMP
296

GRSMLMPG
297

GRSMLMPP
298

GRSMLMPS
299

GRSMLMS
300

GRSMLMSG
301

GRSMLMSP
302

GRSMLMSS
303

GSGPPLGR
304

GSPPLGR
305

GSSPPLGR
306

GTGRGPSWVGS
307

S

HMMQYARH
308

HTGRSGAL
309

HVPRQ
310

HVPRQV
311

HVPRQVAPRSF
312

HVPRQVLSGRS
313

HVPRQVLSGRSA
314

N

HWHLGPPT
315

IANLLSMV
316

IDGR
317

IEGR
318

ILNLLSMV
319

ILPRSPAF
320

IPFSWSRF
321

IQNLLSMV
322

ISSGL
323

ISSGLL
324

ISSGLLS
325

ISSGLLSGRSANI
326

ISSGLLSGRSANP
327

ISSGLLSGRSANP
328

RG

ISSGLLSGRSDDH
329

ISSGLLSGRSDIH
330

ISSGLLSGRSDNH
331

ISSGLLSGRSDNI
332

ISSGLLSGRSDNP
333

ISSGLLSGRSDQH
334

ISSGLLSGRSDTH
335

ISSGLLSGRSDYH
336

ISSGLLSGRSGNH
337

ISSGLLSGRSNI
338

ISSGLLSGRSNIG
339

ISSGLLSGRSNIGS
340

ISSGLLSS
341

ISSGLLSSGGSGG
342

SLSGRSDNH

ISSGLLSSGGSGG
343

SLSGRSGNH

ISSGLSS
344

IVSRSA
345

KGLTGRSDRHQA
346

KGPKVKVVTL
347

KNLYGRSENNGN
348

KRMPVQFL
349

LAAPLGLL
350

LAHG
351

LAHGL
352

LAHGLF
353

LAPLGLQRR
354

LARAG
355

LARAGI
356

LARAGL
357

LKAAPRWA
358

LKAAPRWF
359

LKAAPVWA
360

LKAAPVWF
361

LKGRSYYY
362

LLAPSHRA
363

LLEALRAL
364

LLESLRAL
365

LLLPAHGG
366

LLLPLLGS
367

LLNALRAL
368

LLNSLRAL
369

LLQALRAL
370

LLQSLRAL
371

LLSALRAL
372

LLSSLRAL
373

LNGRSDNH
374

LPAGLLL
375

LPAGLLLR
376

LPAHLVLL
377

LPAHLVLV
378

LPGGLSPW
379

LPSHLVLL
380

LPSHLVLV
381

LPTFV
382

LPTFVH
383

LPTFVHL
384

LRSGW
385

LSGR
386

LSGRS
387

LSGRSA
388

LSGRSALAHGLF
389

LSGRSAN
390

LSGRSANI
391

LSGRSANP
392

LSGRSD
393

LSGRSDD
394

LSGRSDDH
395

LSGRSDI
396

LSGRSDIH
397

LSGRSDN
398

LSGRSDNH
399

LSGRSDNH
400

LSGRSDNHGGAV
401

GLLAPP

LSGRSDNHGGSG
402

GSISSGLLSS

LSGRSDNHGGSG
403

GSQNQALRMA

LSGRSDNHGGVH
404

MPLGFLGP

LSGRSDNI
405

LSGRSDNP
406

LSGRSDQ
407

LSGRSDQH
408

LSGRSDT
409

LSGRSDTH
410

LSGRSDY
411

LSGRSDYH
412

LSGRSENH
413

LSGRSG
414

LSGRSGN
415

LSGRSGNH
416

LSGRSGNHGGSG
417

GSISSGLLSS

LSGRSGNHGGSG
418

GSQNQALRMA

LSGRSGNP
419

LSGRSVTQ
420

LSQARWRK
421

LTFPTYIF
422

LTFPTYWF
423

LTGRSDRH
424

LTGRSGA
425

LTGRSGA
426

LYAAPRWA
427

LYAAPRWF
428

LYAAPVWA
429

LYAAPVWF
430

LYGRSENN
431

MDAFLESS
432

MGLFSEAG
433

MGPWFM
434

MIAPVAYR
435

MLRSGW
436

MLRSGWR
437

MLRSGWRG
438

MLRSGWRL
439

MLRSGWRS
440

MTFPTYIF
441

MTFPTYWF
442

NHRIGRSDNHRR
443

NMPSFKLVTG
444

NTLSGRSENHSG
445

NTLSGRSGNHGS
446

NZPRVRLVLP
447

PAGLWLDP
448

PAGRR
449

PAGRRS
450

PAGRRSL
451

PASLWYTQ
452

PESRRWMP
453

PFHLSR
454

PHGFFQ
455

PLARAGI
456

PLARAGL
457

PLGL
458

PLGLAG
459

PLGLWA
460

PLGVRGK
461

PLTGRSGG
462

PLTGRSGGGGSS
463

PPLGR
464

PPPDMKLFPG
465

PPPEVRSFSV
466

PPPVLKLLEW
467

PPSIARSDNLAN
468

PQHRIVSF
469

PRFKIIGG
470

PRFRIIGG
471

PRPFVKSVDQ
472

PRQV
473

PRSF
474

PSPPVKMMPE
475

PTNGGSGGSS
476

PTNL
477

PTNLGSGGSS
478

PVGYTSSL
479

PVPRLKLIKD
480

PVQPIGPQ
481

QALAMSAI
482

QFQALRM
483

QGPMFKSLWD
484

QGRAITFI
485

QHQALRM
486

QNQALRIA
487

QNQALRM
488

QNQALRMA
489

QNQALRMAGGSGG
490

SLSGRSDNH

QNQALRMAGGSGG
491

SLSGRSGNH

QSRRVP
492

QSRRVPL
493

QSRRVPV
494

QTRRVP
495

QTRRVPL
496

QTRRVPV
497

QYIVSRSA
498

RALRAP
499

REPFMKSLPW
500

RFPLKV
501

RFPSLKSFPL
502

RFPYGVW
503

RFYRNQFF
504

RGPA
505

RGPAFNPM
506

RGPATPIM
507

RGPKLYW
508

RHLAKL
509

RIGRSDNH
510

RKMPNITV
511

RKSSIIIRMRDVVL
512

RKTVQHWW
513

RLGRSDNN
514

RMHLRSLG
515

RPLARAGI
516

RPLARAGL
517

RPLNGRSDNHKA
518

RPLNGRSDNHKK
519

RPLNGRSDNHKR
520

RPLNGRSDNHQA
521

RPLNGRSDNHQK
522

RPLNGRSDNHQR
523

RPLNGRSDNHRA
524

RPLNGRSDNHRK
525

RPLNGRSDNHRR
526

RPLSGRSDNHKA
527

RPLSGRSDNHKK
528

RPLSGRSDNHKR
529

RPLSGRSDNHQA
530

RPLSGRSDNHQK
531

RPLSGRSDNHQR
532

RPLSGRSDNHRA
533

RPLSGRSDNHRK
534

RPLSGRSDNHRR
535

RPSPMWAY
536

RRHDGLRA
537

RRHDGLRS
538

RSLVFAPI
539

RSPSRLKC
540

RVPKVKVMLD
541

SAGFSLPA
542

SAPAVESE
543

SAPYFRMMDM
544

SARGPSRW
545

SCGPPLGR
546

SCSPPLGR
547

SGGPLGVR
548

SGGPPLGR
549

SGPPLGR
550

SGRS
551

SGRSA
552

SGRSAN
553

SGRSANI
554

SGRSANP
555

SGRSANPRG
556

SGRSD
557

SGRSDD
558

SGRSDDH
559

SGRSDI
560

SGRSDIH
561

SGRSDN
562

SGRSDNI
563

SGRSDNP
564

SGRSDQ
565

SGRSDQH
566

SGRSDT
567

SGRSDTH
568

SGRSDY
569

SGRSDYH
570

SGRSG
571

SGRSGN
572

SGRSGNH
573

SGSPPLGR
574

SIARSDNL
575

SISSGLLSGRSDNI
576

SNPFKY
577

SPLPLRVP
578

SPLPLRVP
579

SPLTGRSG
580

SPPLGR
581

SRRVP
582

SRRVPL
583

SRRVPV
584

SSGPPLGR
585

SSPPLGR
586

SSRGPAYL
587

SSRHRRALD
588

SSSFDKGKYKKGD
589

DA

SSSFDKGKYKRGD
590

DA

SSSPPLGR
591

STFPFGMF
592

STVFHM
593

SVHHLI
594

SVSGLLSH
595

SVSGLLSS
596

SVSGLRSH
597

SVSGLRSS
598

TARG
599

TARGP
600

TARGPALAHGLF
601

TARGPS
602

TARGPSF
603

TARGPSFK
604

TARGPSW
605

TARGPSW
606

TARGPVPRQV
607

TFVH
608

TGLSGRSVTQTS
609

TGRGPSWV
610

TLRLGRSDNNKN
611

TLSGLRSP
612

TSGRSANP
613

TSGRSGNP
614

TSLSGRSANPRG
615

TSLSGRSGNPRG
616

TSSGLRSP
617

TSTSGRSANPRG
618

TSTSGRSANPRGGG
619

AVGLLAPP

TSTSGRSANPRGGG
620

VHMPLGFLGP

TSTSGRSGNPRG
621

TVSGLRSP
622

VAGRSMRP
623

VAPQLKSLVP
624

VAQFVLTE
625

VHMPLGFLGP
626

VHMPLGFLGPGGL
627

SGRSDNH

VHMPLGFLGPGGT
628

STSGRSANPRG

VLPELRSVFS
629

VLSKQMSF
630

VPAGRRS
631

VPAGRRSL
632

VPRQ
633

VPRQV
634

VSRSA
635

VVPEGRRS
636

WATPRPMR
637

WDHPISLL
638

XXQAR(A/V)X
639

YDPZVKVVLA
640

YGAGLGVV
641

YIVSRSA
642

YKKFVGSL
643

YVPRVKALEM
644

Examples of the CMs further include truncation variants of the aforementioned amino acid sequences that retain the recognition site for the corresponding protease. These include C-terminal and/or N-terminal truncation variants comprising at least 3 contiguous amino acids of the above-described amino acid sequences, or at least 4, or at least 5, or at least 6, or at least 7 amino acids of the foregoing amino acid sequences that retain a recognition site for a protease. In certain embodiments, the truncation variant of the above-described amino acid sequences is an amino acid sequence corresponding to any of the above, but that is C- and/or N-terminally truncated by 1 to about 10 amino acids, 1 to about 9 amino acids, 1 to about 8 amino acids, 1 to about 7 amino acids, 1 to about 6 amino acids, 1 to about 5 amino acids, 1 to about 4 amino acids, or 1 to about 3 amino acids, and which: (1) has at least three amino acid residues; and (2) retains a recognition site for a protease. In some of the foregoing embodiments, the truncated CM is an N-terminally truncated CM. In some embodiments, the truncated CM is a C-terminally truncated CM. In some embodiments, the truncated C is a C- and an N-terminally truncated CM.

In some embodiments, each of the CMs in the ACC may independently comprise a total of about 3 amino acids to about 25 amino acids. In some embodiments, each of the CMs in the ACC may independently comprise a total of about 3 amino acids to about 25 amino acids, about 3 amino acids to about 20 amino acids, about 3 amino acids to about 15 amino acids, about 3 amino acids to about 10 amino acids, about 3 amino acids to about 5 amino acids, about 5 amino acids to about 25 amino acids, about 5 amino acids to about 20 amino acids, about 5 amino acids to about 15 amino acids, about 5 amino acids to about 10 amino acids, about 10 amino acids to about 25 amino acids, about 10 amino acids to about 20 amino acids, about 10 amino acids to about 15 amino acids, about 15 amino acids to about 25 amino acids, about 15 amino acids to about 20 amino acids, or about 20 amino acids to about 25 amino acids.

In some embodiments, the ACC may comprise multiple CMs that comprise substrates for different proteases. In some embodiments, some or all of the CMs in the ACC comprise substrates for different proteases. In some embodiments, the CMs comprise substrates for the same protease.

Linkers

The monomer constructs may comprise one or more linkers between two components. In some embodiments, the first monomer can include a linker disposed between the CP1 and the CM1. In some embodiments, the CP1 and the CM1 directly abut each other in the first monomer. In some embodiments, the first monomer comprises a linker disposed between the CM1 and the SMM1. In some embodiments, the CM1 and the SMM1 directly abut each other in the first monomer. In some embodiments, the first monomer comprises a linker disposed between the CP1 and the CM4 (the CM coupling the CP1 and the AMM1). In some embodiments, the CP1 and the CM4 directly abut each other in the first monomer. In some embodiments, the first monomer comprises a linker disposed between the CM4 and the AMM1. In some embodiments, the CM4 and the AMM1 directly abut each other in the first monomer.

In some embodiments, the second monomer can include a linker disposed between the CP2 and the CM2. In some embodiments, the CP2 and the CM2 directly abut each other in the second monomer. In some embodiments, the second monomer comprises a linker disposed between the CM2 and the SMM2. In some embodiments the CM2 and the SMM2 directly abut each other in the second monomer. In some embodiments, the second monomer comprises a linker disposed between the CP2 and the CM5 (the CM coupling the CP2 and the AMM2). In some embodiments, the CP2 and the CM5 directly abut each other in the second monomer. In some embodiments, the second monomer comprises a linker disposed between the CM5 and the AMM2. In some embodiments, the CM5 and the AMM2 directly abut each other in the second monomer.

In some embodiments, the third monomer can include a linker disposed between the CP3 and the CM3. In some embodiments, the CP3 and the CM3 directly abut each other in the third monomer. In some embodiments, the third monomer comprises a linker disposed between the CM3 and the SMM3. In some embodiments, the CM3 and the SMM3 directly abut each other in the third monomer. In some embodiments, the third monomer comprises a linker disposed between the CP3 and the CM6 (the CM coupling the CP3 and the AMM3). In some embodiments, the CP3 and the CM6 directly abut each other in the third monomer. In some embodiments, the third monomer comprises a linker disposed between the CM6 and the AMM3. In some embodiments, the CM6 and the AMM3 directly abut each other in the third monomer.

In some embodiments, one or more linkers (e.g., flexible linkers) can be introduced into the activatable cytokine construct to provide flexibility at one or more of the junctions between domains, between moieties, between moieties and domains, or at any other junctions where a linker would be beneficial. In some embodiments, where the ACC is provided as a conformationally constrained construct, a flexible linker can be inserted to facilitate formation and maintenance of a structure in the uncleaved activatable cytokine construct. Any of the linkers described herein can provide the desired flexibility to facilitate the inhibition of the binding of a target (e.g., a receptor of a cytokine), or to facilitate cleavage of a CM by a protease. In some embodiments, linkers are included in the ACC that are all or partially flexible, such that the linker can include a flexible linker as well as one or more portions that confer less flexible structure to provide for a desired ACC. Some linkers may include cysteine residues, which may form disulfide bonds and reduce flexibility of the construct. A linker length may be determined by counting, in a N- to C-direction, the number of amino acids from the N-terminus of the linker adjacent to the C-terminal amino acid of the preceding component, to the C-terminus of the linker adjacent to the N-terminal amino acid of the following component (i.e., where the linker length does not include either the C-terminal amino acid of the preceding component or the N-terminal amino acid of the following component).

In some embodiments, a linker can include a total of about 1 amino acid to about 25 amino acids (e.g., about 1 amino acid to about 24 amino acids, about 1 amino acid to about 22 amino acids, about 1 amino acid to about 20 amino acids, about 1 amino acid to about 18 amino acids, about 1 amino acid to about 16 amino acids, about 1 amino acid to about 15 amino acids, about 1 amino acid to about 14 amino acids, about 1 amino acid to about 12 amino acids, about 1 amino acid to about 10 amino acids, about 1 amino acid to about 8 amino acids, about 1 amino acid to about 6 amino acids, about 1 amino acid to about 5 amino acids, about 1 amino acid to about 4 amino acids, about 1 amino acid to about 3 amino acids, about 1 amino acid to about 2 amino acids, about 2 amino acids to about 25 amino acids, about 2 amino acids to about 24 amino acids, about 2 amino acids to about 22 amino acids, about 2 amino acids to about 20 amino acids, about 2 amino acids to about 18 amino acids, about 2 amino acids to about 16 amino acids, about 2 amino acids to about 15 amino acids, about 2 amino acids to about 14 amino acids, about 2 amino acids to about 12 amino acids, about 2 amino acids to about 10 amino acids, about 2 amino acids to about 8 amino acids, about 2 amino acids to about 6 amino acids, about 2 amino acids to about 5 amino acids, about 2 amino acids to about 4 amino acids, about 2 amino acids to about 3 amino acids, about 4 amino acids to about 25 amino acids, about 4 amino acids to about 24 amino acids, about 4 amino acids to about 22 amino acids, about 4 amino acids to about 20 amino acids, about 4 amino acids to about 18 amino acids, about 4 amino acids to about 16 amino acids, about 4 amino acids to about 15 amino acids, about 4 amino acids to about 14 amino acids, about 4 amino acids to about 12 amino acids, about 4 amino acids to about 10 amino acids, about 4 amino acids to about 8 amino acids, about 4 amino acids to about 6 amino acids, about 4 amino acids to about 5 amino acids, about 5 amino acids to about 25 amino acids, about 5 amino acids to about 24 amino acids, about 5 amino acids to about 22 amino acids, about 5 amino acids to about 20 amino acids, about 5 amino acids to about 18 amino acids, about 5 amino acids to about 16 amino acids, about 5 amino acids to about 15 amino acids, about 5 amino acids to about 14 amino acids, about 5 amino acids to about 12 amino acids, about 5 amino acids to about 10 amino acids, about 5 amino acids to about 8 amino acids, about 5 amino acids to about 6 amino acids, about 6 amino acids to about 25 amino acids, about 6 amino acids to about 24 amino acids, about 6 amino acids to about 22 amino acids, about 6 amino acids to about 20 amino acids, about 6 amino acids to about 18 amino acids, about 6 amino acids to about 16 amino acids, about 6 amino acids to about 15 amino acids, about 6 amino acids to about 14 amino acids, about 6 amino acids to about 12 amino acids, about 6 amino acids to about 10 amino acids, about 6 amino acids to about 8 amino acids, about 8 amino acids to about 25 amino acids, about 8 amino acids to about 24 amino acids, about 8 amino acids to about 22 amino acids, about 8 amino acids to about 20 amino acids, about 8 amino acids to about 18 amino acids, about 8 amino acids to about 16 amino acids, about 8 amino acids to about 15 amino acids, about 8 amino acids to about 14 amino acids, about 8 amino acids to about 12 amino acids, about 8 amino acids to about 10 amino acids, about 10 amino acids to about 25 amino acids, about 10 amino acids to about 24 amino acids, about 10 amino acids to about 22 amino acids, about 10 amino acids to about 20 amino acids, about 10 amino acids to about 18 amino acids, about 10 amino acids to about 16 amino acids, about 10 amino acids to about 15 amino acids, about 10 amino acids to about 14 amino acids, about 10 amino acids to about 12 amino acids, about 12 amino acids to about 25 amino acids, about 12 amino acids to about 24 amino acids, about 12 amino acids to about 22 amino acids, about 12 amino acids to about 20 amino acids, about 12 amino acids to about 18 amino acids, about 12 amino acids to about 16 amino acids, about 12 amino acids to about 15 amino acids, about 12 amino acids to about 14 amino acids, about 14 amino acids to about 25 amino acids, about 14 amino acids to about 24 amino acids, about 14 amino acids to about 22 amino acids, about 14 amino acids to about 20 amino acids, about 14 amino acids to about 18 amino acids, about 14 amino acids to about 16 amino acids, about 14 amino acids to about 15 amino acids, about 15 amino acids to about 25 amino acids, about 15 amino acids to about 24 amino acids, about 15 amino acids to about 22 amino acids, about 15 amino acids to about 20 amino acids, about 15 amino acids to about 18 amino acids, about 15 amino acids to about 16 amino acids, about 16 amino acids to about 25 amino acids, about 16 amino acids to about 24 amino acids, about 16 amino acids to about 22 amino acids, about 16 amino acids to about 20 amino acids, about 16 amino acids to about 18 amino acids, about 18 amino acids to about 25 amino acids, about 18 amino acids to about 24 amino acids, about 18 amino acids to about 22 amino acids, about 18 amino acids to about 20 amino acids, about 20 amino acids to about 25 amino acids, about 20 amino acids to about 24 amino acids, about 20 amino acids to about 22 amino acids, about 22 amino acid to about 25 amino acids, about 22 amino acid to about 24 amino acids, or about 24 amino acid to about 25 amino acids).

In some embodiments of any of the ACCs described herein, the linker includes a total of about 1 amino acid, about 2 amino acids, about 3 amino acids, about 4 amino acids, about 5 amino acids, about 6 amino acids, about 7 amino acids, about 8 amino acids, about 9 amino acids, about 10 amino acids, about 11 amino acids, about 12 amino acids, about 13 amino acids, about 14 amino acids, about 15 amino acids, about 16 amino acids, about 17 amino acids, about 18 amino acids, about 19 amino acids, about 20 amino acids, about 21 amino acids, about 22 amino acids, about 23 amino acids, about 24 amino acids, or about 25 amino acids.

In some embodiments, a linker can be rich in glycine (Gly or G) residues. In some embodiments, the linker can be rich in serine (Ser or S) residues. In some embodiments, the linker can be rich in glycine and serine residues. In some embodiments, the linker has one or more glycine-serine residue pairs (GS) (e.g., 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 or more GS pairs). In some embodiments, the linker has one or more Gly-Gly-Gly-Ser (GGGS) sequences (e.g., 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 or more GGGS sequences). In some embodiments, the linker has one or more Gly-Gly-Gly-Gly-Ser (GGGGS) sequences (e.g., 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 or more GGGGS sequences). In some embodiments, the linker has one or more Gly-Gly-Ser-Gly (GGSG) sequences (e.g., 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 or more GGSG sequences).

In some embodiments of any of the ACCs described herein, a linker includes any one of or a combination of one or more of: (GS)n, (GGS)n, (GSGGS)n (SEQ ID NO: 645), (GGGGS)n (SEQ ID NO: 646), (GGGS)n (SEQ ID NO: 647), GGSG (SEQ ID NO: 648), GGSGG (SEQ ID NO: 649), GSGSG (SEQ ID NO: 650), GSGGG (SEQ ID NO: 651), GGGSG (SEQ ID NO: 652), GSSSG (SEQ ID NO: 653), GSSGGSGGSGG (SEQ ID NO: 654), GGGS (SEQ ID NO: 655), GGGSGGGS (SEQ ID NO: 656), GGGSGGGSGGGS (SEQ ID NO: 657), GGGGSGGGGSGGGGS (SEQ ID NO: 658), GGGGSGGGGSGGGGSGGGGS (SEQ ID NO: 659), GGGGSGGGGSGGGGSGGGGSGGGGS (SEQ ID NO: 660), GGGGSGGGGS (SEQ ID NO: 661), GGGGS (SEQ ID NO: 662), GS, GGGGSGS (SEQ ID NO: 663), GGGGSGGGGSGGGGSGS (SEQ ID NO: 664), GGSLDPKGGGGS (SEQ ID NO: 665), PKSCDKTHTCPPCPAPELLG (SEQ ID NO: 666), SKYGPPCPPCPAPEFLG (SEQ ID NO: 667), GKSSGSGSESKS (SEQ ID NO: 668), GSTSGSGKSSEGKG (SEQ ID NO: 669), GSTSGSGKSSEGSGSTKG (SEQ ID NO: 670), GSTSGSGKPGSGEGSTKG (SEQ ID NO: 671), and GSTSGSGKPGSSEGST (SEQ ID NO: 672), where n is an integer of one or more.

Non-limiting examples of linkers can include a sequence that is at least 70% identical (e.g., at least 72%, at least 74%, at least 75%, at least 76%, at least 78%, at least 80%, at least 82%, at least 84%, at least 85%, at least 86%, at least 88%, at least 90%, at least 92%, at least 94%, at least 95%, at least 96%, at least 97%, at least 98%, at least 99%, or 100% identical) to the exemplary linker sequence described herein.

In some embodiments, an ACC can include at least 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, or 20 linker sequence(s) (e.g., the same or different linker sequences of any of the exemplary linker sequences described herein or known in the art). In some embodiments, a linker comprises sulfo-SIAB, SMPB, and sulfo-SMPB, wherein the linkers react with primary amines sulfhydryls.

Additional Exemplary linker sequences are listed in the following Table 2:

TABLE 2

Exemplary linker sequences

SEQ

SEQ

SEQ

ID

ID

ID

Sequences
NO
Sequences
NO
Sequences
NO

(GSGGS)n
645
GKSSGSGSESKS
668
GGGS
655

n can be any integer

that is 1 or greater

(GGGS)n
647
GSTSGSGKSSEGKG
669
GSSGGSGGSGG
654

n can be any integer

that is 1 or greater

GGSG
648
GSTSGSGKSSEGSG
670
GGGSGGGS
656

STKG

GGSGG
649
GSTSGSGKPGSGEG
671
GGGSGGGSGGG
657

STKG

S

GSGSG
650
GSTSGSGKPGSSEG
672
GGGGSGGGGSG
658

ST

GGGS

GSGGG
651
GGGGSGGGGSGGG
660
(GGGGS)n
646

GSGGGGSGGGGS

n can be any

integer that is 1 or

greater

GGGSG
652
GGGGSGGGGS
661
GGGGSGS
663

GSSSG
653
PKSCDKTHTCPPCP
666
GGGGSGGGGSG
664

APELLG

GGGSGS

GSSGGS
673
SKYGPPCPPCPAPE
667
GGSLDPKGGGG
665

FLG

S

ESKY
674
GPQGTAGQ
676
YGAGLGW
677

SGGG
675
SGGGG
678

Conjugation to Agents

The ACCs may be conjugated with one or more agents, for example, a targeting moiety to facilitate delivery to a cell or tissue of interest, an agent (e.g., a therapeutic agent, an antineoplastic agent), a toxin, or a fragment thereof.

In some embodiments, the ACC can be conjugated to a cytotoxic agent, including, without limitation, a toxin (e.g., an enzymatically active toxin of bacterial, fungal, plant, or animal origin, or fragments thereof) or a radioactive isotope. In some embodiments of, the activatable cytokine construct can be conjugated to a cytotoxic agent including, without limitation, a toxin (e.g., an enzymatically active toxin of bacterial, fungal, plant, or animal origin, or fragments thereof), or a radioactive isotope.

Non-limiting exemplary cytotoxic agents that can be conjugated to any of the ACCs described herein include: dolastatins and derivatives thereof (e.g., auristatin E, AFP, monomethyl auristatin D (MMAD), monomethyl auristatin F (MMAF), monomethyl auristatin E (MMAE), desmethyl auristatin E (DMAE), auristatin F, desmethyl auristatin F (DMAF), dolastatin 16 (DmJ), dolastatin 16 (Dpv), auristatin derivatives (e.g., auristatin tyramine, auristatin quinolone), maytansinoids (e.g., DM-1, DM-4), maytansinoid derivatives, duocarmycin, alpha-amanitin, turbostatin, phenstatin, hydroxyphenstatin, spongistatin 5, spongistatin 7, halistatin 1, halistatin 2, halistatin 3, halocomstatin, pyrrolobenzimidazoles (PBI), cibrostatin6, doxaliform, cemadotin analogue (CemCH2-SH), Pseudomonas toxin A (PES8) variant, Pseudomonase toxin A (ZZ-PE38) variant, ZJ-101, anthracycline, doxorubicin, daunorubicin, bryostatin, camptothecin, 7-substituted campothecin, 10, 11-difluoromethylenedioxycamptothecin, combretastatins, debromoaplysiatoxin, KahaMide-F, discodermolide, and Ecteinascidins.

Non-limiting exemplary enzymatically active toxins that can be conjugated to any of the ACCs described herein include: diphtheria toxin, exotoxin A chain from Pseudomonas aeruginosa, ricin A chain, abrin A chain, modeccin A chain, alpha-sarcin, Aleuriies fordii proteins, dianfhin proteins, Phytoiaca Americana proteins (e.g., PAPI, PAPII, and PAP-8), Momordica charantia inhibitor, curcin, crotirs, Sapaonaria officinalis inhibitor, geionin, mitogeliin, restrictocin, phenomycin, neomycin, and tricothecenes.

Non-limiting exemplary anti-neoplastics that can be conjugated to any of the ACCs described herein include: adriamycin, cerubidine, bleomycin, alkeran, velban, oncovin, fluorouracil, methotrexate, thiotepa, bisantrene, novantrone, thioguanine, procarabizine, and cytarabine.

Non-limiting exemplary antivirals that can be conjugated to any of the ACCs described herein include: acyclovir, vira A, and symmetrel.

Non-limiting exemplary antifungals that can be conjugated to any of the ACCs described herein include: nystatin.

Non-limiting exemplary conjugatable detection reagents that can be conjugated to any of the ACCs described herein include: fluorescein and derivatives thereof, fluorescein isothiocyanate (FITC).

Non-limiting exemplary antibacterials that can be conjugated to any of the activatable cytokine constructs described herein include: aminoglycosides, streptomycin, neomycin, kanamycin, amikacin, gentamicin, and tobramycin.

Non-limiting exemplary 3beta,16beta,17alpha-trihydroxycholest-5-en-22-one 16-O-(2-O-4-methoxybenzoyl-beta-D-xylopyranosyl)-(1→3)-(2-O-acetyl-alpha-L-arabinopyranoside) (OSW-1) that can be conjugated to any of the activatable cytokine constructs described herein include: s-nitrobenzyloxycarbonyl derivatives of 06-benzylguanine, toposisomerase inhibitors, hemiasterlin, cephalotaxine, homoharringionine, pyrrol obenzodiazepine dimers (PBDs), functionalized pyrrolobenzodiazepenes, calcicheamicins, podophyiitoxins, taxanes, and vinca alkoids.

Non-limiting exemplary radiopharmaceuticals that can be conjugated to any of the activatable cytokine constructs described herein include: ¹²³I, ⁸⁹Zr, ¹²⁵I, ¹³¹I, ^99mTc, ²⁰¹Tl, ⁶²Cu, ¹⁸F, ⁶⁸Ga, ¹³N, ¹⁵O, ³⁸K, ⁸²Rb, ¹¹¹In, ¹³³Xe, ¹¹C, and ⁹⁹mTc (Technetium).

Non-limiting exemplary heavy metals that can be conjugated to any of the ACCs described herein include: barium, gold, and platinum.

Non-limiting exemplary anti-mycoplasmals that can be conjugated to any of the ACCs described herein include: tylosine, spectinomycin, streptomycin B, ampicillin, sulfanilamide, polymyxin, and chloramphenicol.

Those of ordinary skill in the art will recognize that a large variety of possible moieties can be conjugated to any of the activatable cytokine constructs described herein. Conjugation can include any chemical reaction that will bind the two molecules so long as the ACC and the other moiety retain their respective activities. Conjugation can include many chemical mechanisms, e.g., covalent binding, affinity binding, intercalation, coordinate binding, and complexation. In some embodiments, the preferred binding is covalent binding. Covalent binding can be achieved either by direct condensation of existing side chains or by the incorporation of external bridging molecules. Many bivalent or polyvalent linking agents are useful in conjugating any of the activatable cytokine constructs described herein. For example, conjugation can include organic compounds, such as thioesters, carbodiimides, succinimide esters, glutaraldehyde, diazobenzenes, and hexamethylene diamines. In some embodiments, the activatable cytokine construct can include, or otherwise introduce, one or more non-natural amino acid residues to provide suitable sites for conjugation.

In some embodiments of any of the ACCs described herein, an agent and/or conjugate is attached by disulfide bonds (e.g., disulfide bonds on a cysteine molecule) to the cytokine protein(s). Since many cancers naturally release high levels of glutathione, a reducing agent, glutathione present in the cancerous tissue microenvironment can reduce the disulfide bonds, and subsequently release the agent and/or the conjugate at the site of delivery.

In some embodiments of any of the ACCs described herein, when the conjugate binds to its target in the presence of complement within the target site (e.g., diseased tissue (e.g., cancerous tissue)), the amide or ester bond attaching the conjugate and/or agent to the linker is cleaved, resulting in the release of the conjugate and/or agent in its active form. These conjugates and/or agents when administered to a subject, will accomplish delivery and release of the conjugate and/or the agent at the target site (e.g., diseased tissue (e.g., cancerous tissue)). These conjugates and/or agents are particularly effective for the in vivo delivery of any of the conjugates and/or agents described herein.

In some embodiments, the linker is not cleavable by enzymes of the complement system. For example, the conjugate and/or agent is released without complement activation since complement activation ultimately lyses the target cell. In such embodiments, the conjugate and/or agent is to be delivered to the target cell (e.g., hormones, enzymes, corticosteroids, neurotransmitters, or genes). Furthermore, the linker is mildly susceptible to cleavage by serum proteases, and the conjugate and/or agent is released slowly at the target site.

In some embodiments of any of the ACCs described herein, the conjugate and/or agent is designed such that the conjugate and/or agent is delivered to the target site (e.g., disease tissue (e.g., cancerous tissue)) but the conjugate and/or agent is not released.

In some embodiments of any of the ACCs described herein, the conjugate and/or agent is attached to a cytokine protein either directly or via a non-cleavable linker. Exemplary non-cleavable linkers include amino acids (e.g., D-amino acids), peptides, or other organic compounds that may be modified to include functional groups that can subsequently be utilized in attachment to cytokines by methods described herein.

In some embodiments of any of the ACCs described herein, an ACC includes at least one point of conjugation for an agent. In some embodiments, all possible points of conjugation are available for conjugation to an agent. In some embodiments, the one or more points of conjugation include, without limitation, sulfur atoms involved in disulfide bonds, sulfur atoms involved in interchain disulfide bonds, sulfur atoms involved in interchain sulfide bonds but not sulfur atoms involved in intrachain disulfide bonds, and/or sulfur atoms of cysteine or other amino acid residues containing a sulfur atom. In such cases, residues may occur naturally in the protein construct structure or may be incorporated into the protein construct using methods including, without limitation, site-directed mutagenesis, chemical conversion, or mis-incorporation of non-natural amino acids.

This disclosure also provides methods and materials for preparing an ACC for conjugation. In some embodiments of any of the ACCs described herein, an ACC is modified to include one or more interchain disulfide bonds. For example, disulfide bonds in the ACC can undergo reduction following exposure to a reducing agent such as, without limitation, TCEP, DTT, or β-mercaptoethanol. In some cases, the reduction of the disulfide bonds is only partial. As used herein, the term partial reduction refers to situations where an ACC is contacted with a reducing agent and a fraction of all possible sites of conjugation undergo reduction (e.g., not all disulfide bonds are reduced). In some embodiments, an activatable cytokine construct is partially reduced following contact with a reducing agent if less than 99%, (e.g., less than 98%, 97%, 96%, 95%, 90%, 85%, 80%, 75%, 70%, 65%, 60%, 55%, 50% 45%, 40%, 35% 30%, 5% 20%, 15%, 10% or less than 5%) of all possible sites of conjugation are reduced. In some embodiments, the ACC having a reduction in one or more interchain disulfide bonds is conjugated to a drug reactive with free thiols.

This disclosure also provides methods and materials for conjugating a therapeutic agent to a particular location on an ACC. In some embodiments of any of the ACC described herein, an ACC is modified so that the therapeutic agents can be conjugated to the ACC at particular locations on the ACC. For example, an ACC can be partially reduced in a manner that facilitates conjugation to the ACC. In such cases, partial reduction of the ACC occurs in a manner that conjugation sites in the ACC are not reduced. In some embodiments, the conjugation site(s) on the ACC are selected to facilitate conjugation of an agent at a particular location on the protein construct. Various factors can influence the “level of reduction” of the ACC upon treatment with a reducing agent. For example, without limitation, the ratio of reducing agent to ACC, length of incubation, incubation temperature, and/or pH of the reducing reaction solution can require optimization in order to achieve partial reduction of the ACC with the methods and materials described herein. Any appropriate combination of factors (e.g., ratio of reducing agent to ACC, the length and temperature of incubation with reducing agent, and/or pH of reducing agent) can be used to achieve partial reduction of the ACC (e.g., general reduction of possible conjugation sites or reduction at specific conjugation sites).

An effective ratio of reducing agent to ACC can be any ratio that at least partially reduces the ACC in a manner that allows conjugation to an agent (e.g., general reduction of possible conjugation sites or reduction at specific conjugation sites). In some embodiments, the ratio of reducing agent to ACC will be in a range from about 20:1 to 1:1, from about 10:1 to 1:1, from about 9:1 to 1:1, from about 8:1 to 1:1, from about 7:1 to 1:1, from about 6:1 to 1:1, from about 5:1 to 1:1, from about 4:1 to 1:1, from about 3:1 to 1:1, from about 2:1 to 1:1, from about 20:1 to 1:1.5, from about 10:1 to 1:1.5, from about 9:1 to 1:1.5, from about 8:1 to 1:1.5, from about 7:1 to 1:1.5, from about 6:1 to 1:1.5, from about 5:1 to 1:1.5, from about 4:1 to 1:1.5, from about 3:1 to 1:1.5, from about 2:1 to 1:1.5, from about 1.5:1 to 1:1.5, or from about 1:1 to 1:1.5. In some embodiments, the ratio is in a range of from about 5:1 to 1:1. In some embodiments, the ratio is in a range of from about 5:1 to 1.5:1. In some embodiments, the ratio is in a range of from about 4:1 to 1:1. In some embodiments, the ratio is in a range from about 4:1 to 1.5:1. In some embodiments, the ratio is in a range from about 8:1 to about 1:1. In some embodiments, the ratio is in a range of from about 2.5:1 to 1:1.

An effective incubation time and temperature for treating an ACC with a reducing agent can be any time and temperature that at least partially reduces the ACC in a manner that allows conjugation of an agent to an ACC (e.g., general reduction of possible conjugation sites or reduction at specific conjugation sites). In some embodiments, the incubation time and temperature for treating an ACC will be in a range from about 1 hour at 37° C. to about 12 hours at 37° C. (or any subranges therein).

An effective pH for a reduction reaction for treating an ACC with a reducing agent can be any pH that at least partially reduces the ACC in a manner that allows conjugation of the ACC to an agent (e.g., general reduction of possible conjugation sites or reduction at specific conjugation sites).

When a partially-reduced ACC is contacted with an agent containing thiols, the agent can conjugate to the interchain thiols in the ACC. An agent can be modified in a manner to include thiols using a thiol-containing reagent (e.g., cysteine or N-acetyl cysteine). For example, the ACC can be partially reduced following incubation with reducing agent (e.g., TEPC) for about 1 hour at about 37° C. at a desired ratio of reducing agent to ACC. An effective ratio of reducing agent to ACC can be any ratio that partially reduces at least two interchain disulfide bonds located in the ACC in a manner that allows conjugation of a thiol-containing agent (e.g., general reduction of possible conjugation sites or reduction at specific conjugation sites).

In some embodiments of any of the ACCs described herein, an ACC is reduced by a reducing agent in a manner that avoids reducing any intrachain disulfide bonds. In some embodiments of any of the ACCs described herein, an ACC is reduced by a reducing agent in a manner that avoids reducing any intrachain disulfide bonds and reduces at least one interchain disulfide bond.

In some embodiments of any of the ACCs described herein, the ACC can also include an agent conjugated to the ACC. In some embodiments, the conjugated agent is a therapeutic agent.

In some embodiments, the agent (e.g., agent conjugated to an activatable cytokine construct) is a detectable moiety such as, for example, a label or other marker. For example, the agent is or includes a radiolabeled amino acid, one or more biotinyl moieties that can be detected by marked avidin (e.g., streptavidin containing a fluorescent marker or enzymatic activity that can be detected by optical or calorimetric methods), one or more radioisotopes or radionuclides, one or more fluorescent labels, one or more enzymatic labels, and/or one or more chemiluminescent agents. In some embodiments, detectable moieties are attached by spacer molecules.

In some embodiments, the agent (e.g., cytotoxic agent conjugated to an activatable cytokine construct) is linked to the ACC using a carbohydrate moiety, sulfhydryl group, amino group, or carboxylate group.

In some embodiments, the agent (e.g., cytotoxic agent conjugated to an activatable cytokine construct) is conjugated to the ACC via a conjugating moiety. A conjugating moiety may comprise linker(s) and CM(s) described herein, as well as other type of molecules. In some embodiments, the agent (e.g., cytotoxic agent conjugated to an activatable cytokine construct) is conjugated to a cysteine or a lysine in the ACC. In some embodiments, the agent (e.g., cytotoxic agent conjugated to an activatable cytokine construct) is conjugated to another residue of the ACC, such as those residues disclosed herein. In some embodiments, the conjugating moiety is a thiol-containing conjugating moiety.

Those of ordinary skill in the art will recognize that a large variety of possible moieties can be coupled to the ACCs of the disclosure. (See, for example, “Conjugate Vaccines”, Contributions to Microbiology and Immunology, J. M. Cruse and R. E. Lewis, Jr (eds), Carger Press, New York, (1989), the entire contents of which are incorporated herein by reference). In general, an effective conjugation of an agent (e.g., cytotoxic agent) to an ACC can be accomplished by any chemical reaction that will bind the agent to the ACC while also allowing the agent and the ACC to retain functionality.

In some embodiments, a variety of bifunctional protein-coupling agents can be used to conjugate the agent to the ACC including, without limitation, N-succinimidyl-3-(2-pyridyldithiol) propionate (SPDP), iminothiolane (IT), bifunctional derivatives of imidoesters (e.g., dimethyl adipimidate HCL), active esters (e.g., disuccinimidyl suberate), aldehydes (e.g., glutareldehyde), bis-azido compounds (e.g., bis (p-azidobenzoyl) hexanediamine), bis-diazonium derivatives (e.g., bis-(p-diazoniumbenzoyl)-ethylenediamine), diisocyanates (e.g., tolyene 2,6-diisocyanate), and bis-active fluorine compounds (e.g., 1,5-difluoro-2,4-dinitrobenzene). For example, a ricin immunotoxin can be prepared as described in Vitetta et al., Science 238: 1098 (1987). In some embodiments, a carbon-14-labeled 1-isothiocyanatobenzyl-3-methyldiethylene triaminepentaacetic acid (MX-DTPA) chelating agent can be used to conjugate a radionucleotide to the ACC. (See, e.g., WO94/11026).

Examples of conjugating moieties are described in the literature. (See, for example, Ramakrishnan, S. et al., Cancer Res. 44:201-208 (1984) describing use of MBS (M-maleimidobenzoyl-N-hydroxysuccinimide ester). See also, U.S. Pat. No. 5,030,719, describing use of halogenated acetyl hydrazide derivative coupled to an ACC by way of an oligopeptide linker. In some embodiments, suitable conjugating moieties include: (i) EDC (1-ethyl-3-(3-dimethylamino-propyl) carbodiimide hydrochloride; (ii) SMPT (4-succinimidyloxycarbonyl-alpha-methyl-alpha-(2-pridyl-dithio)-toluene (Pierce Chem. Co., Cat. (21558G); (iii) SPDP (succinimidyl-6 [3-(2-pyridyldithio) propionamido] hexanoate (Pierce Chem. Co., Cat #21651G); (iv) Sulfo-LC-SPDP (sulfosuccinimidyl 6 [3-(2-pyridyldithio)-propianamide] hexanoate (Pierce Chem. Co. Cat. #2165-G); and (v) sulfo-NHS (N-hydroxysulfo-succinimide: Pierce Chem. Co., Cat. #24510) conjugated to EDC. Additional conjugating moieties include SMCC, sulfo-SMCC, SPDB, or sulfo-SPDB.

The conjugating moieties described above contain components that have different attributes, thus leading to conjugates with differing physio-chemical properties. For example, sulfo-NHS esters of alkyl carboxylates are more stable than sulfo-NHS esters of aromatic carboxylates. NHS-ester containing conjugating moieties are less soluble than sulfo-NHS esters. Further, the conjugating moieties SMPT contains a sterically-hindered disulfide bond, and can form conjugates with increased stability. Disulfide linkages, are in general, less stable than other linkages because the disulfide linkage is cleaved in vitro, resulting in less conjugate available. Sulfo-NHS, in particular, can enhance the stability of carbodimide couplings. Carbodimide couplings (such as EDC) when used in conjunction with sulfo-NHS, forms esters that are more resistant to hydrolysis than the carbodimide coupling reaction alone.

In some embodiments of any of the ACCs, an agent can be conjugated to the ACC using a modified amino acid sequence included in the amino acid sequence of the ACC. By inserting conjugation-enabled amino acids at specific locations within the amino acid sequence of the ACC, the protein construct can be designed for controlled placement and/or dosage of the conjugated agent (e.g., cytotoxic agent). For example, the ACC can be modified to include a cysteine amino acid residue at positions on the first monomer, the second monomer, and/or the third monomer that provide reactive thiol groups and does not negatively impact protein folding and/or assembly and does not alter the binding of cytokine to its binding partners. In some embodiments, the ACC can be modified to include one or more non-natural amino acid residues within the amino acid sequence of the ACC to provide suitable sites for conjugation. In some embodiments, the ACC can be modified to include enzymatically activatable peptide sequences within the amino acid sequence of the ACC.

Nucleic Acids

Provided herein are nucleic acids including sequences that encode the first monomer construct (or the protein portion of the first monomer construct) (e.g., any of the first monomers constructs described herein), the second monomer construct (or the protein portion of the second monomer construct) (e.g., any of the second monomer constructs described herein), and the third monomer construct (or the protein portion of the third monomer construct) (e.g., any of the third monomer constructs described herein) of any of the ACCs described herein. In some embodiments, a set of nucleic acids together encode the first monomer construct (or the protein portion of the first monomer construct), the second monomer construct (or the protein portion of the second monomer construct), and the third monomer construct (or the protein portion of the third monomer construct). In some embodiments, the nucleic acid sequence encoding the first monomer construct (or the protein portion of the first monomer construct) is at least 70% identical (e.g., at least 72% identical, at least 74% identical, at least 76% identical, at least 78% identical, at least 80% identical, at least 82% identical, at least 84% identical, at least 86% identical, at least 88% identical, at least 90% identical, at least 92% identical, at least 94% identical, at least 96% identical, at least 98% identical, at least 99% identical, or 100% identical) to the nucleic acid sequence encoding the second monomer construct (or the protein portion of the second monomer construct). In some embodiments, the nucleic acid sequence encoding the first monomer construct (or the protein portion of the first monomer construct) is at least 70% identical (e.g., at least 72% identical, at least 74% identical, at least 76% identical, at least 78% identical, at least 80% identical, at least 82% identical, at least 84% identical, at least 86% identical, at least 88% identical, at least 90% identical, at least 92% identical, at least 94% identical, at least 96% identical, at least 98% identical, at least 99% identical, or 100% identical) to the nucleic acid sequence encoding the third monomer construct (or the protein portion of the third monomer construct). In some embodiments, the nucleic acid sequence encoding the second monomer construct (or the protein portion of the second monomer construct) is at least 70% identical (e.g., at least 72% identical, at least 74% identical, at least 76% identical, at least 78% identical, at least 80% identical, at least 82% identical, at least 84% identical, at least 86% identical, at least 88% identical, at least 90% identical, at least 92% identical, at least 94% identical, at least 96% identical, at least 98% identical, at least 99% identical, or 100% identical) to the nucleic acid sequence encoding the third monomer construct (or the protein portion of the third monomer construct).

Vectors

Provided herein are vectors and sets of vectors including any of the nucleic acids described herein. One skilled in the art will be capable of selecting suitable vectors or sets of vectors (e.g., expression vectors) for making any of the ACCs described herein, and using the vectors or sets of vectors to express any of the ACCs described herein. For example, in selecting a vector or a set of vectors, the cell must be considered because the vector(s) may need to be able to integrate into a chromosome of the cell and/or replicate in it. Exemplary vectors that can be used to produce an ACC are also described below.

As used herein, the term “vector” refers to a polynucleotide capable of inducing the expression of a recombinant protein (e.g., a first or second monomer) in a cell (e.g., any of the cells described herein). A “vector” is able to deliver nucleic acids and fragments thereof into a host cell, and includes regulatory sequences (e.g., promoter, enhancer, poly(A) signal). Exogenous polynucleotides may be inserted into the expression vector in order to be expressed. The term “vector” also includes artificial chromosomes, plasmids, retroviruses, and baculovirus vectors.

Methods for constructing suitable vectors that include any of the nucleic acids described herein, and suitable for transforming cells (e.g., mammalian cells) are well-known in the art. See, e.g., Sambrook et al., Eds. “Molecular Cloning: A Laboratory Manual,” 2^ndEd., Cold Spring Harbor Press, 1989 and Ausubel et al., Eds. “Current Protocols in Molecular Biology,” Current Protocols, 1993.

Non-limiting examples of vectors include plasmids, transposons, cosmids, and viral vectors (e.g., any adenoviral vectors (e.g., pSV or pCMV vectors), adeno-associated virus (AAV) vectors, lentivirus vectors, and retroviral vectors), and any Gateway® vectors. A vector can, for example, include sufficient cis-acting elements for expression; other elements for expression can be supplied by the host mammalian cell or in an in vitro expression system. Skilled practitioners will be capable of selecting suitable vectors and mammalian cells for making any of the ACCs described herein.

In some embodiments of any of the ACCs described herein, the ACC may be made biosynthetically using recombinant DNA technology and expression in eukaryotic or prokaryotic species.

In some embodiments, the vector includes a nucleic acid encoding the first monomer and the second monomer of any of the ACCs described herein. In some embodiments, the vector is an expression vector.

In some embodiments, a set of vectors together include a set of nucleic acids that together encode the first, the second, and the third monomer constructs of any of the ACCs described herein. In some embodiments, the pair of vectors is a set of expression vectors.

Cells

Also provided herein are host cells including any of the vector or sets of vectors described herein including any of the nucleic acids described herein.

Any of the ACCs described herein can be produced by any cell (e.g., a mammalian cell). In some embodiments, a host cell is a mammalian cell (e.g., a human cell), a rodent cell (e.g., a mouse cell, a rat cell, a hamster cell, or a guinea pig cell), or a non-human primate cell.

Methods of introducing nucleic acids and vectors (e.g., any of the vectors or any of the sets of vectors described herein) into a cell are known in the art. Non-limiting examples of methods that can be used to introducing a nucleic acid into a cell include: lipofection, transfection, calcium phosphate transfection, cationic polymer transfection, viral transduction (e.g., adenoviral transduction, lentiviral transduction), nanoparticle transfection, and electroporation.

In some embodiments, the introducing step includes introducing into a cell a vector (e.g., any of the vectors or sets of vectors described herein) including a nucleic acid encoding the monomers that make up any of the ACCs described herein.

In some embodiments of any of the methods described herein, the cell can be a eukaryotic cell. As used herein, the term “eukaryotic cell” refers to a cell having a distinct, membrane-bound nucleus. Such cells may include, for example, mammalian (e.g., rodent, non-human primate, or human), insect, fungal, or plant cells. In some embodiments, the eukaryotic cell is a yeast cell, such as Saccharomyces cerevisiae. In some embodiments, the eukaryotic cell is a higher eukaryote, such as mammalian, avian, plant, or insect cells. Non-limiting examples of mammalian cells include Chinese hamster ovary (CHO) cells and human embryonic kidney cells (e.g., HEK293 cells).

In some embodiments, the cell contains the nucleic acid encoding the first monomer and the second monomer of any one of the ACCs described herein. In some embodiments, the cell contains the pair of nucleic acids that together encode the first monomer and the second monomer of any of the ACCs described herein.

Methods of Producing Activatable Cytokine Constructs

Provided herein are methods of producing any of the ACCs described herein that include: (a) culturing any of the recombinant host cells described herein in a liquid culture medium under conditions sufficient to produce the ACC; and (b) recovering the ACC from the host cell and/or the liquid culture medium.

Methods of culturing cells are well known in the art. Cells can be maintained in vitro under conditions that favor cell proliferation, cell differentiation and cell growth. For example, cells can be cultured by contacting a cell (e.g., any of the cells described herein) with a cell culture medium that includes the necessary growth factors and supplements sufficient to support cell viability and growth.

In some embodiments of any of the methods described herein, the method further includes isolating the recovered ACC. Non-limiting examples of methods of isolation include: ammonium sulfate precipitation, polyethylene glycol precipitation, size exclusion chromatography, ligand-affinity chromatography, ion-exchange chromatography (e.g., anion or cation), and hydrophobic interaction chromatography.

In some embodiments of any of the methods described herein, the method further includes formulating the isolated ACC into a pharmaceutical composition. Various formulations are known in the art and are described herein. Any of the isolated ACCs described herein can be formulated for any route of administration (e.g., intravenous, intratumoral, subcutaneous, intradermal, oral (e.g., inhalation), transdermal (e.g., topical), transmucosal, or intramuscular).

Also provided herein are ACCs produced by any of the methods described herein. Also provided are compositions (e.g., pharmaceutical compositions) that include any of the ACCs produced by any of the methods described herein. Also provided herein are kits that include at least one dose of any of the compositions (e.g., pharmaceutical compositions) described herein.

In some embodiments, the ACCs may comprise one or more tags that can be for purification, isolation, and/or detection of the ACC. Examples of such tags include affinity tags, such as His tag (e.g., 6×-His (hexahistidine) tag), FLAG tag, c-Myc tag, Glutathione-S-transferase (GST) tag, Maltose-Binding Protein (MBP) tag, Calmodulin-Binding Protein (CBP) tag, and Streptavidin/Biotin-Based tag. In these chases, the ACCs may be isolated or purified using the tag(s). In some examples, the tags may be removed from the ACCs.

In some embodiments, the cells used in the production process can produce a protein portion of the first, the second, and the third monomer constructs (e.g., with one or more affinity tags). The monomers may then associate non-covalently to form a trimer. In cases where the three monomers are the same, the cell may produce the monomer construct (e.g., with one or more affinity tags). The monomer construct may then associate non-covalently to form a homotrimer.

ACCs expressed in cells herein may be purified. The purification may be performed using an affinity column, e.g., an HSA-affinity column, or a streptavidin-affinity column, or other columns compatible with the tags described above. The sample from the affinity column may be further purified by other chromatography technology, e.g., size exclusion chromatography (SEC). The purified ACCs may have a purity of at least 80%, 90%, 95%, or 99%.

Methods of Treatment

Provided herein are methods of treating a disease (e.g., a cancer (e.g., any of the cancers described herein)) in a subject including administering a therapeutically effective amount of any of the ACCs, the nucleic acids, vectors, compositions comprising the ACCs, nucleic acids, and/or the vectors described herein to the subject.

As used herein, the term “subject” refers to any organism such as a mammal. In some embodiments, the subject is a feline (e.g., a cat), a canine (e.g., a dog), an equine (e.g., a horse), a rabbit, a pig, a rodent (e.g., a mouse, a rat, a hamster or a guinea pig), a non-human primate (e.g., a simian (e.g., a monkey (e.g., a baboon, a marmoset), or an ape (e.g., a chimpanzee, a gorilla, an orangutan, or a gibbon)), or a human. In some embodiments, the subject is a human.

In some embodiments, the subject has been previously identified or diagnosed as having the disease (e.g., cancer (e.g., any of the cancers described herein)).

As used herein, the term “treat” includes reducing the severity, frequency or the number of one or more (e.g., 1, 2, 3, 4, or 5) symptoms or signs of a disease (e.g., a cancer (e.g., any of the cancers described herein)) in the subject (e.g., any of the subjects described herein). In some embodiments where the disease is cancer, treating results in reducing cancer growth, inhibiting cancer progression, inhibiting cancer metastasis, or reducing the risk of cancer recurrence in a subject having cancer.

In some embodiments of any of the methods described herein, the disease is a cancer. Also provided herein are methods of treating a subject in need thereof (e.g., any of the exemplary subjects described herein or known in the art) that include administering to the subject a therapeutically effective amount of any of the ACCs described herein or any of the compositions (e.g., pharmaceutical compositions) described herein.

In some embodiments of these methods, the subject has been identified or diagnosed as having a cancer. Non-limiting examples of cancer include: solid tumor, hematological tumor, sarcoma, osteosarcoma, glioblastoma, neuroblastoma, melanoma, rhabdomyosarcoma, Ewing sarcoma, osteosarcoma, B-cell neoplasms, multiple myeloma, a lymphoma (e.g., B-cell lymphoma, B-cell non-Hodgkin's lymphoma, Hodgkin's lymphoma, cutaneous T-cell lymphoma), a leukemia (e.g., hairy cell leukemia, chronic lymphocytic leukemia (CLL), acute myeloid leukemia (AML), chronic myeloid leukemia (CML), acute lymphocytic leukemia (ALL)), myelodysplastic syndromes (MDS), Kaposi sarcoma, retinoblastoma, stomach cancer, urothelial carcinoma, lung cancer, renal cell carcinoma, gastric and esophageal cancer, pancreatic cancer, prostate cancer, brain cancer, colon cancer, bone cancer, lung cancer, breast cancer, colorectal cancer, ovarian cancer, nasopharyngeal adenocarcimoa, non-small cell lung carcinoma (NSCLC), squamous cell head and neck carcinoma, endometrial cancer, bladder cancer, cervical cancer, liver cancer, and hepatocellular carcinoma. In some embodiments, the cancer is a lymphoma. In some embodiments, the lymphoma is Burkitt's lymphoma. In some aspects, the subject has been identified or diagnosed as having familial cancer syndromes such as L1 Fraumeni Syndrome, Familial Breast-Ovarian Cancer (BRCA1 or BRAC2 mutations) Syndromes, and others. The disclosed methods are also useful in treating non-solid cancers. Exemplary solid tumors include malignancies (e.g., sarcomas, adenocarcinomas, and carcinomas) of the various organ systems, such as those of lung, breast, lymphoid, gastrointestinal (e.g., colon), and genitourinary (e.g., renal, urothelial, or testicular tumors) tracts, pharynx, prostate, and ovary. Exemplary adenocarcinomas include colorectal cancers, renal-cell carcinoma, liver cancer, non-small cell carcinoma of the lung, and cancer of the small intestine.

Exemplary cancers described by the National Cancer Institute include: Acute Lymphoblastic Leukemia, Adult; Acute Lymphoblastic Leukemia, Childhood; Acute Myeloid Leukemia, Adult; Adrenocortical Carcinoma; Adrenocortical Carcinoma, Childhood; AIDS-Related Lymphoma; AIDS-Related Malignancies; Anal Cancer; Astrocytoma, Childhood Cerebellar; Astrocytoma, Childhood Cerebral; Bile Duct Cancer, Extrahepatic; Bladder Cancer; Bladder Cancer, Childhood; Bone Cancer, Osteosarcoma/Malignant Fibrous Histiocytoma; Brain Stem Glioma, Childhood; Brain Tumor, Adult; Brain Tumor, Brain Stem Glioma, Childhood; Brain Tumor, Cerebellar Astrocytoma, Childhood; Brain Tumor, Cerebral Astrocytoma/Malignant Glioma, Childhood; Brain Tumor, Ependymoma, Childhood; Brain Tumor, Medulloblastoma, Childhood; Brain Tumor, Supratentorial Primitive Neuroectodermal Tumors, Childhood; Brain Tumor, Visual Pathway and Hypothalamic Glioma, Childhood; Brain Tumor, Childhood (Other); Breast Cancer; Breast Cancer and Pregnancy; Breast Cancer, Childhood; Breast Cancer, Male; Bronchial Adenomas/Carcinoids, Childhood; Carcinoid Tumor, Childhood; Carcinoid Tumor, Gastrointestinal; Carcinoma, Adrenocortical; Carcinoma, Islet Cell; Carcinoma of Unknown Primary; Central Nervous System Lymphoma, Primary; Cerebellar Astrocytoma, Childhood; Cerebral Astrocytoma/Malignant Glioma, Childhood; Cervical Cancer; Childhood Cancers; Chronic Lymphocytic Leukemia; Chronic Myelogenous Leukemia; Chronic Myeloproliferative Disorders; Clear Cell Sarcoma of Tendon Sheaths; Colon Cancer; Colorectal Cancer, Childhood; Cutaneous T-Cell Lymphoma; Endometrial Cancer; Ependymoma, Childhood; Epithelial Cancer, Ovarian; Esophageal Cancer; Esophageal Cancer, Childhood; Ewing's Family of Tumors; Extracranial Germ Cell Tumor, Childhood; Extragonadal Germ Cell Tumor; Extrahepatic Bile Duct Cancer; Eye Cancer, Intraocular Melanoma; Eye Cancer, Retinoblastoma; Gallbladder Cancer; Gastric (Stomach) Cancer; Gastric (Stomach) Cancer, Childhood; Gastrointestinal Carcinoid Tumor; Germ Cell Tumor, Extracranial, Childhood; Germ Cell Tumor, Extragonadal; Germ Cell Tumor, Ovarian; Gestational Trophoblastic Tumor; Glioma, Childhood Brain Stem; Glioma, Childhood Visual Pathway and Hypothalamic; Hairy Cell Leukemia; Head and Neck Cancer; Hepatocellular (Liver) Cancer, Adult (Primary); Hepatocellular (Liver) Cancer, Childhood (Primary); Hodgkin's Lymphoma, Adult; Hodgkin's Lymphoma, Childhood; Hodgkin's Lymphoma During Pregnancy; Hypopharyngeal Cancer; Hypothalamic and Visual Pathway Glioma, Childhood; Intraocular Melanoma; Islet Cell Carcinoma (Endocrine Pancreas); Kaposi's Sarcoma; Kidney Cancer; Laryngeal Cancer; Laryngeal Cancer, Childhood; Leukemia, Acute Lymphoblastic, Adult; Leukemia, Acute Lymphoblastic, Childhood; Leukemia, Acute Myeloid, Adult; Leukemia, Acute Myeloid, Childhood; Leukemia, Chronic Lymphocytic; Leukemia, Chronic Myelogenous; Leukemia, Hairy Cell; Lip and Oral Cavity Cancer; Liver Cancer, Adult (Primary); Liver Cancer, Childhood (Primary); Lung Cancer, Non-Small Cell; Lung Cancer, Small Cell; Lymphoblastic Leukemia, Adult Acute; Lymphoblastic Leukemia, Childhood Acute; Lymphocytic Leukemia, Chronic; Lymphoma, AIDS-Related; Lymphoma, Central Nervous System (Primary); Lymphoma, Cutaneous T-Cell; Lymphoma, Hodgkin's, Adult; Lymphoma, Hodgkin's, Childhood; Lymphoma, Hodgkin's During Pregnancy; Lymphoma, Non-Hodgkin's, Adult; Lymphoma, Non-Hodgkin's, Childhood; Lymphoma, Non-Hodgkin's During Pregnancy; Lymphoma, Primary Central Nervous System; Macroglobulinemia, Waldenstrom's; Male Breast Cancer; Malignant Mesothelioma, Adult; Malignant Mesothelioma, Childhood; Malignant Thymoma; Medulloblastoma, Childhood; Melanoma; Melanoma, Intraocular; Merkel Cell Carcinoma; Mesothelioma, Malignant; Metastatic Squamous Neck Cancer with Occult Primary; Multiple Endocrine Neoplasia Syndrome, Childhood; Multiple Myeloma/Plasma Cell Neoplasm; Mycosis Fungoides; Myelodysplastic Syndromes; Myelogenous Leukemia, Chronic; Myeloid Leukemia, Childhood Acute; Myeloma, Multiple; Myeloproliferative Disorders, Chronic; Nasal Cavity and Paranasal Sinus Cancer; Nasopharyngeal Cancer; Nasopharyngeal Cancer, Childhood; Neuroblastoma; Non-Hodgkin's Lymphoma, Adult; Non-Hodgkin's Lymphoma, Childhood; Non-Hodgkin's Lymphoma During Pregnancy; Non-Small Cell Lung Cancer; Oral Cancer, Childhood; Oral Cavity and Lip Cancer; Oropharyngeal Cancer; Osteosarcoma/Malignant Fibrous Histiocytoma of Bone; Ovarian Cancer, Childhood; Ovarian Epithelial Cancer; Ovarian Germ Cell Tumor; Ovarian Low Malignant Potential Tumor; Pancreatic Cancer; Pancreatic Cancer, Childhood; Pancreatic Cancer, Islet Cell; Paranasal Sinus and Nasal Cavity Cancer; Parathyroid Cancer; Penile Cancer; Pheochromocytoma; Pineal and Supratentorial Primitive Neuroectodermal Tumors, Childhood; Pituitary Tumor; Plasma Cell Neoplasm/Multiple Myeloma; Pleuropulmonary Blastoma; Pregnancy and Breast Cancer; Pregnancy and Hodgkin's Lymphoma; Pregnancy and Non-Hodgkin's Lymphoma; Primary Central Nervous System Lymphoma; Primary Liver Cancer, Adult; Primary Liver Cancer, Childhood; Prostate Cancer; Rectal Cancer; Renal Cell (Kidney) Cancer; Renal Cell Cancer, Childhood; Renal Pelvis and Ureter, Transitional Cell Cancer; Retinoblastoma; Rhabdomyosarcoma, Childhood; Salivary Gland Cancer; Salivary Gland Cancer, Childhood; Sarcoma, Ewing's Family of Tumors; Sarcoma, Kaposi's; Sarcoma (Osteosarcoma)/Malignant Fibrous Histiocytoma of Bone; Sarcoma, Rhabdomyosarcoma, Childhood; Sarcoma, Soft Tissue, Adult; Sarcoma, Soft Tissue, Childhood; Sezary Syndrome; Skin Cancer; Skin Cancer, Childhood; Skin Cancer (Melanoma); Skin Carcinoma, Merkel Cell; Small Cell Lung Cancer; Small Intestine Cancer; Soft Tissue Sarcoma, Adult; Soft Tissue Sarcoma, Childhood; Squamous Neck Cancer with Occult Primary, Metastatic; Stomach (Gastric) Cancer; Stomach (Gastric) Cancer, Childhood; Supratentorial Primitive Neuroectodermal Tumors, Childhood; T-Cell Lymphoma, Cutaneous; Testicular Cancer; Thymoma, Childhood; Thymoma, Malignant; Thyroid Cancer; Thyroid Cancer, Childhood; Transitional Cell Cancer of the Renal Pelvis and Ureter; Trophoblastic Tumor, Gestational; Unknown Primary Site, Cancer of, Childhood; Unusual Cancers of Childhood; Ureter and Renal Pelvis, Transitional Cell Cancer; Urethral Cancer; Uterine Sarcoma; Vaginal Cancer; Visual Pathway and Hypothalamic Glioma, Childhood; Vulvar Cancer; Waldenstrom's Macro globulinemia; and Wilms' Tumor.

Further exemplary cancers include diffuse large B-cell lymphoma (DLBCL) and mantle cell lymphoma (MCL).

Metastases of the aforementioned cancers can also be treated or prevented in accordance with the methods described herein.

In some embodiments, these methods can result in a reduction in the number, severity, or frequency of one or more symptoms of the cancer in the subject (e.g., as compared to the number, severity, or frequency of the one or more symptoms of the cancer in the subject prior to treatment).

In some embodiments, the methods of treating a disease (e.g., cancer) in a subject may comprise administering the ACC(s), nucleic acid(s), vector(s), composition (e.g., pharmaceutical composition) herein in combination with one or more immune checkpoint inhibitors (e.g., a PD-1 and/or PD-L1). The immune checkpoint inhibitors may be antibodies against PD-1 or PD-L1, e.g., those in Table 3 below.

In some embodiments of any of the methods described herein, the methods further include administering to a subject an additional therapeutic agent (e.g., one or more of the therapeutic agents listed in Table 3).

TABLE 3

Additional Therapeutic Agents

Antibody Trade Name (antibody name)
Target

Raptiva ™ (efalizumab)
CD11a

Arzerra ™ (ofatumumab)
CD20

Bexxar ™ (tositumomab)
CD20

Gazyva ™ (obinutuzumab)
CD20

Ocrevus ™ (ocrelizumab)
CD20

Rituxan ™ (rituximab)
CD20

Zevalin ™ (ibritumomab tiuxetan)
CD20

Adcetris ™ (brentuximab vedotin)
CD30

Myelotarg ™ (gemtuzumab)
CD33

Mylotarg ™ (gemtuzumab ozogamicin)
CD33

(vadastuximab)
CD33

(vadastuximab talirine)
CD33

Campath ™ (alemtuzumab)
CD52

Lemtrada ™ (alemtuzumab)
CD52

Tactress ™ (tamtuvetmab)
CD52

Soliris ™ (eculizumab)
Complement C5

Ultomiris ™ (ravulizumab)
Complement C5

(olendalizumab)
Complement C5

Yervoy ™ (ipilimumab)
CTLA-4

(tremelimumab)
CTLA-4

Orencia ™ (abatacept)
CTLA-4

Hu5c8
CD40L

(letolizumab)
CD40L

Rexomun ™ (ertumaxomab)
CD3/Her2

Erbitux ™ (cetuximab)
EGFR

Portrazza ™ (necitumumab)
EGFR

Vectibix ™ (panitumumab)
EGFR

CH806
EGFR

(depatuxizumab)
EGFR

(depatuxizumab mafodotin)
EGFR

(futuximab:modotuximab)
EGFR

ICR62 (imgatuzumab)
EGFR

(laprituximab)
EGFR

(losatuxizumab)
EGFR

(losatuxizumab vedotin)
EGFR

mAb 528
EGFR

(matuzumab)
EGFR

(nimotuzumab)
EGFR

(tomuzotuximab)
EGFR

(zalutumumab)
EGFR

MDX-447
EGFR/CD64

(adecatumumab)
EpCAM

Panorex ™ (edrecolomab)
EpCAM

Vicinium ™
EpCAM

Synagis ™ (palivizumab)
F protein of RSV

ReoPro ™ (abiciximab)
Glycoprotein receptor IIb/IIIa

Herceptin ™ (trastuzumab)
Her2

Herceptin ™ Hylecta (trastuzumab;
Her2

Hyaluronidase)

(trastuzumab deruxtecan)
Her2

(hertuzumab verdotin)
Her2

Kadcyla ™ (trastuzumab emtansine)
Her2

(margetuximab)
Her2

(timigutuzumab)
Her2

Xolair ™ (omalizumab)
IgE

(ligelizumab)
IgE

(figitumumab)
IGF1R

(teprotumumab)
IGF1R

Simulect ™ (basiliximab)
IL2R

Zenapax ™ (daclizumab)
IL2R

Zinbryta ™ (daclizumab)
IL2R

Actemra ™ (tocilizumab)
IL-6 receptor

Kevzara ™ (sarilumab)
IL-6 receptor

(vobarilizumab)
IL-6 receptor

Stelara ™ (ustekinumab)
IL-12/IL-23

Tysabri ™ (natalizumab)
Integrinα4

(abrilumab)
Integrinα4

Jagged 1 or Jagged 2

(fasinumab)
NGF

(fulranumab)
NGF

(tanezumab)
NGF

Notch, e.g., Notch 1

Pidilizumab
Delta like-1 (PD-1 pathway

inhibitor)

Opdivo ® (nivolumab)
PD1

Keytruda ® (pembrolizumab)
PD1

Libtayo ® (cemiplimab)
PD1

BGB-A317 (tislelizumab)
PD1

PDR001 (spartalizumab)
PD1

JNJ-63723283 (cetrelimab)
PD1

TSR042 (dostarlimab)
PD1

AGEN2034 (balstilimab)
PD1

JS001 (toripalimab)
PD1

IOBI308 (sintilimab)
PD1

BCD100 (prolgolimab)
PD1

CBT-501 (genolimzumab
PD1

ABBV181 (budigalimab)
PD1

AK105
PD1

BI-754091
PD1

INCSHR-1210
PD1

MEDI0680
PD1

MGA012
PD1

SHR-1210
PD1

Imfinzi ™ (durvalumab)
PD-L1

Tecentriq ® (atezolizumab)
PD-L1

Bavencio ® (avelumab)
PD-L1

KN035 (envafolimab)
PD-L1

BMS936559 (MDX1105)
PD-L1

BGBA 333
PD-L1

FAZ053
PD-L1

LY-3300054
PD-L1

SH-1316
PD-L1

AMP-224
PD-L2

(bavituximab)
Phosphatidylserine

huJ591
PSMA

RAV12
RAAG12

Prolia ™ (denosumab)
RANKL

GC1008 (fresolimumab)
TGFbeta

Cimzia ™ (Certolizumab Pegol)
TNFα

Remicade ™ (infliximab)
TNFα

Humira ™ (adalimumab)
TNFα

Simponi ™ (golimumab)
TNFα

Enbrel ™ (etanercept)
TNF-R

(mapatumumab)
TRAIL-R1

Avastin ™ (bevacizumab)
VEGF

Lucentis ™ (ranibizumab)
VEGF

(brolucizumab)
VEGF

(vanucizumab)
VEGF

Compositions/Kits

Also provided herein are compositions (e.g., pharmaceutical compositions) including any of the ACCs, nucleic acids, and/or vectors described herein and one or more (e.g., 1, 2, 3, 4, or 5) pharmaceutically acceptable carriers (e.g., any of the pharmaceutically acceptable carriers described herein), diluents, or excipients.

In some embodiments, the compositions (e.g. pharmaceutical compositions) that include any of the ACCs, nucleic acids, and/or vectors described herein can be disposed in a sterile vial or a pre-loaded syringe.

In some embodiments, the compositions (e.g. pharmaceutical compositions) that include any of the ACCs described herein can be formulated for different routes of administration (e.g., intravenous, subcutaneous, intramuscular, intraperitoneal, or intratumoral).

In some embodiments, any of the pharmaceutical compositions described herein can include one or more buffers (e.g., a neutral-buffered saline, a phosphate-buffered saline (PBS), amino acids (e.g., glycine), one or more carbohydrates (e.g., glucose, mannose, sucrose, dextran, or mannitol), one or more antioxidants, one or more chelating agents (e.g., EDTA or glutathione), one or more preservatives, and/or a pharmaceutically acceptable carrier (e.g., bacteriostatic water, PBS, or saline).

As used herein, the phrase “pharmaceutically acceptable carrier” refers to any and all solvents, dispersion media, coatings, antibacterial agents, antimicrobial agents, isotonic and absorption delaying agents, and the like, compatible with pharmaceutical administration. Suitable carriers include, but are not limited to: water, saline, ringer's solutions, dextrose solution, and about 5% human serum albumin.

In some embodiments of any of the pharmaceutical compositions described herein, any of the ACCs described herein are prepared with carriers that protect against rapid elimination from the body, e.g., sustained and controlled release formulations, including implants and microencapsulated delivery systems. Biodegradable, biocompatible polymers can be used, e.g., ethylene vinyl acetate, polyanhydrides, polyglycolic acid, collage, polyorthoesters, and polylactic acid. Methods for preparation of such pharmaceutical compositions and formulations are apparent to those skilled in the art.

Also provided herein are kits that include any of the ACCs described herein, any of the compositions that include any of the ACCs described herein, or any of the pharmaceutical compositions that include any of the ACCs described herein. Also provided are kits that include one or more second therapeutic agent(s) selected from Table 3 in addition to an ACC described herein. The second therapeutic agent(s) may be provided in a dosage administration form that is separate from the ACC. Alternatively, the second therapeutic agent(s) may be formulated together with the ACC.

Any of the kits described herein can include instructions for using any of the compositions (e.g., pharmaceutical compositions) and/or any of the ACCs described herein. In some embodiments, the kits can include instructions for performing any of the methods described herein. In some embodiments, the kits can include at least one dose of any of the compositions (e.g., pharmaceutical compositions) described herein. In some embodiments, the kits can provide a syringe for administering any of the pharmaceutical compositions described herein.

The present disclosure includes the following aspects including any combinations of any of the following aspects:

1. An activatable cytokine construct (ACC) comprising:

- a first monomer construct comprising a first cytokine protein (CP1), a first cleavable moiety (CM1), and a first steric masking moiety (SMM1), wherein the CM1 is positioned between the CP1 and the SMM1;
- a second monomer construct comprising a second cytokine protein (CP2), a second cleavable moiety (CM2), and a second steric masking moiety (SMM2), wherein the CM2 is positioned between the CP2 and the SMM2; and
- a third monomer construct comprising a third cytokine protein (CP3), a third cleavable moiety (CM3), and a third steric masking moiety (SMM3), wherein the CM3 is positioned between the CP3 and the SMM3,
- wherein:
- the CP1, the CP2, and the CP3 bind to one another thereby forming a trimer of the first, the second, and the third monomer constructs; and
- the SMM1, the SMM2, and the SMM3 are globular molecules.

2. The ACC of aspect 1, wherein the CP1, the CP2, and the CP3 are the same cytokine.

3. The ACC of aspect 2, wherein the cytokine is a member of tumor necrosis factor or tumor necrosis factor super family.

4. The ACC of aspect 2, wherein the CP1, the CP2 and the CP3 are tumor necrosis factor superfamily member 14 (TNFSF14).

5. The ACC of aspect 2, wherein each of the CP1, the CP2, and the CP3 comprises a sequence that is at least 80%, 90%, 95%, or 99% identical to SEQ ID NO: 54.

6. The ACC of any one or combination of aspects 1-5, wherein the SMM1, the SMM2, and the SMM3 are the same globular molecule.

7. The ACC of aspect 6, wherein the globular molecule is an albumin.

8. The ACC of aspect 7, wherein the albumin is a human serum albumin.

9. The ACC of aspect 7, wherein the albumin comprises a sequence that is at least 80%, 90%, 95%, or 99% identical to a human serum albumin.

10. The ACC of any one or combination of aspects 1-9, wherein the first monomer construct comprises at least one linker.

11. The ACC of aspect 10, wherein the at least one linker comprises a linker L1 disposed between the CP1 and the CM1, and/or a linker L2 between the CM1 and the SMM1.

12. The ACC any one or combination of aspects 1-11, wherein the second monomer construct comprises at least one linker.

13. The ACC of aspect 12, wherein the at least one linker comprises a linker L3 disposed between the CP2 and the CM2, and/or a linker L4 between the CM2 and the SMM2.

14. The ACC of any one or combination of aspects 1-13, wherein the third monomer construct comprises at least one linker.

15. The ACC of aspect 14, wherein the at least one linker comprises a linker L5 disposed between the CP3 and the CM3, and/or a linker L6 between the CM3 and the SMM3.

16. The ACC of any one or combination of aspects 1-15, wherein:

- the first monomer construct further comprises a first affinity masking moiety (AMM1) and optionally a fourth cleavable moiety (CM4) positioned between the AMM1 and the CP1,
- the second monomer construct further comprises a second affinity masking moiety (AMM2) and optionally a fifth cleavable moiety (CM5) positioned between the AMM2 and the CP2, and
- the third monomer construct further comprises a third affinity masking moiety (AMM3) and optionally a sixth cleavable moiety (CM6) positioned between the AMM3 and the CP3.

17. The ACC of aspect 16, wherein the AMM1, the AMM2, and the AMM3 are the same.

18. The ACC of aspect 16, wherein the each of AMM1, the AMM2, and the AMM3 comprises a sequence of SEQ ID NO: 61.

19. The ACC of aspect 16, wherein the each of AMM1, the AMM2, and the AMM3 comprises a sequence that at least 80%, 90%, 95%, or 99% identical to SEQ ID NO:

61.

20. The ACC of any one or combination of aspects 1-19, wherein the CM1, the CM2, and the CM3 comprise a substrate of the same protease.

21. The ACC of any one or combination of aspects 1-19, wherein the CM1, the CM2, and the CM3 comprise substrates of different proteases.

22. The ACC of any one or combination of aspects 1-19, wherein each of the CM1, the CM2, and the CM3 comprises a sequence that is at least 95% identical to SEQ ID NO: 62 or 63.

23. The ACC of any one or combination of aspects 16-22, wherein the CM4, the CM5, and the CM6 comprise a substrate of the same protease.

24. The ACC of any one or combination of aspects 16-22, wherein the CM4, the CM5, and the CM6 comprise substrates of different proteases.

25. The ACC of any one or combination of aspects 16-22, wherein each of the CM4, the CM5, and the CM6 comprises a sequence that is at least 95% identical to SEQ ID NO. 62 or 63.

26. The ACC of any one or combination of aspects 20-25, wherein the protease(s) is/are produced by a tumor in a subject.

27. The ACC of any one or combination of aspects 20-25, wherein the protease(s) is/are selected from the group consisting of: ADAM8, ADAM9, ADAM10, ADAM12, ADAM15, ADAM17/TACE, ADAMDEC1, ADAMTS1, ADAMTS4, ADAMTS5, BACE, Renin, Cathepsin D, Cathepsin E, Caspase 1, Caspase 2, Caspase 3, Caspase 4, Caspase 5, Caspase 6, Caspase 7, Caspase 8, Caspase 9, Caspase 10, Caspase 14, Cathepsin B, Cathepsin C, Cathepsin K, Cathespin L, Cathepsin S, Cathepsin V/L2, Cathepsin X/Z/P, Cruzipain, Legumain, Otubain-2, KLK4, KLK5, KLK6, KLK7, KLK8, KLK10, KLK11, KLK13, KLK14, Meprin, Neprilysin, PSMA, BMP-1, MMP-1, MMP-2, MMP-3, MMP-7, MMP-9, MMP-10, MMP-11, MMP-12, MMP-13, MMP-14, MMP-15, MMP-16, MMP-17, MMP-19, MMP-20, MMP-23, MMP-24, MMP-26, MMP-27, activated protein C, cathepsin A, cathepsin G, Chymase, FVIIa, FIXa, FXa, FXIa, FXIIa, Elastase, Granzyme B, Guanidinobenzoatase, HtrA1, human neutrophil lyase, lactoferrin, marapsin, NS3/4A, PACE4, Plasmin, PSA, tPA, thrombin, tryptase, uPA, DESC1, DPP-4, FAP, Hepsin, Matriptase-2, MT-SP1/Matripase, TMPRSS2, TMPRSS3, and TMPRSS4.

28. The ACC of any one or combination of aspects 16-27, wherein the first monomer construct further comprises a linker L7 between the AMM1 and the CM4 and/or a linker L8 between the CM4 and the CP1.

29. The ACC of aspect any one or combination of aspects 16-28, wherein the second monomer construct further comprises a linker L9 between the AMM2 and the CM5 and/or a linker L10 between the CM5 and the CP2.

30. The ACC of any one or combination of aspects 16-29, wherein the third monomer construct further comprises a linker L11 between the AMM3 and the CM6 and/or a linker L12 between the CM6 and the CP3.

31. The ACC of any one or combination of aspects 11-30, wherein each of the linkers L1-L12 has a total length of 2 to 30 amino acids.

32. The ACC of any one or combination of aspects 11-31, wherein each of the linkers L1-L12 independently comprises a sequence of any one of SEQ ID NO: 64-69, 75-77, GGS, SGG, GSG, GS, or G.

33. The ACC of any one or combination of aspects 1-32, wherein in a N- to C-terminal direction:

- the first monomer construct comprises the CP1, the CM1, and the SMM1,
- the second monomer construct comprises the CP2, the CM2, and the SMM2, and
- the third monomer construct comprises the CP3, the CM3, and the SMM3.

34. The ACC of any one or combination of aspects 1-32, wherein in a N- to C-terminal direction:

- the first monomer construct comprises the SMM1, the CM1, and the CP1,
- the second monomer construct comprises the SMM2, the CM2, and the CP2, and
- the third monomer construct comprises the SMM3, the CM3, and the CP3.

35. The ACC of any one or combination of aspects 16-34, wherein in a N- to C-terminal direction:

- the first monomer construct comprises the AMM1, the CM4, the CP1, the CM1, and the SMM1,
- the second monomer construct comprises the AMM2, the CM5, the CP2, the CM2, and the SMM2, and
- the third monomer construct comprises the AMM3, the CM6, the CP3, the CM3, and the SMM3.

36. The ACC of any one or combination of aspects 16-34, wherein in a N- to C-terminal direction:

- the first monomer construct comprises the SMM1, the AMM1, the CM1, and the CP1;
- the second monomer construct comprises the SMM2, the AMM2, the CM2, and the CP2, and
- the third monomer construct comprises the SMM3, the AMM3, the CM3, and the CP3.

37. The ACC of any one or combination of aspects 16-34, wherein in a N- to C-terminal direction:

- the first monomer construct comprises, the AMM1, the SMM1, the CM1, and the CP1;
- the second monomer construct comprises the AMM2, the SMM2, the CM2, and the CP2, and
- the third monomer construct comprises the AMM3, the SMM3, the CM3, and the CP3.

38. The ACC of any one or combination of aspects 16-34, wherein in a N- to C-terminal direction:

- the first monomer construct comprises the SMM1, the CM1, the CP1, the CM4, and AMM1,
- the second monomer construct comprises the SMM2, the CM2, the CP2, the CM5, and AMM2, and
- the third monomer construct comprises the SMM3, the CM3, the CP3, the CM6, and the AMM3.

39. The ACC of any one or combination of aspects 16-34, wherein in a N- to C-terminal direction:

- the first monomer construct comprises the CP1, the CM1, the AMM1, and the SMM1;
- the second monomer construct comprises the CP2, the CM2, the AMM2, and the SMM2; and
- the third monomer construct comprises the CP3, the CM3, the AMM3, and the SMM3.

40. The ACC of any one or combination of aspects 16-34, wherein in a N- to C-terminal direction:

- the first monomer construct comprises the CP1, the CM1, the SMM1, and the AMM1;
- the first monomer construct comprises the CP2, the CM2, the SMM2, and the AMM2; and
- the first monomer construct comprises the CP3, the CM3, the SMM3, and the AMM3.

41. The ACC of any one or combination of aspects 1-40, wherein, in an inactive state, the ACC is characterized by having a reduced level of an activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof as compared to a control level of the activity of at least one of the CP1, the CP2, the CP3, or the trimer thereof.

42. The ACC of aspect 41, wherein the ACC is characterized by at least a 2-fold, 5-fold, 10-fold, 500-fold, 10³-fold, 10⁴-fold, 10⁵-fold, or 10⁶-fold reduction in the activity of the trimer of CP1, CP2, and CP3 as compared to the activity of a control trimer of CP1, CP2, and CP3 that does not comprise a steric masking moiety or an affinity masking moiety.

43. The ACC of aspect 41 or 42, wherein the activity is activation of herpes virus entry mediator (HVEM).

44. The ACC of aspect 41 or 42, wherein the activity is activation of lymphotoxin beta receptor.

45. The ACC of aspect 41 or 42, wherein the activity is activation of herpes virus entry mediator (HVEM) and activation of lymphotoxin beta receptor.

46. The ACC of any one or combination of aspects 41-45, wherein the control trimer of CP1, CP2, and CP3 results from activation of the ACC.

47. An activatable cytokine construct (ACC) comprising:

- a first monomer construct comprising a first cytokine protein (CP1), a first cleavable moiety (CM1), and a first affinity masking moiety (AMM1), wherein the CM1 is positioned between the CP1 and the AMM1;
- a second monomer construct comprising a second cytokine protein (CP2), a second cleavable moiety (CM2), and a second affinity masking moiety (AMM2), wherein the CM2 is positioned between the CP2 and the AMM2; and
- a third monomer construct comprising a third cytokine protein (CP3), a third cleavable moiety (CM3), and a third affinity steric masking moiety (AMM3), wherein the CM3 is positioned between the CP3 and the AMM3,
- wherein the CP1, the CP2, and the CP3 bind to one another thereby forming a trimer of the first, the second, and the third monomer constructs.

48. An ACC of any one or combination of aspects 1-47, wherein the first monomer construct, the second monomer construct, and the third monomer construct are identical.

49. An ACC of any one or combination of aspects 1-48, wherein the ACC does not comprise any domain that facilitates formation of a trimer other than CP1, CP2, and CP3.

50. The ACC of aspect 49, wherein the ACC does not comprise any domain other than the CP1, the CP2, and the CP3 that covalently links the first, the second, and the third monomer constructs.

51. The ACC of aspect 49, wherein the ACC does not comprise a coil-coiled domain, an Fc domain, or a domain other than the CP1, the CP2, or the CP3 that is capable forming a disulfide bond.

52. The ACC of any one or combination of aspects 1-51, wherein the CP1, CP2, and CP3 are identical and each comprises the amino acid sequence of SEQ ID NO: 54.

53. The ACC of aspect 46, wherein the first monomer construct, the second monomer construct, and the third monomer construct are identical and each monomer comprises:

- a. the amino acid sequence of SEQ ID NO: 54; and
- b. an AMM comprising an amino acid sequence that is at least 95% identical to that of SEQ ID NO: 61; and
- c. an SMM comprising an albumin.

54. A composition comprising the ACC of any one or combination of aspects 1-53.

55. The composition of aspect 54, wherein the composition is a pharmaceutical composition.

56. A container, vial, syringe, injector pen, or kit comprising at least one dose of the composition of aspect 54 or 55.

57. A nucleic acid encoding a polypeptide that comprises at least one of the first monomer construct, the second monomer construct, or the third monomer construct of the ACC of any one or combination of aspects 1-53.

58. The nucleic acid of aspect 57, comprising a sequence of any one of SEQ ID NOs: 9, 11, 13, 25, 31, 41, 43, 45, or 47.

59. A set of nucleic acids that together encode polypeptides that comprise the first monomer construct, the second monomer construct, and the third monomer construct in the ACC of any one or combination of aspects 1-53.

60. A vector comprising the nucleic acid or a set of nucleic acids of any of aspects 57-59.

61. A cell comprising the nucleic acid of any one or combination of aspects 57-59 or the vector of aspect 60.

62. A method of treating a subject in need thereof comprising administering to the subject a therapeutically effective amount of the ACC of any one or combination of aspects 1-53 or the composition of aspect 54 or 55.

63. The method of aspect 62, wherein the subject has been identified or diagnosed as having a cancer.

64. The method of aspect 62 or 63, further comprising administering an immune checkpoint inhibitor.

65. The method of aspect 64, wherein the immune checkpoint inhibitor is an anti-PD-1 antibody or anti-PD-L1 antibody.

66. A method of producing an ACC comprising:

- culturing a cell of aspect 61 in a liquid culture medium under conditions sufficient to produce the ACC; and
- recovering the ACC from the cell or the liquid culture medium.

67. The method of aspect 66, further comprising purifying the recovered ACC using affinity chromatography.

68. The method of aspect 66 or 67, further comprising formulating the recovered ACC into a pharmaceutical composition.

EXAMPLES

The invention is further described in the following examples, which do not limit the scope of the invention described in the claims.

Example 1: Activity of LIGHT Cytokine Constructs Engineered with a Non-Cleavable HSA Steric Mask

Cytokine construct LIGHT-21linker_HSA_Myc_cMyc (ProC1184) was prepared by recombinant methods. The 1^st, 2^ndand 3^rdmonomer constructs of this construct were identical, with each being a polypeptide having the amino acid sequence shown in FIG. 2A (SEQ ID NO: 102). Each of the 1^st, 2^ndand 3^rdmonomer constructs comprises, from N-terminus to C-terminus, a modified signal sequence from a mouse IgG kappa signal sequence (SEQ ID NO: 78), a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79), a non-cleavable linker having the amino acid sequence of SEQ ID NO: 65, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a non-cleavable linker having the of SGG, and a Myc Tag sequence having the SEQ ID NO: 59. The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 103, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, LIGHT-21linker_HSA_cMyc. The expressed trimeric polypeptides were purified using an HSA-affinity column (e.g., POROS CaptureSelect HSA resin), followed by size exclusion chromatography (SEC), if necessary, to obtain the trimeric protein in at least 95% purity. The final cytokine construct that is assayed did not include the signal sequence.

Cytokine construct LIGHT-10GS-Strep (Prod 188) was also prepared by recombinant methods. The 1^st, 2^ndand 3^rdmonomer constructs of this CC were identical, with each being a polypeptide having the amino acid sequence shown in FIG. 2A (SEQ ID NO: 86). Each of the 1^st, 2^ndand 3^rdmonomer constructs comprises, from N-terminus to C-terminus, a modified signal sequence from a mouse IgG kappa signal sequence (SEQ ID NO: 78), a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54), a non-cleavable linker having the sequence of SEQ ID NO: 66, and a Strep Tag sequence (SEQ ID NO: 60). The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 87, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, LIGHT-10GS-Strep. The expressed trimeric polypeptides were purified using a streptavidin-affinity column (e.g., streptavidin agarose resin), followed by size exclusion chromatography (SEC), if necessary, to obtain the trimeric protein in at least 95% purity. The final cytokine construct that is assayed did not have the signal sequence.

Activity of the LIGHT cytokine was evaluated using an HVEM cell-based assay and a Lymphotoxin beta receptor cell-based assay (A375 IL-8 ELISA), as described below.

The activity of each cytokine construct was tested in vitro using a recombinant human HVEM/NF-kB reporter Jurkat cell line expressing firefly luciferase gene (BPS Biosciences #79310). Cells were cultured in RPMI 1640 media supplemented with 10% HI FBS (heat inactivated fetal bovine serum) and 1% Pen/Strep (penicillin-streptomycin). The addition of LIGHT to these cells activates the HVEM receptor and subsequently signals NF-kB transcription factors to bind to the DNA elements required to induce transcription of the luciferase reporter gene. Expression of the luciferase reporter gene can be quantified using the ONE-Glo Luciferase Assay system (commercially available from Promega).

LIGHT-responsive Jurkat HVEM/NF-kB luciferase reporter cells were prepared at a concentration of 390,000 cells/mL in RPMI 1640 media (ThermoFisher Scientific, e.g., Catalog #11875093) supplemented with 10% HI FBS and 90 μL aliquots were pipetted into wells of a white flat-bottom 96-well plate (35,000 cells/well). The tested cytokines were diluted to a starting concentration of 450 nM in RPMI 1640 media supplemented with 10% HI FBS. Duplicates of four-fold serial dilutions were prepared from which 10 μL was added to each well. The plate was shaken for 1-2 minutes at 250 rpm then placed in a 37° C. incubator for 4 hours. Following the 4-hour incubation, the plate was removed from the incubator and allowed to equilibrate to room temperature. The ONE-Glo Luciferase reagent was prepared by transferring the contents of the ONE-Glo Assay Buffer to the lyophilized ONE-Glo Assay Substrate and inverting until the substrate was thoroughly dissolved. 15 mL aliquots of the reagent were stored at −20° C. and thawed to room temperature out of direct light on the day of the assay. Once the reagent and plate were equilibrated to room temperature, 100 μL aliquots of the ONE-Glo Luciferase reagent were pipetted into each well of the plate. The plate was placed on a plate shaker at 250 rpm covered from direct light for 1-2 minutes. After thorough mixing, the luciferase expression was measured using the Tecan Infinite M Plex multimode plate reader. Dose-response curves were generated and EC50 values were obtained by sigmoidal fit non-linear regression using GraphPad Prism software.

The activity of each cytokine construct was tested in vitro using A375 cells, a human melanoma cell line with a high expression of lymphotoxin beta receptor (LTbR). Cells were cultured in Dulbecco's Modified Eagle Medium (DMEM) media supplemented with 10% HI FBS and 1% Pen/Strep. The addition of LIGHT to these cells activates the LTbR which modulates a variety of inflammatory signals, including the secretion of IL-8. The IL-8 secretion by LTbR-activated A375 cells can be measured using the human IL-8/CXCL8 DuoSet ELISA kit (R&D Systems, Catalog #DY208).

A375 cells were prepared at a concentration of 400,000 cells/mL in DMEM media supplemented with 10% HI FBS and 100 μL aliquots were pipetted into the wells of a clear, flat-bottom 96-well plate (40,000 cells/well). The plate was incubated at 37° C. for 3-5 hours. Following incubation, the tested cytokines were diluted to a starting concentration of 5 nM or 400 nM in DMEM media supplemented with 10% HI FBS. Duplicates of four-fold serial dilutions were prepared from which 100 μL was added to each well. The plate was tapped lightly to mix then placed in a 37° C. incubator overnight. On the same day, another clear, flat-bottom 96-well plate was coated with 100 μL of the recommended dilution of IL-8 capture antibody provided in the R&D Systems IL-8 ELISA kit. The plate was then covered and incubated overnight at room temperature. The following day, IL-8 production was analyzed by following the protocol provided in the R&D IL-8 ELISA kit, Once complete, the IL-8 levels were measured using a spectrophotometer at 450 nm. Dose-response curves were generated and EC50 values were obtained by sigmoidal fit non-linear regression using GraphPad Prism software.

The data in FIGS. 2A and 2B show that LIGHT activity of the construct ProC1184 (engineered with a non-cleavable HSA moiety at its C-terminal extremity) was reduced as compared to the LIGHT construct ProC1188 (engineered with a short non-cleavable Strep Tag). This data indicates that the non-cleavable HSA moiety provides steric hindrance, blocking the engagement of LIGHT with its receptors, and activation of downstream signaling. EC50 values for ProC1184 and ProC1188 were computed from the HVEM assay results and Lymphotoxin beta receptor assay and are provided below in Table 4 and Table 5 respectively.

TABLE 4

EC50 [nM]: HVEM Reporter Assay

ProC1184
ProC1188

EC50
>10e6
0.8433

TABLE 5

EC50 [pM]: Lymphotoxin beta receptor Reporter Assay

ProC1184
ProC1188

EC50
79.3
5.3

The data in Table 4 above indicates an extremely high (e.g., greater than 10⁶fold (one million fold)) masking efficiency for ProC1184 as calculated by comparing the EC50 of the control ProC1188 trimer to the EC50 of the masked ProC1184 in the HVEM Reporter Assay.

Example 2: Activity of LIGHT Cytokine Constructs Engineered with a Cleavable Affinity Peptide Mask

Cytokine construct ProC_mLm16_1490_LIGHT-10GS-Strep (ProC1192) was prepared by recombinant methods. The 1^st, 2^ndand 3^rdmonomer constructs of this ACC were identical, with each being a polypeptide having the amino acid sequence shown in FIG. 3A (SEQ ID NO: 88). Each of the 1^st, 2^ndand 3^rdmonomer constructs comprises, from N-terminus to C-terminus, a signal sequence from a modified mouse IgG kappa signal sequence (SEQ ID NO: 78), a header sequence (SEQ ID NO: 76), an affinity masking peptide having the sequence of SEQ ID NO: 61, a linker having the sequence of SEQ ID NO: 68, a cleavable moiety having the sequence of SEQ ID NO: 62, a linker having the sequence of GGS, a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79), a non-cleavable linker having the sequence of SEQ ID NO: 66, and a Strep Tag sequence (SEQ ID NO: 60). The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 89, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_mLm16_1490_LIGHT-10GS-Strep. The final cytokine construct that is assayed did not have the signal sequence.

The data in FIGS. 3A and 3B show that LIGHT activity of the ACC ProC1192 engineered with a cleavable affinity peptide mask at its N-terminal extremity was reduced as compared to the LIGHT construct ProC1188 engineered with a short non-cleavable Strep Tag. This data indicates that the cleavable affinity peptide mask provides effective masking by blocking the engagement of LIGHT with its receptors, and activation of downstream signaling.

To cleave the affinity peptide mask, LIGHT-containing ACCs were treated overnight at 37° C. with recombinant human proteases such as urokinase-type plasminogen activator (uPA). The results from these assays (FIGS. 3A and 3B) indicate that the treatment of LIGHT-containing ACCs with proteases could restore activity to a level that is comparable to the LIGHT cytokine engineered with no masking moiety (no affinity peptide mask or HSA moiety).

EC50 values for ProC1192 and ProC1188 were computed from the HVEM assay results and Lymphotoxin beta receptor assay and are provided below in Table 6 and Table 7 respectively.

TABLE 6

EC50 [nM]: HVEM Reporter Assay

ProC1192
ProC1192 + uPa
ProC1188

EC50
25.6
0.999
1.0

TABLE 7

EC50 [pM]: Lymphotoxin beta receptor Reporter Assay

ProC1192
ProC1192 + uPa
ProC1188

EC50
31.3
2.0
5.3

The data in Table 6 above indicates a masking efficiency for ProC1192 of greater than 20-fold as calculated by comparing the EC50 of either the control ProC1188 trimer or the protease-activated ProC1 192 to the EC50 of the masked ProC1 184 in the HVEM Reporter Assay.

Example 3: Activity of LIGHT Cytokine Constructs Engineered with a Cleavable Affinity Peptide Mask and a Non-Cleavable HSA Steric Masking Moiety

Cytokine construct ProC_mLm-16_1490_LIGHT_21linker_HSA-cMyc (ProC1163) was prepared by recombinant methods. The 1^st, 2^ndand 3^rdmonomer constructs of this CC were identical, with each being a polypeptide having the amino acid sequence shown SEQ ID NO: 130. Each of the 1^st, 2^ndand 3^rdmonomer constructs comprises, from N-terminus to C-terminus, a signal sequence from a modified mouse IgG kappa signal sequence (SEQ ID NO: 78), a header sequence (SEQ ID NO: 76), a masking peptide having the sequence of SEQ ID NO: 61, a linker having the sequence of SEQ ID NO: 68, a cleavable moiety having the sequence of SEQ ID NO: 62, a linker having the sequence of GGS, a mature cytokine protein that corresponds to truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79), a non-cleavable linker having the of SEQ ID NO: 65, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a non-cleavable linker having the sequence of SGG) and a Myc Tag sequence (SE ID NO: 59). The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 131, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_mLm-16_1490_LIGHT-21linker_HSA_cMyc. The expressed trimeric polypeptides were purified using an HSA-affinity column (e.g., POROS CaptureSelect HSA resin), followed by size exclusion chromatography (SEC), if necessary, to obtain the trimeric protein in at least 95% purity. The final cytokine construct that is assayed did not have the signal sequence.

The data in FIGS. 4A and 4B show that LIGHT activity of the ACC ProC1163 engineered with a non-cleavable HSA moiety at its C-terminal extremity and a cleavable affinity peptide at its N-terminal extremity was reduced as compared to the LIGHT construct ProC1184 engineered with a non-cleavable HSA moiety. This data indicates that the non-cleavable HSA moiety and the cleavable affinity peptide can each reduce independently LIGHT activity. It also indicates that both approaches can be combined to further reduce LIGHT signaling activity. FIG. 4C similarly shows that the LIGHT activity of the ACC ProC1163 (with peptide mask in addition to non-cleavable HSA moiety) was reduced as compared to the LIGHT construct ProC1184 (non-cleavable HSA moiety), and that the LIGHT activity of the uPa protease-activated ProC1163 ACC was recovered to a level comparable to the ProC1184 construct. Both ProC1184 and ProC1163 display LIGHT activity that is lower than that of the control ProC1188 construct (engineered with a short non-cleavable Strep Tag).

Example 4: Activity of LIGHT Activatable Cytokine Constructs Engineered with a Cleavable Affinity Peptide Mask and a Cleavable HSA Steric Masking Moiety

Cytokine construct ProC_LIGHT-1204DNI-HSA-His (ProC1491) was prepared by recombinant methods. The 1^st, 2^ndand 3^rdmonomer constructs of this ACC were identical, with each being a polypeptide having the amino acid sequence shown in FIG. 5A (SEQ ID NO: 90). Each of the 1^st, 2^ndand 3^rdmonomer constructs comprises, from N-terminus to C-terminus, a modified signal sequence from a mouse IgG kappa signal sequence (SEQ ID NO: 78), a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79), a linker having the SEQ ID NO: 64, a cleavable moiety having the of SEQ ID NO: 63, a linker having the sequence of GS, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a linker having the sequence of S, and a His Tag having the of SEQ ID NO: 58. The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 91, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_LIGHT-1204DNI-HSA-His. The final cytokine construct that is assayed did not have the signal sequence.

Cytokine construct ProC_mLm16-LIGHT-1204DNI-HSA-His (ProC1492) was prepared by recombinant methods. The 1^st, 2^ndand 3^rdmonomer constructs of this ACC were identical, with each being a polypeptide having the amino acid sequence shown in FIG. 5A (SEQ ID NO: 92). Each of the 1^st, 2^ndand 3^rdmonomer constructs comprises, from N-terminus to C-terminus, a modified signal sequence from a mouse IgG kappa signal sequence (SEQ ID NO: 78), a header sequence of SEQ ID NO: 76, a masking peptide having the sequence of SEQ ID NO: 61, a linker having the sequence of SEQ ID NO: 68, a cleavable moiety having the sequence of SEQ ID NO: 81, a linker having the sequence of GGS, a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79), a linker having the SEQ ID NO: 64, a cleavable moiety having the of SEQ ID NO: 63, a linker of the sequence GS, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a linker having the sequence S, and a His Tag having the sequence of SEQ ID NO: 58. The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 93, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_mLm16-LIGHT-1204DNI-HSA-His. The final cytokine construct that is assayed did not have the signal sequence.

The data in FIG. 5A show that, in the HVEM reporter assay, activity of LIGHT ProC1492 containing a cleavable peptide mask at its N-terminal extremity and a cleavable HSA moiety at its C-terminal extremity (dual mask) was further reduced as compared to the activity of LIGHT ProC1491 containing only a cleavable HSA moiety at its C-terminal extremity (single mask). Upon protease activation by uPa, ProC1491 and ProC1492 lost their masking potential and recovered LIGHT cytokine activity.

The data in FIG. 5B show that in the Lymphotoxin beta receptor assay (A375 ILL-8 ELISA), both ProC1491 and ProC1492 have reduced activity as compared to the unmasked LIGHT ProC1189. Upon protease activation by uPa, both ProC1491 and ProC1492 recovered activity similar to LIGHT ProC1189.

EC50 values for ProC1491 and ProC1492 were computed from the HVEM assay results and Lymphotoxin beta receptor assay and are provided below in Table 8 and Table 9 respectively.

TABLE 8

EC50 [nM]: HVEM Reporter Assay

ProC1491
ProC1491 + uPa
ProC1492
ProC1492 + uPa

EC50
10.51
1.3
67.5
7.7

TABLE 9

EC50 [pM]: Lymphotoxin beta receptor Reporter Assay

ProC1491
ProC1491 + uPa
ProC1492
ProC1492 + uPa

EC50
437.2
3.2
671.3
ambiguous

All-together, these data indicate that LIGHT activation of both HVEM and Lymphotoxin beta receptor pathway can be reduced by adding either or the combination of a cleavable peptide affinity mask (affinity masking moiety) and a cleavable HSA moiety (steric masking moiety) to LIGHT protein. Upon protease activation, LIGHT recovers its full signaling potential.

Example 6. In Vitro Characterization of Additional Cytokine Constructs

Additional activatable cytokine constructs were also prepared by recombinant methods. The 1^st, 2^ndand 3^rdmonomer constructs of these ACCs were identical.

In some ACCs, the HSA moiety was engineered at the N-terminal extremity of LIGHT, and the affinity peptide mask was engineered at the C-terminal extremity of LIGHT.

Cytokine construct ProC_cMyc-HSA-21GS-1204DNI-LIGHT (ProC1497) (SEQ ID NO: 120) comprises, from N-terminus to C-terminus, a modified signal sequence from a mouse IgG kappa signal sequence (SEQ ID NO: 78), a linker with sequence of GSG, a Myc Tag having the sequence of SEQ ID NO: 59, a linker having sequence of G, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a linker having the SEQ ID NO: 64, a cleavable moiety having the of SEQ ID NO: 63, a linker having the GS, and a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79). The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 121, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_cMyc-HSA-21GS-1204DNI-LIGHT. The final cytokine construct that is assayed did not have the signal sequence.

Cytokine construct ProC_cMyc-HSA-21GS-1204DNI-LIGHT-mLm16 (ProC1498) (SEQ ID NO: 126) comprises, from N-terminus to C-terminus, a signal sequence from a modified mouse IgG kappa signal sequence (SEQ ID NO: 78), a linker with sequence of GSG, a Myc Tag having the of SEQ ID NO: 59, a linker having sequence of G, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a linker having the SEQ ID NO: 64, a cleavable moiety having the of SEQ ID NO: 63, a linker having the GS, a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79), a linker having the SEQ ID NO: 75, a cleavable moiety having the of SEQ ID NO: 62, a linker having the SEQ ID NO: 68, and a masking peptide having the sequence of SEQ ID NO: 61. The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 127, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_cMyc-HSA-21GS-1204DNI-LIGHT-mLm16. The final cytokine construct that is assayed did not have the signal sequence.

The data in FIG. 6A show that, in the HVEM reporter assay, activity of ACC ProC1497, engineered with a cleavable HSA moiety at its N-terminal extremity, or activity of ACC ProC1498, engineered with a cleavable HSA moiety at its N-terminal extremity and a cleavable affinity peptide mask at its C-terminal extremity is significantly reduced as compared to LIGHT ProC1189 engineered without a mask. Activity of ProC1498 was further reduced as compared to activity of ProC1497. It also indicates that the addition of a peptide affinity mask and an HSA moiety at either the C-terminal or N-Terminal extremity of LIGHT can be combined to further reduces LIGHT signaling activity. Upon protease activation by uPa, both ProC1497 and ProC1498 recovered activity similar to LIGHT ProC1189.

EC50 values for ProC1497 and ProC1498 were computed from the HVEM assay results are provided below in Table 10.

TABLE 10

EC50 [nM]: HVEM Reporter Assay

ProC1189
ProC1497
ProC1497 + uPa
ProC1498
ProC1498 + uPa

EC50
0.86
19
0.89
n.d.
3.43

The data in Table 10 above indicates a masking efficiency for ProC1497 of 22-fold (22×) as calculated by comparing the EC50 of the intact ProC1497 ACC to the EC50 of the uPa protease-cleaved (activated) ProC1497 ACC in the HVEM Reporter Assay. The data in Table 10 indicates an extremely high (e.g., greater than 10⁶fold (one million fold)) masking efficiency for ProC1498 as calculated by comparing the EC50 of the intact ProC1498 ACC to the EC50 of the uPa protease-cleaved (activated) ProC1498 ACC in the HVEM Reporter Assay. The EC50 values for the masked ACC ProC1498 was not detectable (n.d.) because no cytokine activity was detected at the concentrations tested in the HVEM reporter assay.

In some ACCs, the HSA moiety and affinity peptide mask were engineered on the same extremity of LIGHT, either N-terminal or C-terminal, such that a single cleavable moiety (CM) can be cleaved to remove both the HSA moiety and the affinity peptide mask.

Cytokine construct ProC_cMyc-HSA-mLm16-1490DNI-LIGHT (ProC1488) (SEQ ID NO: 124) comprises, from N-terminus to C-terminus, a signal sequence from a modified mouse IgG kappa signal sequence (SEQ ID NO: 78), a linker with sequence of GSG, a Myc Tag having the of SEQ ID NO: 59, a linker having sequence of G, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a linker having the SEQ ID NO: 67, a header having the sequence (SEQ ID NO: 76), a affinity masking peptide having the sequence of SEQ ID NO: 61, a linker having the SEQ ID NO: 68, a cleavable moiety having the amino acid sequence of SEQ ID NO: 62, a linker having the GGS, and a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54). The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 125, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_cMyc-HSA-mLm16-1490DNI-LIGHT. The final cytokine construct that is assayed did not have the signal sequence.

Cytokine construct ProC_LIGHT-1490DNI-mLm16-HSA-cMyc (ProC1489) comprises, from N-terminus to C-terminus, a modified signal sequence from a mouse IgG kappa signal sequence (SEQ ID NO: 122), a mature cytokine protein that corresponds to a truncated human LIGHT polypeptide (SEQ ID NO: 54) (i.e., the ectodomain domain of human LIGHT, corresponding to residues 85-240 of SEQ ID NO: 79), a linker having the SEQ ID NO: 75, a cleavable moiety having the of SEQ ID NO: 62, a linker having the SEQ ID NO: 68, a masking peptide having the sequence of SEQ ID NO: 61, a linker having the SEQ ID NO: 66, a Human Serum Albumin (HSA) sequence (SEQ ID NO: 56), a linker having sequence of S, and a Myc Tag having the of SEQ ID NO: 59. The polypeptide was prepared by transforming a host cell with a polynucleotide having the sequence of SEQ ID NO: 123, followed by cultivation of the resulting recombinant host cells. Trimerization of the resulting expressed polypeptides yielded cytokine construct, ProC_LIGHT-1490DNI-mLm16-HSA-cMyc. The final cytokine construct that is assayed did not have the signal sequence.

Activity of ACCs ProC1488 and ProC1489 was evaluated in the HVEM assay. Data in FIG. 6B show that when the HSA moiety and affinity peptide mask were engineered on the same extremity of LIGHT, either N-terminal or C-terminal, LIGHT activity is significantly reduced as compared to unmasked LIGHT ProC1189. Upon protease activation by uPa, both ProC1488 and ProC1489 recovered activity similar to LIGHT ProC1189.

EC50 values for ProC1488 and ProC1489 were computed from the HVEM assay results are provided below in Table 11.

TABLE 11

EC50 [nM]: HVEM Reporter Assay

ProC1189
ProC1488
ProC1488 + uPa
ProC1489
ProC1489 + uPa

EC50
0.58
n.d.
0.63
n.d.
2.27

The EC50 values for the masked ACCs ProC1488 and ProC1489 were not detectable (n.d.) because no cytokine activity was detected at the concentrations tested in the HVEM reporter assay. This indicates that the masking of the LIGHT cytokine was very effective. The data in Table 11 above indicates an extremely high (e.g., greater than 10⁶fold (one million fold)) masking efficiency for ProC1488 as calculated by comparing the EC50 of the intact ProC1488 ACC to the EC50 of the uPa protease-cleaved (activated) ProC1488 ACC in the HVEM Reporter Assay. The data in Table 11 indicates an extremely high (e.g., greater than 10⁶fold (one million fold) masking efficiency for ProC1489 of greater than 10{circumflex over ( )}6 (one million-fold) as calculated by comparing the EC50 of the intact ProC1489 ACC to the EC50 of the uPa protease-cleaved (activated) ProC1489 ACC in the HVEM Reporter Assay.

Example 7. In Vitro Characterization of a Human-Mouse Cross-Reactive LIGHT ACC

Tang et al. (Cancer Cell. 2016 Mar. 14; 29(3):285-296) have previously reported that 4 points mutations in human LIGHT (SEQ ID No: 55) retains binding to human HVEM and lymphotoxin beta receptor but confers binding to mouse HVEM and lymphotoxin beta receptor.

ACCs ProC1486 (ProC_mhLIGHT_1204DNI_HSA-cMyc) and ProC1487 (ProC_mLm-16_mhLIGHT_1204DNI_HSA-cMyc) have been engineered similarly to ProC1491 and ProC1492 respectively, with the differences that ProC1486 and ProC1487 contain a mature cytokine protein that corresponds to the ectodomain of human LIGHT with four points mutations (Tang et al.) and a C-terminal linker (SGG) and cMyc tag (SEQ ID NO: 59) in place of the linker and His tag present on ProC1491 and 1492. ProC1491 and 1492 contain a non-mutated a mature cytokine protein that corresponds to the ectodomain of human LIGHT.

Binding of ProC1486 and ProC1487 to mouse and human lymphotoxin beta receptor was evaluated by flow cytometry. Binding to mouse receptor was evaluated using the MC38 cell line. Binding to human receptor was evaluated using the A375 cell line. The engagement of ProC1486 or ProC1487 to mouse or human receptor was detected with a PE-conjugated anti-human CD258 (LIGHT) Antibody [Biolegend Cat #: 318706 Clone: T5-39]. Data in FIG. 7A shows that ProC1486 and ProC1487 do not bind to A375 or MC38. Upon protease treatment with uPa, both ProC1486 and ProC1487 recovered binding to human and mouse lymphotoxin beta receptor. It indicates that human/mouse LIGHT ACCs engineered with a cleavable HSA moiety and/or a cleavable peptide affinity mask have reduced or no binding to mouse or human lymphotoxin beta receptor. Binding is recovered upon protease activation.

Activity of ACCs ProC1486 and ProC1487 was evaluated in the HVEM reporter assay and the A375-IL8 reporter assay as previously described.

Data in FIGS. 7B and 7C shows that activity of ProC1486 and ProC1487 was almost abolished in the HVEM assay and reduced in the Lymphotoxin beta receptor assay. Activity of ProC1487 engineered with both a peptide affinity mask and a HSA moiety was further reduced in the lymphotoxin beta receptor assay as compared to ProC1486 which is engineered with a HSA moiety only. This data indicated that the same peptide affinity mask and HSA moiety used to reduce human LIGHT activity can be used to reduce activity of a human-mouse cross-reactive LIGHT ACC. Upon protease activation with uPa, activity of ProC1486 and ProC1487 was significantly increased.

ACC ProC2076 (ProC_cMyc-HSA-mLm16-1490-mhLIGHT) has been engineered similarly to ProC1488 with the differences that ProC2076 contains a mature cytokine protein that corresponds to the ectodomain of human LIGHT with four points mutations (Tang et al., Cancer Cell. 2016 Mar. 14; 29(3):285-296).

Activity of ACCs ProC1486, ProC1487 and ProC2076 was evaluated in the Mouse HVEM reporter assay. The Mouse HVEM reporter cell line was generated by transfection of the NF-kB luc-reporter HEK-293s (BPS Bioscience, #60650) with a Mouse HVEM plasmind (Origene, #MC212911). Cells were transfected using Lipofectamine™ 2000 Transfection Reagent (ThermoFisher, #11668019) Cells expressing Mouse HVEM were selected using 0.8 mg/mL Geneticin (ThermoFisher, #10131035).

Cells were cultured in MEM media supplemented with 10% HI FBS (heat inactivated fetal bovine serum) 1% Pen/Strep (penicillin-streptomycin), Non Essential Amico Acid (ThermoFisher, #11140050), Sodium Pyruvate (ThermoFisher, #J61840.18), 50 ug/mL Hygromycin B (Thermofisher, #10687010) and 0.8 mg/mL Geneticin (ThermoFisher, #10131035). The addition of human-mouse cross-reactive LIGHT to these cells activated the Mouse HVEM receptor and subsequently signals NF-kB transcription factors to bind to the DNA elements required to induce transcription of the luciferase reporter gene. Expression of the luciferase reporter gene was quantified using the ONE-Glo Luciferase Assay system (commercially available from Promega).

LIGHT-responsive Jurkat HVEM/NF-kB luciferase reporter cells were plated at 20,000 cells per well in DMEM media (ThermoFisher Scientific, e.g., Catalog #10564011) supplemented with 10% HI FBS in a white flat-bottom 96-well plate. After overnight incubation, the media was aspirated. The tested cytokines were diluted to a starting concentration of 25 nM in DMEM media supplemented with 10% HI FBS. Duplicates of five-fold serial dilutions were prepared from which 100 μL was added to each well. The plate was shaken for 1-2 minutes at 250 rpm then placed in a 37° C. incubator for 4 hours. Following the 5-hour incubation, the plate was removed from the incubator and allowed to equilibrate to room temperature. The ONE-Glo Luciferase reagent was prepared by transferring the contents of the ONE-Glo Assay Buffer to the lyophilized ONE-Glo Assay Substrate and inverting until the substrate was thoroughly dissolved. 15 mL aliquots of the reagent were stored at −20° C. and thawed to room temperature out of direct light on the day of the assay. Once the reagent and plate were equilibrated to room temperature, 100 μL aliquots of the ONE-Glo Luciferase reagent were pipetted into each well of the plate. The plate was placed on a plate shaker at 250 rpm covered from direct light for 1-2 minutes. After thorough mixing, the luciferase expression was measured using the Tecan Infinite M Plex multimode plate reader. Dose-response curves were generated and EC50 values were obtained by sigmoidal fit non-linear regression using GraphPad Prism software.

Data in FIGS. 8A and 8B shows that activity of ProC1486, ProC1487 and ProC2076 was significantly reduced in the HVEM assay. Activity of ProC2076, engineered with a cleavable HSA moiety at its C-terminal extremity (FIG. 8A), and activity of ProC1487 (FIG. 8.B), engineered with a cleavable HSA moiety at its C-terminal extremity and a cleavable affinity peptide mask at its N-terminal extremity, were further reduced as compared to ProC2076 which was engineered with a cleavable HSA moiety and a peptide affinity mask at it's N-terminal extremity. Upon protease activation with uPa, activity of ProC1486, ProC1487 and ProC2076 was significantly increased (FIGS. 8A and 8B).

Example 8. In Vivo Characterization of a Human LIGHT ACC in HT-29 Xenograft Mice

The antitumor in vivo activity of human LIGHT ACC ProC1491 engineered with a cleavable HSA domain at the C-terminal extremity of LIGHT, and the antitumor activity of human LIGHT ProC1189 engineered with a His tag at the C-terminal extremity of LIGHT were evaluated in the HT-29 xenograft model. LTβR activation induced by its ligand lymphotoxin-α/β, LIGHT or an agonistic mAb triggers an IFNg-dependent tumor growth inhibition both in vitro and in vivo in HT29 and WiDr colon carcinoma models (Lukashev et al, Cancer Research, 2006).

To evaluate the in vivo antitumor activity of ProC1491 and ProC1189, on day 0, 2×10⁶HT29-Luc2 tumor cells in 100 μL serum-free RPMI were injected SC in the flank of 7-8 weeks female nu/nu mice. When tumors reached ˜60-100 mm³mice received an intraperitoneal injection of each test article dosed at 1 mg/kg. Each animal received a dose of test article on day 1, 5, 8, 12, 15, 19 and 22. Body weights and tumor measurements were recorded twice weekly for the duration of the study. Mice experiments were conducted according to the IACUC protocol AP303 (Use of Subcutaneous Mouse Tumor Models to Evaluate the Anti-Tumor Activity and IACUC Guideline G01: Management of Tumor Models).

Percent tumor growth inhibition (% TGI) was calculated with the following formula: TGI (%) [1−(RTV of the treated group)/(RTV of the control group)]×100(%), were RTW=(tumor volume on measured day)/(tumor volume on day 0). Data in FIG. 9 shows that, in the HT-29 xenograft mice model, human LIGHT ACC ProC1491 engineered with a cleavable HSA domain at the C-terminal extremity of LIGHT was more potent at promoting tumor growth inhibition than human LIGHT ProC1189 engineered with a His tag at the C-terminal extremity of LIGHT. The relative percent TGI are indicated in Table 12. This indicates that human LIGHT ACC ProC1491 is more potent than human LIGHT ProC1189 at inducing tumor localized antitumor activity.

TABLE 12

Percent Tumor growth inhibition in HT-29 xenograft mice model:

ProC1491
ProC1189

% TGI
52.5%
21.1%

Example 9. In Vivo Characterization of a Human-Mouse Cross-Reactive LIGHT ACC in MC38 Syngeneic Mice

The antitumor activity of human-mouse cross-reactive LIGHT ACC ProC1486, ProC1487 and ProC2076 was evaluated using the MC38 colon adenocarcinoma syngeneic mice model.

Mice experiments were conducted according to the IACUC protocol AP303 (Use of Subcutaneous Mouse Tumor Models to Evaluate the Anti-Tumor Activity and IACUC Guideline G01: Management of Tumor Models).

Seven to nine weeks old female C57BL/6 mice were implanted with MC38 tumor cells in serum-free medium. The animals were dosed intra-peritoneally with LIGHT ACC as single agent or in combination with a mouse anti-PD-1 antibody (clone RPMI1-14; BioXCell, Cat #BP0146) and tumor measurements were recorded twice weekly for the duration of the study. Percent tumor growth inhibition (% TGI) was calculated with the following formula: TGI (%)=[1−(RTV of the treated group)/(RTV of the control group)], 100(%), were RTW=(tumor volume on measured day)/(tumor volume on day 0).

In some experiments, tumor and spleen were collected to evaluate PharmacoDymanic (PD) biomarkers of LIGHT ACC activity. Tumor samples were processed according to the Miltenyi tumor dissociation kit (Miltenyi, Cat #130-096-730). Spleens were processed mechanically using a syringe plunger and treated with ACK lysis buffer (ThermoFisher, cat #A1049201) to remove red blood cells. Immune cells were analyzed by Flow cytometry using an Attune NxT Flow cytometer (ThermoFisher). Flow cytometry data were plotted and analyzed using Prism Software.

Data in FIGS. 10A and 10B show that ProC1486 and ProC1487 had single agent antitumor activity in the MC38 syngeneic mice model. The antitumor activity of ProC1486 and ProC1487 was further enhanced when dosed in combination with anti PD-1. ProC2076 had minimal single agent activity (FIG. 10B). Its antitumor activity was also increased in combination with an anti-PD-1 antibody in the MC38 syngeneic mice model (FIG. 10B).

Data in FIGS. 11A-111B show that at day 6 post treatment initiation in the MC38 syngeneic mice model, ProC1487, dosed as a single agent or in combination with an anti-PD-1 antibody, was able to increase the level of CD8+ T cells in the tumor micro-environment (FIG. 11A) as well as to promote the production of Th1 cytokines (IFNγ, TNFα) by CD8+ T cells (FIG. 11B). ProC1487 had no or limited activity in the spleen, indicating that the activity of ProC1487 is only localized in the tumor. In some cases, the data were analyzed in Prism Software using a statistical t-test. The significance of the test is illustrated in FIGS. 11A and 11B with an asterix sign.

TABLE 12

Example Sequences

SEQ ID

NO:
NOTES
SEQUENCE

1

GQSGS

2
ProC1189/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_LIGHT-10GS-
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

His
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

Protein
HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSGGGSGG

GSGHHHHHH

3
ProC1189/
CAGGAACGGCGCTCCCACGAGGTCAATCCGGCGGCTCAT

ProC_LIGHT-10GS-
TTGACTGGAGCCAACTCTAGTCTTACCGGGAGCGGCGGT

His
CCATTGCTGTGGGAGACGCAACTTGGATTGGCTTTTCTTC

DNA
GGGGATTGTCTTACCACGATGGAGCACTCGTTGTTACGAA

AGCCGGTTACTACTACATTTATTCTAAGGTCCAGTTGGGT

GGAGTTGGCTGTCCCCTGGGACTTGCAAGCACTATCACTC

ACGGACTGTACAAGAGGACACCCCGATACCCCGAGGAAC

TCGAGCTGCTTGTGAGCCAACAGTCTCCATGTGGGCGCGC

AACTAGTTCTTCACGGGTGTGGTGGGACTCCAGTTTCCTG

GGAGGTGTTGTTCATCTCGAGGCAGGTGAAGAAGTAGTT

GTCAGGGTACTTGATGAACGGCTTGTTAGACTCCGGGAT

GGAACGAGGTCCTATTTCGGTGCGTTCATGGTAAGCGGG

GGCGGAAGTGGGGGCGGGTCAGGTCATCATCACCACCAT

CATTGA

4
ProC1193/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

16_1490_LIGHT_10GS_
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

His
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSGGGS

GGGSGHHHHHH

5
ProC1193/
CAAGGACAAAGTGGTTCCCGACACCCGTGCAGGCATGAC

ProC_mLm-
CCACATATAATCTGTTATAAGTTTGGTGGAGGCTCCTCCG

16_1490_LIGHT_10GS_
GCGGGTCTATCAGTTCCGGTCTCCTCAGCGGTCGCAGTGA

His
TAATATCGGCGGTTCTCAGGAACGCAGGTCACACGAGGT

DNA
AAATCCAGCCGCCCATTTGACTGGCGCTAATAGTTCTCTT

ACGGGTAGCGGTGGCCCTCTTCTGTGGGAAACGCAGTTG

GGCTTGGCTTTCCTTAGAGGTCTCAGCTATCACGACGGCG

CCCTCGTCGTTACAAAGGCCGGGTACTATTATATTTATTC

TAAGGTACAGCTTGGCGGGGGGGGTGCCCGCTGGGTCT

TGCATCTACGATCACTCATGGTCTCTACAAAAGAACACCA

AGGTATCCAGAAGAACTTGAGCTCCTCGTTAGCCAACAG

TCCCCCTGCGGACGGGCTACTTCCTCTAGCCGGGTATGGT

GGGATAGCAGTTTCCTTGGGGGGGTCGTGCATCTCGAGG

CTGGAGAGGAGGTAGTAGTCAGGGTCTTGGATGAGAGAT

TGGTAAGGCTTCGAGACGGTACAAGATCATACTTTGGGG

CCTTCATGGTGAGCGGGGGTGGCAGCGGCGGTGGCAGCG

GGCATCATCACCATCACCATTGA

6
ProC1188/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_LIGHT-10GS-
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

Strep
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

DNA
HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSGGGSGG

GSGSAWSHPQFEK

7
ProC1188/
CAGGAACGCAGGTCCCATGAAGTAAACCCGGCGGCCCAT

ProC_LIGHT-10GS-
CTTACGGGTGCAAATTCAAGCTTGACAGGCAGCGGAGGG

Strep
CCGCTCCTGTGGGAGACGCAACTTGGGCTTGCGTTTCTCC

DNA
GGGGCCTGTCATATCACGACGGTGCTCTTGTGGTAACGA

AAGCAGGGTACTATTATATATATAGCAAGGTTCAGTTGG

GTGGGGTTGGATGCCCGCTTGGACTCGCGTCCACTATTAC

TCACGGGTTGTATAAGAGGACACCGCGATACCCAGAGGA

GCTGGAACTCCTTGTTTCACAGCAGTCTCCTTGCGGGAGA

GCCACATCTTCATCCAGGGTCTGGTGGGACTCTTCTTTCT

TGGGCGGCGTTGTTCATCTGGAAGCGGGGGAAGAGGTTG

TAGTGAGGGTACTCGACGAGAGGCTGGTGAGGCTGCGAG

ACGGGACCCGCTCATATTTCGGAGCCTTCATGGTATCAGG

AGGGGGCTCCGGTGGGGGGTCAGGAAGCGCATGGTCACA

CCCTCAGTTCGAGAAATGA

8
ProC1192/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm16_1490_
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

LIGHT-10GS-Strep
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

Protein
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSGGGS

GGGSGSAWSHPQFEK

9
ProC1192/
CAAGGACAGAGTGGAAGTCGACACCCTTGTAGGCACGAC

ProC_mLm16_1490_
CCACATATAATCTGCTATAAATTTGGTGGGGGTTCCAGCG

LIGHT-10GS-Strep
GTGGAAGTATCAGCTCCGGCCTTCTTAGTGGCAGGAGTG

DNA
ACAATATTGGCGGATCTCAAGAGCGACGCAGTCACGAGG

TAAATCCTGCAGCACACTTGACAGGTGCTAACAGCTCACT

TACCGGAAGTGGGGGGCCGCTGTTGTGGGAGACGCAGCT

CGGGTTGGCCTTTCTTCGAGGGCTCTCTTATCACGACGGT

GCATTGGTGGTGACCAAAGCAGGGTATTACTACATATAC

TCTAAGGTGCAACTGGGTGGAGTAGGTTGTCCATTGGGG

CTCGCCTCTACAATAACTCATGGTCTGTATAAGCGAACCC

CGCGGTATCCCGAAGAGCTTGAACTCCTCGTCAGCCAGC

AATCTCCCTGTGGTCGGGCAACATCATCTAGCAGAGTGTG

GTGGGACTCCTCTTTTTTGGGTGGTGTAGTACATCTGGAA

GCGGGCGAAGAAGTGGTCGTCCGAGTGCTTGACGAACGA

CTCGTTAGACTGCGAGACGGAACTCGGAGCTACTTTGGA

GCTTTTATGGTTAGCGGTGGTGGTTCAGGAGGTGGGAGT

GGGAGTGCATGGTCACACCCGCAATTCGAGAAATGA

10
ProC1491/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_LIGHT-
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

1204DNI-HSA-His
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

Protein
HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGGGS

SGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIAFA

QYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLHT

LFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKDD

NPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPYF

YAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSHHHHHH

11
ProC1491/
CAGGAGAGGAGATCACATGAAGTCAACCCGGCCGCCCAT

ProC_LIGHT-
CTTACTGGTGCCAATAGTAGTCTTACAGGTTCTGGCGGAC

1204DNI-HSA-His
CCTTGCTTTGGGAGACCCAGCTGGGACTGGCTTTCCTTAG

DNA
AGGCCTGAGTTATCACGACGGGGCGTTGGTCGTTACTAA

AGCCGGGTATTACTATATATACTCTAAGGTTCAGCTCGGC

GGTGTAGGATGCCCACTGGGTCTTGCGTCTACAATTACAC

ATGGTCTGTATAAGAGGACTCCCAGATATCCAGAAGAAC

TGGAATTGCTTGTTTCCCAGCAATCTCCGTGCGGACGCGC

AACGAGCTCCAGTAGGGTGTGGTGGGACTCCAGCTTCCT

GGGTGGCGTTGTCCATTTGGAGGCGGGAGAGGAAGTAGT

GGTGCGGGTCCTTGATGAACGCCTTGTACGACTTCGGGAC

GGTACAAGAAGCTACTTTGGGGCTTTCATGGTATCCAGCG

CCGGGGGCGGAAGCAGCGGCGGCAGCTTAAGCGGCAGA

AGCGACAACATCGGCAGCGATGCACATAAAAGTGAGGTG

GCCCACCGCTTTAAAGACCTCGGCGAGGAGAACTTCAAG

GCACTCGTACTTATTGCCTTTGCACAATACCTGCAGCAAT

GTCCGTTTGAAGATCATGTCAAGCTCGTAAATGAAGTGA

CAGAGTTCGCTAAGACCTGTGTAGCTGACGAAAGTGCCG

AAAACTGCGACAAATCATTGCATACATTGTTCGGCGACA

AGCTTTGTACAGTTGCCACGCTCCGCGAGACATACGGCG

AAATGGCCGATTGTTGTGCGAAACAGGAACCCGAAAGAA

ATGAGTGCTTCTTGCAACACAAAGACGATAATCCCAATCT

TCCGCGACTGGTGAGACCCGAAGTAGATGTAATGTGCAC

AGCTTTTCATGACAATGAGGAAACCTTTCTTAAAAAATAT

CTGTACGAAATCGCCCGCCGACACCCGTATTTCTATGCCC

CAGAGCTGTTGTTTTTCGCAAAGCGCTACAAGGCAGCGTT

TACCGAATGCTGCCAGGCCGCTGATAAAGCCGCTTGTCTG

CTGCCTAAGCTTGATGAGCTTCGCGACGAGGGTAAGGCT

TCCAGCGCTAAACAACGCCTGAAGTGTGCATCTTTGCAA

AAATTTGGTGAACGAGCCTTCAAGGCTTGGGCTGTTGCCA

GGCTGAGTCAACGGTTCCCGAAGGCGGAGTTTGCGGAGG

TTTCCAAGTTGGTAACGGACCTGACAAAGGTACATACCG

AATGCTGCCATGGCGACCTGTTGGAGTGCGCCGATGATC

GAGCGGATCTTGCCAAGTATATTTGCGAAAACCAAGACT

CCATTTCCAGTAAACTTAAGGAGTGTTGTGAGAAACCTCT

CCTTGAAAAGAGCCATTGTATAGCGGAGGTCGAAAACGA

TGAAATGCCCGCTGATCTGCCGTCACTCGCTGCTGACTTC

GTTGAATCCAAGGATGTATGTAAAAACTATGCCGAAGCT

AAGGACGTCTTTCTTGGAATGTTCTTGTATGAATACGCCC

GACGGCATCCTGACTATTCAGTTGTGCTCCTTCTTCGATT

GGCTAAAACTTATGAGACGACACTTGAAAAGTGTTGTGC

CGCCGCCGACCCACATGAGTGCTACGCTAAGGTTTTCGA

CGAATTTAAGCCCTTGGTTGAAGAACCGCAGAATCTCATT

AAGCAAAATTGTGAGCTCTTTGAACAACTCGGTGAATAC

AAATTTCAGAACGCGCTTCTGGTTAGATATACGAAGAAA

GTGCCACAGGTGAGCACCCCTACATTGGTTGAGGTCAGT

AGGAACCTCGGCAAGGTGGGATCTAAGTGCTGCAAACAC

CCGGAGGCAAAGAGAATGCCTTGCGCTGAGGATTATCTC

TCAGTGGTTCTGAATCAGCTTTGCGTTCTTCACGAAAAGA

CTCCCGTCAGCGACCGAGTCACGAAGTGCTGTACCGAGA

GCCTTGTTAATAGACGACCTTGCTTCTCCGCGCTTGAGGT

GGATGAGACCTACGTCCCAAAGGAATTCAACGCCGAGAC

GTTCACTTTCCATGCCGATATTTGCACCTTGTCAGAAAAG

GAGCGACAGATAAAAAAGCAAACTGCTTTGGTGGAGCTG

GTTAAGCATAAGCCTAAAGCGACGAAGGAACAGCTCAAA

GCCGTAATGGATGATTTCGCTGCCTTCGTGGAGAAATGTT

GTAAGGCCGATGACAAGGAAACCTGCTTCGCTGAAGAGG

GTAAAAAGCTCGTCGCCGCTAGTCAGGCGGCACTTGGTTT

GAGCCACCATCACCACCACCACtga

12
ProC1492/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRCDNIG

ProC_mLm16-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

LIGHT-1204DNI-
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

HSA-His (1490DNI
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

has S to C mutation)
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGG

Protein
GSSGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIA

FAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSL

HTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHK

DDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHP

YFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDE

GKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEF

AEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQ

DSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFV

ESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLA

KTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQN

CELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGK

VGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDR

VTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADIC

TLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAF

VEKCCKADDKETCFAEEGKKLVAASQAALGLSHHHHHH

13
ProC1492/
CAGGGCCAGTCTGGATCCAGACACCCATGCAGACACGAC

ProC_mLm16-
CCCCACATCATCTGTTACAAATTCGGCGGAGGCAGCTCC

LIGHT-1204DNI-
GGCGGCAGCATCTCCAGCGGACTGCTGAGCGGCAGAtGC

HSA-His (1490DNI
GATAACATCGGCGGAAGCCAGGAGAGGAGATCACATGA

has S to C mutation)
AGTCAACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGT

DNA
CTTACAGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGC

TGGGACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGG

GGCGTTGGTCGTTACTAAAGCCGGGTATTACTATATATAC

TCTAAGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTC

TTGCGTCTACAATTACACATGGTCTGTATAAGAGGACTCC

CAGATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCA

ATCTCCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTG

GTGGGACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAG

GCGGGAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGC

CTTGTACGACTTCGGGACGGTACAAGAAGCTACTTTGGG

GCTTTCATGGTATCCAGCGCCGGGGGCGGAAGCAGCGGC

GGCAGCTTAAGCGGCAGAAGCGACAACATCGGCAGCGAT

GCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTC

GGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCCTTTG

CACAATACCTGCAGCAATGTCCGTTTGAAGATCATGTCAA

GCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCTGTGT

AGCTGACGAAAGTGCCGAAAACTGCGACAAATCATTGCA

TACATTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTC

CGCGAGACATACGGCGAAATGGCCGATTGTTGTGCGAAA

CAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACACAAA

GACGATAATCCCAATCTTCCGCGACTGGTGAGACCCGAA

GTAGATGTAATGTGCACAGCTTTTCATGACAATGAGGAA

ACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGCCGAC

ACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAA

GCGCTACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGC

TGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTT

CGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTG

AAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCA

AGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGA

AGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACC

TGACAAAGGTACATACCGAATGtTGCCATGGCGACCTGTT

GGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTATAT

TTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAGGA

GTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATA

GCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTGCCG

TCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTA

AAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTT

CTTGTATGAATACGCCCGACGGCATCCTGACTATTCAGTT

GTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACGACAC

TTGAAAAGTGTTGTGCCGCGGCGGACCCACATGAGTGCT

ACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGA

ACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAA

CAACTCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTA

GATATACGAAGAAAGTGCCACAGGTGAGCACCCCTACAT

TGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTA

AGTGCTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCG

CTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGT

TCTTCACGAAAAGACTCCCGTCAGCGACCGAGTCACGAA

GTGCTGTACCGAGAGCCTTGTTAATAGACGACCTTGCTTC

TCCGCGCTTGAGGTGGATGAGACCTACGTCCCAAAGGAA

TTCAACGCCGAGACGTTCACTTTCCATGCCGATATTTGCA

CCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCAAACTG

CTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGA

AGGAACAGCTCAAAGCCGTAATGGATGATTTCGCTGCCT

TCGTGGAGAAATGTTGTAAGGCCGATGACAAGGAAACCT

GCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTC

AGGCGGCACTTGGTTTGAGCCACCATCACCACCACCACtga

14
ProC1655/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm16-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

LIGHT-1204DNI-
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

HSA-His 1490
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGG

GSSGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIA

FAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSL

HTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHK

DDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHP

YFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDE

GKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEF

AEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQ

DSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFV

ESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLA

KTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQN

CELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGK

VGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDR

VTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADIC

TLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAF

VEKCCKADDKETCFAEEGKKLVAASQAALGLSHHHHHH

15
ProC1655/
CAGGGCCAGTCTGGATCCAGACACCCATGCAGACACGAC

ProC_mLm16-
CCCCACATCATCTGTTACAAATTCGGCGGAGGCAGCTCC

LIGHT-1204DNI-
GGCGGCAGCATCTCCAGCGGACTGCTGAGCGGCAGAAGC

HSA-His 1490
GATAACATCGGCGGAAGCCAGGAGAGGAGATCACATGA

DNA
AGTCAACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGT

CTTACAGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGC

TGGGACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGG

GGCGTTGGTCGTTACTAAAGCCGGGTATTACTATATATAC

TCTAAGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTC

TTGCGTCTACAATTACACATGGTCTGTATAAGAGGACTCC

CAGATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCA

ATCTCCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTG

GTGGGACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAG

GCGGGAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGC

CTTGTACGACTTCGGGACGGTACAAGAAGCTACTTTGGG

GCTTTCATGGTATCCAGCGCCGGGGGCGGAAGCAGCGGC

GGCAGCTTAAGCGGCAGAAGCGAtAACATCGGCAGCGAT

GCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTC

GGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCCTTTG

CACAATACCTGCAGCAATGTCCGTTTGAAGATCATGTCAA

GCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCTGTGT

AGCTGACGAAAGTGCCGAAAACTGCGACAAATCATTGCA

TACATTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTC

CGCGAGACATACGGCGAAATGGCCGATTGTTGTGCGAAA

CAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACACAAA

GACGATAATCCCAATCTTCCGCGACTGGTGAGACCCGAA

GTAGATGTAATGTGCACAGCTTTTCATGACAATGAGGAA

ACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGCCGAC

ACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAA

GCGCTACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGC

TGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTT

CGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTG

AAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCA

AGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGA

AGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACC

TGACAAAGGTACATACCGAATGtTGCCATGGCGACCTGTT

GGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTATAT

TTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAGGA

GTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATA

GCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTGCCG

TCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTA

AAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTT

CTTGTATGAATACGCCCGACGGCATCCTGACTATTCAGTT

GTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACGACAC

TTGAAAAGTGTTGTGCCGCGGCGGACCCACATGAGTGCT

ACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGA

ACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAA

CAACTCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTA

GATATACGAAGAAAGTGCCACAGGTGAGCACCCCTACAT

TGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTA

AGTGCTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCG

CTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGT

TCTTCACGAAAAGACTCCCGTCAGCGACCGAGTCACGAA

GTGCTGTACCGAGAGCCTTGTTAATAGACGACCTTGCTTC

TCCGCGCTTGAGGTGGATGAGACCTACGTCCCAAAGGAA

TTCAACGCCGAGACGTTCACTTTCCATGCCGATATTTGCA

CCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCAAACTG

CTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGA

AGGAACAGCTCAAAGCCGTAATGGATGATTTCGCTGCCT

TCGTGGAGAAATGTTGTAAGGCCGATGACAAGGAAACCT

GCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTC

AGGCGGCACTTGGTTTGAGCCACCATCACCACCACCACtga

16
ProC1499/
DAHKSEVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVK

ProC_HSA-21GS-
LVNEVTEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRE

1204DNI-LIGHT
TYGEMADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDV

Protein
MCTAFHDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKA

AFTECCQAADKAACLLPKLDELRDEGKASSAKQRLKCASL

QKFGERAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHT

ECCHGDLLECADDRADLAKYICENQDSISSKLKECCEKPLLE

KSHCIAEVENDEMPADLPSLAADFVESKDVCKNYAEAKDV

FLGMFLYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADP

HECYAKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNAL

LVRYTKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMP

CAEDYLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCF

SALEVDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALV

ELVKHKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAE

EGKKLVAASQAALGLSSAGGGSSGGSLSGRSDNIGSQERRS

HEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRGLSYHD

GALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGLYKRTP

RYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVVHLEAG

EEVVVRVLDERLVRLRDGTRSYFGAFMV

17
ProC1499/
GATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGAC

ProC_HSA-21GS-
CTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCCT

1204DNI-LIGHT
TTGCACAATACCTGCAGCAATGTCCGTTTGAAGATCATGT

DNA
CAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCTG

TGTAGCTGACGAAAGTGCCGAAAACTGCGACAAATCATT

GCATACATTGTTCGGCGACAAGCTTTGTACAGTTGCCACG

CTCCGCGAGACATACGGCGAAATGGCCGATTGTTGTGCG

AAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACAC

AAAGACGATAATCCCAATCTTCCGCGACTGGTGAGACCC

GAAGTAGATGTAATGTGCACAGCTTTTCATGACAATGAG

GAAACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGCC

GACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGC

AAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCAGGCC

GCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGC

TTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGCC

TGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTT

CAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCC

GAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGA

CCTGACAAAGGTACATACCGAATGCTGCCATGGCGACCT

GTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTA

TATTTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAG

GAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGT

ATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTG

CCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTAT

GTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAA

TGTTCTTGTATGAATACGCCCGACGGCATCCTGACTATTC

AGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACG

ACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACATGAG

TGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTG

AAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCT

TTGAACAACTCGGTGAATACAAATTTCAGAACGCGCTTCT

GGTTAGATATACGAAGAAAGTGCCACAGGTGAGCACCCC

TACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGG

ATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATGCC

TTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTT

TGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGTC

ACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACCT

TGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCAA

AGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGATAT

TTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCA

AACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGC

GACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTCGC

TGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAGGA

AACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGC

TAGTCAGGCGGCACTTGGTTTGTCCAGCGCCGGGGGCGG

AAGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGACAACA

TCGGCAGCCAGGAGAGACGGAGCCACGAGGTGAACCCC

GCTGCCCACCTGACCGGCGCCAACAGCAGTCTGACCGGC

AGCGGCGGCCCTCTGCTGTGGGAGACACAGCTGGGCCTG

GCCTTTCTGAGAGGCCTGTCCTACCACGACGGCGCCCTGG

TCGTGACCAAGGCCGGCTACTACTACATCTACAGCAAGG

TGCAGCTGGGAGGCGTGGGCTGCCCTCTGGGCCTGGCAT

CTACCATCACGCACGGCCTGTACAAGCGGACCCCTAGAT

ATCCTGAGGAACTGGAACTCCTGGTGTCCCAGCAGAGCC

CTTGCGGCAGAGCTACAAGCAGCTCAAGAGTGTGGTGGG

ACAGCAGCTTCCTGGGCGGAGTGGTCCACCTGGAAGCTG

GAGAAGAAGTGGTGGTCCGGGTGCTGGACGAGAGACTCG

TGAGGCTGAGAGACGGAACAAGAAGCTACTTCGGCGCTT

TTATGGTGtga

18
ProC1495/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_LIGHT-
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

1204DNI-HSA-cMyc
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

Protein
HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGGGS

SGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIAFA

QYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLHT

LFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKDD

NPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPYF

YAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISEE

DL

19
ProC1495/
CAGGAGAGGAGATCACATGAAGTCAACCCGGCCGCCCAT

ProC_LIGHT-
CTTACTGGTGCCAATAGTAGTCTTACAGGTTCTGGCGGAC

1204DNI-HSA-cMyc
CCTTGCTTTGGGAGACCCAGCTGGGACTGGCTTTCCTTAG

DNA
AGGCCTGAGTTATCACGACGGGGCGTTGGTCGTTACTAA

AGCCGGGTATTACTATATATACTCTAAGGTTCAGCTCGGC

GGTGTAGGATGCCCACTGGGTCTTGCGTCTACAATTACAC

ATGGTCTGTATAAGAGGACTCCCAGATATCCAGAAGAAC

TGGAATTGCTTGTTTCCCAGCAATCTCCGTGCGGACGCGC

AACGAGCTCCAGTAGGGTGTGGTGGGACTCCAGCTTCCT

GGGTGGCGTTGTCCATTTGGAGGCGGGAGAGGAAGTAGT

GGTGCGGGTCCTTGATGAACGCCTTGTACGACTTCGGGAC

GGTACAAGAAGCTACTTTGGGGCTTTCATGGTATCCAGCG

CCGGGGGCGGAAGCAGCGGCGGCAGCTTAAGCGGCAGA

AGCGACAACATCGGCAGCGATGCACATAAAAGTGAGGTG

GCCCACCGCTTTAAAGACCTCGGCGAGGAGAACTTCAAG

GCACTCGTACTTATTGCCTTTGCACAATACCTGCAGCAAT

GTCCGTTTGAAGATCATGTCAAGCTCGTAAATGAAGTGA

CAGAGTTCGCTAAGACCTGTGTAGCTGACGAAAGTGCCG

AAAACTGCGACAAATCATTGCATACATTGTTCGGCGACA

AGCTTTGTACAGTTGCCACGCTCCGCGAGACATACGGCG

AAATGGCCGATTGTTGTGCGAAACAGGAACCCGAAAGAA

ATGAGTGCTTCTTGCAACACAAAGACGATAATCCCAATCT

TCCGCGACTGGTGAGACCCGAAGTAGATGTAATGTGCAC

AGCTTTTCATGACAATGAGGAAACCTTTCTTAAAAAATAT

CTGTACGAAATCGCCCGCCGACACCCGTATTTCTATGCCC

CAGAGCTGTTGTTTTTCGCAAAGCGCTACAAGGCAGCGTT

TACCGAATGCTGCCAGGCCGCTGATAAAGCCGCTTGTCTG

CTGCCTAAGCTTGATGAGCTTCGCGACGAGGGTAAGGCT

TCCAGCGCTAAACAACGCCTGAAGTGTGCATCTTTGCAA

AAATTTGGTGAACGAGCCTTCAAGGCTTGGGCTGTTGCCA

GGCTGAGTCAACGGTTCCCGAAGGCGGAGTTTGCGGAGG

TTTCCAAGTTGGTAACGGACCTGACAAAGGTACATACCG

AATGCTGCCATGGCGACCTGTTGGAGTGCGCCGATGATC

GAGCGGATCTTGCCAAGTATATTTGCGAAAACCAAGACT

CCATTTCCAGTAAACTTAAGGAGTGTTGTGAGAAACCTCT

CCTTGAAAAGAGCCATTGTATAGCGGAGGTCGAAAACGA

TGAAATGCCCGCTGATCTGCCGTCACTCGCTGCTGACTTC

GTTGAATCCAAGGATGTATGTAAAAACTATGCCGAAGCT

AAGGACGTCTTTCTTGGAATGTTCTTGTATGAATACGCCC

GACGGCATCCTGACTATTCAGTTGTGCTCCTTCTTCGATT

GGCTAAAACTTATGAGACGACACTTGAAAAGTGTTGTGC

CGCCGCCGACCCACATGAGTGCTACGCTAAGGTTTTCGA

CGAATTTAAGCCCTTGGTTGAAGAACCGCAGAATCTCATT

AAGCAAAATTGTGAGCTCTTTGAACAACTCGGTGAATAC

AAATTTCAGAACGCGCTTCTGGTTAGATATACGAAGAAA

GTGCCACAGGTGAGCACCCCTACATTGGTTGAGGTCAGT

AGGAACCTCGGCAAGGTGGGATCTAAGTGCTGCAAACAC

CCGGAGGCAAAGAGAATGCCTTGCGCTGAGGATTATCTC

TCAGTGGTTCTGAATCAGCTTTGCGTTCTTCACGAAAAGA

CTCCCGTCAGCGACCGAGTCACGAAGTGCTGTACCGAGA

GCCTTGTTAATAGACGACCTTGCTTCTCCGCGCTTGAGGT

GGATGAGACCTACGTCCCAAAGGAATTCAACGCCGAGAC

GTTCACTTTCCATGCCGATATTTGCACCTTGTCAGAAAAG

GAGCGACAGATAAAAAAGCAAACTGCTTTGGTGGAGCTG

GTTAAGCATAAGCCTAAAGCGACGAAGGAACAGCTCAAA

GCCGTAATGGATGATTTCGCTGCCTTCGTGGAGAAATGTT

GTAAGGCCGATGACAAGGAAACCTGCTTCGCTGAAGAGG

GTAAAAAGCTCGTCGCCGCTAGTCAGGCGGCACTTGGTTT

GAGTGGTGGAGAACAAAAACTCATTTCCGAGGAAGATCT

Ttga

20
ProC1496/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm16-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

LIGHT-1204DNI-
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

HSA-cMyc
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGG

GSSGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIA

FAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSL

HTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHK

DDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHP

YFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDE

GKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEF

AEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQ

DSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFV

ESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLA

KTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQN

CELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGK

VGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDR

VTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADIC

TLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAF

VEKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISE

EDL

21
ProC1496/
CAGGGACAGTCCGGATCTAGGCATCCATGTCGGCATGAC

ProC_mLm16-
CCACATATCATATGCTACAAATTCGGTGGAGGATCTTCTG

LIGHT-1204DNI-
GAGGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGA

HSA-cMyc
CAATATTGGTGGCTCCCAGGAGAGGAGATCACATGAAGT

DNA
CAACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGTCTT

ACAGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGCTG

GGACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGGG

GCGTTGGTCGTTACTAAAGCCGGGTATTACTATATATACT

CTAAGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTCT

TGCGTCTACAATTACACATGGTCTGTATAAGAGGACTCCC

AGATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCAAT

CTCCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTGGT

GGGACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAGGC

GGGAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGCCT

TGTACGACTTCGGGACGGTACAAGAAGCTACTTTGGGGC

TTTCATGGTATCCAGCGCCGGGGGCGGAAGCAGCGGCGG

CAGCTTAAGCGGCAGAAGCGACAACATCGGCAGCGATGC

ACATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTCGG

CGAGGAGAACTTCAAGGCACTCGTACTTATTGCCTTTGCA

CAATACCTGCAGCAATGTCCGTTTGAAGATCATGTCAAGC

TCGTAAATGAAGTGACAGAGTTCGCTAAGACCTGTGTAG

CTGACGAAAGTGCCGAAAACTGCGACAAATCATTGCATA

CATTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTCCG

CGAGACATACGGCGAAATGGCCGATTGTTGTGCGAAACA

GGAACCCGAAAGAAATGAGTGCTTCTTGCAACACAAAGA

CGATAATCCCAATCTTCCGCGACTGGTGAGACCCGAAGT

AGATGTAATGTGCACAGCTTTTCATGACAATGAGGAAAC

CTTTCTTAAAAAATATCTGTACGAAATCGCCCGCCGACAC

CCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGC

GCTACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGCTG

ATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCG

CGACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAA

GTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAG

GCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAG

GCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTG

ACAAAGGTACATACCGAATGCTGtCATGGCGACCTGTTGG

AGTGCGCCGATGATCGAGCGGATCTTGCCAAGTATATTTG

CGAAAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTG

TTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCG

GAGGTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCA

CTCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAA

ACTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTT

GTATGAATACGCCCGACGGCATCCTGACTATTCAGTTGTG

CTCCTTCTTCGATTGGCTAAAACTTATGAGACGACACTTG

AAAAGTGTTGTGCCGCCGCCGACCCACATGAGTGCTACG

CTAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACC

GCAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACA

ACTCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGA

TATACGAAGAAAGTGCCACAGGTGAGCACCCCTACATTG

GTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAG

TGCTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCT

GAGGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTC

TTCACGAAAAGACTCCCGTCAGCGACCGAGTCACGAAGT

GCTGTACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTC

CGCGCTTGAGGTGGATGAGACCTACGTCCCAAAGGAATT

CAACGCCGAGACGTTCACTTTCCATGCCGATATTTGCACC

TTGTCAGAAAAGGAGCGACAGATAAAAAAGCAAACTGCT

TTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAG

GAACAGCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCG

TGGAGAAATGTTGTAAGGCCGATGACAAGGAAACCTGCT

TCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGG

CGGCACTTGGTTTGAGTGGTGGAGAACAAAAACTCATTT

CCGAGGAAGATCTTtga

22
ProC1184/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_LIGHT_
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

21linker_HSA-cMyc
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

Protein
HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGGGS

SGGSSAGGGSSGGSDAHKSEVAHRFKDLGEENFKALVLIAF

AQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLH

TLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKD

DNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPY

FYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISEE

DL

23
ProC1184/
CAGGAGAGGCGCTCTCATGAAGTAAACCCCGCCGCGCAC

ProC_LIGHT_
CTTACCGGTGCGAATTCCAGCCTTACGGGCTCCGGGGGC

21linker_HSA-cMyc
CCTCTTCTGTGGGAAACCCAACTCGGGCTGGCGTTTCTCA

DNA
GGGGTCTCAGTTACCACGACGGCGCGCTTGTCGTTACTAA

AGCGGGCTACTACTATATCTACTCCAAGGTACAGCTCGGT

GGTGTAGGATGTCCGCTTGGGCTTGCCTCTACCATCACGC

ACGGTCTCTATAAAAGAACCCCAAGATACCCCGAAGAGT

TGGAACTGCTTGTTTCTCAACAGTCCCCTTGTGGTCGGGC

AACCAGTTCATCTCGGGTGTGGTGGGATAGTAGCTTTCTC

GGAGGAGTAGTCCACCTGGAAGCTGGGGAAGAGGTAGTC

GTCCGGGTACTCGATGAACGGCTCGTGCGCCTCCGAGAT

GGGACCCGGTCTTACTTTGGGGCTTTCATGGTTAGCTCTG

CGGGGGGAGGAAGCTCCGGGGGTAGTTCCGCCGGCGGCG

GATCTAGTGGCGGTTCTGATGCTCATAAAAGTGAGGTCG

CGCACAGATTCAAAGACCTCGGCGAGGAAAACTTTAAAG

CCCTCGTATTGATAGCTTTCGCCCAGTACCTCCAGCAGTG

CCCATTCGAGGATCACGTGAAACTCGTGAATGAAGTAAC

GGAATTTGCCAAAACGTGCGTGGCCGACGAGAGTGCCGA

AAATTGCGACAAGTCACTTCACACCCTTTTTGGTGACAAA

TTGTGTACTGTGGCGACGCTTAGGGAAACATACGGAGAA

ATGGCCGATTGCTGTGCCAAACAAGAGCCTGAAAGAAAC

GAATGCTTTCTTCAGCACAAAGACGATAACCCTAACTTGC

CGAGACTGGTGAGACCTGAAGTAGACGTCATGTGTACCG

CGTTCCATGACAACGAAGAGACTTTCTTGAAAAAATACC

TTTATGAAATAGCACGGAGGCACCCTTATTTTTACGCTCC

AGAGCTCCTCTTCTTTGCTAAACGGTACAAAGCGGCGTTT

ACCGAATGTTGCCAAGCTGCGGATAAAGCTGCATGTCTTC

TCCCGAAGTTGGATGAGCTGAGAGATGAGGGTAAAGCGT

CTTCCGCTAAACAACGACTTAAATGCGCTTCTCTGCAGAA

ATTTGGCGAACGAGCGTTCAAAGCCTGGGCCGTTGCGCG

CCTTTCACAGCGGTTTCCGAAAGCCGAGTTCGCCGAGGTT

TCAAAGCTGGTTACGGACTTGACAAAGGTGCATACAGAA

TGCTGCCACGGAGACCTGCTGGAGTGCGCCGATGATCGC

GCTGATTTGGCTAAATATATTTGCGAAAATCAGGACAGC

ATCAGCTCCAAGTTGAAGGAGTGTTGTGAAAAACCGCTG

CTGGAGAAGTCACACTGCATAGCCGAGGTGGAAAACGAC

GAGATGCCGGCAGACCTCCCCAGCCTTGCCGCGGATTTC

GTCGAATCAAAGGATGTATGCAAAAATTACGCGGAAGCA

AAAGATGTATTTCTGGGAATGTTCCTGTACGAGTACGCTA

GGCGACATCCCGACTACAGCGTTGTTCTGCTCTTGAGACT

TGCGAAGACGTACGAGACTACGCTCGAGAAGTGCTGTGC

AGCTGCGGACCCCCATGAGTGTTATGCTAAAGTCTTCGAC

GAATTTAAGCCTTTGGTGGAAGAGCCACAGAACCTGATC

AAACAAAATTGTGAACTGTTCGAACAATTGGGGGAGTAT

AAATTTCAGAACGCTCTCCTTGTTCGGTATACAAAAAAAG

TACCGCAGGTAAGTACGCCGACACTCGTGGAAGTAAGCA

GGAACCTCGGAAAGGTTGGATCAAAATGCTGCAAGCATC

CGGAGGCTAAGCGCATGCCATGCGCTGAGGATTATCTTTC

AGTGGTCCTGAACCAATTGTGCGTGTTGCACGAGAAAAC

TCCAGTAAGCGATAGAGTTACCAAATGTTGTACAGAGAG

CCTGGTTAATCGACGACCTTGCTTCAGCGCCTTGGAAGTC

GATGAGACGTATGTGCCGAAGGAATTTAACGCCGAAACT

TTCACTTTTCATGCAGATATCTGTACATTGAGCGAAAAGG

AAAGGCAAATTAAAAAACAAACTGCGCTTGTGGAATTGG

TCAAGCACAAGCCTAAAGCCACAAAGGAACAGCTCAAA

GCGGTAATGGACGATTTTGCGGCGTTCGTAGAGAAGTGT

TGCAAGGCGGACGATAAAGAAACGTGCTTTGCTGAGGAG

GGAAAAAAGCTTGTTGCTGCCAGTCAAGCGGCGCTTGGC

TTGAGTGGTGGAGAACAAAAACTCATTTCCGAGGAAGAT

CTTTGA

24
ProC1486/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_mhLIGHT_
LSYHDGALVVTKTGYYYIYSKVQLGGVGCPLGLAGTITHGL

1204DNI_HSA-cMyc
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

Protein
HLEAGEEVVVRVLGKRLVRLRDGTRSYFGAFMVSSAGGGS

SGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIAFA

QYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLHT

LFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKDD

NPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPYF

YAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISEE

DL

25
ProC1486/
CAAGAACGCCGATCACACGAAGTGAACCCTGCTGCTCAC

ProC_mhLIGHT_
TTGACTGGAGCTAACTCCAGCCTTACGGGGAGCGGGGGT

1204DNI_HSA-cMyc
CCTTTGCTCTGGGAAACGCAGCTGGGTCTCGCGTTTCTTA

DNA
GAGGGCTGAGTTATCACGATGGCGCCTTGGTCGTCACGA

AGACTGGGTACTACTATATTTATAGTAAGGTACAGTTGGG

GGGAGTGGGGTGCCCTCTCGGCCTGGCTGGGACGATCAC

GCATGGGCTCTACAAGCGCACGCCTAGGTATCCGGAGGA

GTTGGAACTGTTGGTCTCACAGCAGTCCCCGTGCGGGCG

AGCGACTTCCTCCAGTAGAGTGTGGTGGGACTCTAGCTTT

CTCGGGGGAGTGGTTCATCTTGAGGCAGGAGAGGAAGTG

GTGGTACGGGTTTTGGGCAAGAGATTGGTGAGACTGCGG

GATGGTACAAGATCTTATTTTGGTGCTTTCATGGTCTCCA

GCGCCGGGGGCGGAAGCAGCGGCGGCAGCTTAAGCGGC

AGAAGCGACAACATCGGCAGCGATGCTCATAAAAGTGAG

GTCGCGCACAGATTCAAAGACCTCGGCGAGGAAAACTTT

AAAGCCCTCGTATTGATAGCTTTCGCCCAGTACCTCCAGC

AGTGCCCATTCGAGGATCACGTGAAACTCGTGAATGAAG

TAACGGAATTTGCCAAAACGTGCGTGGCCGACGAGAGTG

CCGAAAATTGCGACAAGTCACTTCACACCCTTTTTGGTGA

CAAATTGTGTACTGTGGCGACGCTTAGGGAAACATACGG

AGAAATGGCCGATTGCTGTGCCAAACAAGAGCCTGAAAG

AAACGAATGCTTTCTTCAGCACAAAGACGATAACCCTAA

CTTGCCGAGACTGGTGAGACCTGAAGTAGACGTCATGTG

TACCGCGTTCCATGACAACGAAGAGACTTTCTTGAAAAA

ATACCTTTATGAAATAGCACGGAGGCACCCTTATTTTTAC

GCTCCAGAGCTCCTCTTCTTTGCTAAACGGTACAAAGCGG

CGTTTACCGAATGTTGCCAAGCTGCGGATAAAGCTGCAT

GTCTTCTCCCGAAGTTGGATGAGCTGAGAGATGAGGGTA

AAGCGTCTTCCGCTAAACAACGACTTAAATGCGCTTCTCT

GCAGAAATTTGGCGAACGAGCGTTCAAAGCCTGGGCCGT

TGCGCGCCTTTCACAGCGGTTTCCGAAAGCCGAGTTCGCC

GAGGTTTCAAAGCTGGTTACGGACTTGACAAAGGTGCAT

ACAGAATGCTGCCACGGAGACCTGCTGGAGTGCGCCGAT

GATCGCGCTGATTTGGCTAAATATATTTGCGAAAATCAGG

ACAGCATCAGCTCCAAGTTGAAGGAGTGTTGTGAAAAAC

CGCTGCTGGAGAAGTCACACTGCATAGCCGAGGTGGAAA

ACGACGAGATGCCGGCAGACCTCCCCAGCCTTGCCGCGG

ATTTCGTCGAATCAAAGGATGTATGCAAAAATTACGCGG

AAGCAAAAGATGTATTTCTGGGAATGTTCCTGTACGAGT

ACGCTAGGCGACATCCCGACTACAGCGTTGTTCTGCTCTT

GAGACTTGCGAAGACGTACGAGACTACGCTCGAGAAGTG

CTGTGCAGCTGCGGACCCCCATGAGTGTTATGCTAAAGTC

TTCGACGAATTTAAGCCTTTGGTGGAAGAGCCACAGAAC

CTGATCAAACAAAATTGTGAACTGTTCGAACAATTGGGG

GAGTATAAATTTCAGAACGCTCTCCTTGTTCGGTATACAA

AAAAAGTACCGCAGGTAAGTACGCCGACACTCGTGGAAG

TAAGCAGGAACCTCGGAAAGGTTGGATCAAAATGCTGCA

AGCATCCGGAGGCTAAGCGCATGCCATGCGCTGAGGATT

ATCTTTCAGTGGTCCTGAACCAATTGTGCGTGTTGCACGA

GAAAACTCCAGTAAGCGATAGAGTTACCAAATGTTGTAC

AGAGAGCCTGGTTAATCGACGACCTTGCTTCAGCGCCTTG

GAAGTCGATGAGACGTATGTGCCGAAGGAATTTAACGCC

GAAACTTTCACTTTTCATGCAGATATCTGTACATTGAGCG

AAAAGGAAAGGCAAATTAAAAAACAAACTGCGCTTGTGG

AATTGGTCAAGCACAAGCCTAAAGCCACAAAGGAACAGC

TCAAAGCGGTAATGGACGATTTTGCGGCGTTCGTAGAGA

AGTGTTGCAAGGCGGACGATAAAGAAACGTGCTTTGCTG

AGGAGGGAAAAAAGCTTGTTGCTGCCAGTCAAGCGGCGC

TTGGCTTGAGTGGTGGAGAACAAAAACTCATTTCCGAGG

AAGATCTTTGA

26
ProC1483/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_mhLIGHT_
LSYHDGALVVTKTGYYYIYSKVQLGGVGCPLGLAGTITHGL

21linker_HSA-cMyc
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

Protein
HLEAGEEVVVRVLGKRLVRLRDGTRSYFGAFMVSSAGGGS

SGGSSAGGGSSGGSDAHKSEVAHRFKDLGEENFKALVLIAF

AQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLH

TLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKD

DNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPY

FYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISEE

DL

27
ProC1483/
CAAGAACGCCGATCACACGAAGTGAACCCTGCTGCTCAC

ProC_mhLIGHT_
TTGACTGGAGCTAACTCCAGCCTTACGGGGAGCGGGGGT

21linker_HSA-cMyc
CCTTTGCTCTGGGAAACGCAGCTGGGTCTCGCGTTTCTTA

DNA
GAGGGCTGAGTTATCACGATGGCGCCTTGGTCGTCACGA

AGACTGGGTACTACTATATTTATAGTAAGGTACAGTTGGG

GGGAGTGGGGTGCCCTCTCGGCCTGGCTGGGACGATCAC

GCATGGGCTCTACAAGCGCACGCCTAGGTATCCGGAGGA

GTTGGAACTGTTGGTCTCACAGCAGTCCCCGTGCGGGCG

AGCGACTTCCTCCAGTAGAGTGTGGTGGGACTCTAGCTTT

CTCGGGGGAGTGGTTCATCTTGAGGCAGGAGAGGAAGTG

GTGGTACGGGTTTTGGGCAAGAGATTGGTGAGACTGCGG

GATGGTACAAGATCTTATTTTGGTGCTTTCATGGTCAGCT

CTGCGGGGGGAGGAAGCTCCGGGGGTAGTTCCGCCGGCG

GCGGATCTAGTGGCGGTTCTGATGCTCATAAAAGTGAGG

TCGCGCACAGATTCAAAGACCTCGGCGAGGAAAACTTTA

AAGCCCTCGTATTGATAGCTTTCGCCCAGTACCTCCAGCA

GTGCCCATTCGAGGATCACGTGAAACTCGTGAATGAAGT

AACGGAATTTGCCAAAACGTGCGTGGCCGACGAGAGTGC

CGAAAATTGCGACAAGTCACTTCACACCCTTTTTGGTGAC

AAATTGTGTACTGTGGCGACGCTTAGGGAAACATACGGA

GAAATGGCCGATTGCTGTGCCAAACAAGAGCCTGAAAGA

AACGAATGCTTTCTTCAGCACAAAGACGATAACCCTAAC

TTGCCGAGACTGGTGAGACCTGAAGTAGACGTCATGTGT

ACCGCGTTCCATGACAACGAAGAGACTTTCTTGAAAAAA

TACCTTTATGAAATAGCACGGAGGCACCCTTATTTTTACG

CTCCAGAGCTCCTCTTCTTTGCTAAACGGTACAAAGCGGC

GTTTACCGAATGTTGCCAAGCTGCGGATAAAGCTGCATGT

CTTCTCCCGAAGTTGGATGAGCTGAGAGATGAGGGTAAA

GCGTCTTCCGCTAAACAACGACTTAAATGCGCTTCTCTGC

AGAAATTTGGCGAACGAGCGTTCAAAGCCTGGGCCGTTG

CGCGCCTTTCACAGCGGTTTCCGAAAGCCGAGTTCGCCG

AGGTTTCAAAGCTGGTTACGGACTTGACAAAGGTGCATA

CAGAATGCTGCCACGGAGACCTGCTGGAGTGCGCCGATG

ATCGCGCTGATTTGGCTAAATATATTTGCGAAAATCAGGA

CAGCATCAGCTCCAAGTTGAAGGAGTGTTGTGAAAAACC

GCTGCTGGAGAAGTCACACTGCATAGCCGAGGTGGAAAA

CGACGAGATGCCGGCAGACCTCCCCAGCCTTGCCGCGGA

TTTCGTCGAATCAAAGGATGTATGCAAAAATTACGCGGA

AGCAAAAGATGTATTTCTGGGAATGTTCCTGTACGAGTAC

GCTAGGCGACATCCCGACTACAGCGTTGTTCTGCTCTTGA

GACTTGCGAAGACGTACGAGACTACGCTCGAGAAGTGCT

GTGCAGCTGCGGACCCCCATGAGTGTTATGCTAAAGTCTT

CGACGAATTTAAGCCTTTGGTGGAAGAGCCACAGAACCT

GATCAAACAAAATTGTGAACTGTTCGAACAATTGGGGGA

GTATAAATTTCAGAACGCTCTCCTTGTTCGGTATACAAAA

AAAGTACCGCAGGTAAGTACGCCGACACTCGTGGAAGTA

AGCAGGAACCTCGGAAAGGTTGGATCAAAATGCTGCAAG

CATCCGGAGGCTAAGCGCATGCCATGCGCTGAGGATTAT

CTTTCAGTGGTCCTGAACCAATTGTGCGTGTTGCACGAGA

AAACTCCAGTAAGCGATAGAGTTACCAAATGTTGTACAG

AGAGCCTGGTTAATCGACGACCTTGCTTCAGCGCCTTGGA

AGTCGATGAGACGTATGTGCCGAAGGAATTTAACGCCGA

AACTTTCACTTTTCATGCAGATATCTGTACATTGAGCGAA

AAGGAAAGGCAAATTAAAAAACAAACTGCGCTTGTGGAA

TTGGTCAAGCACAAGCCTAAAGCCACAAAGGAACAGCTC

AAAGCGGTAATGGACGATTTTGCGGCGTTCGTAGAGAAG

TGTTGCAAGGCGGACGATAAAGAAACGTGCTTTGCTGAG

GAGGGAAAAAAGCTTGTTGCTGCCAGTCAAGCGGCGCTT

GGCTTGAGTGGTGGAGAACAAAAACTCATTTCCGAGGAA

GATCTTTGA

28
ProC1485/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

16_mhLIGHT_
RGLSYHDGALVVTKTGYYYIYSKVQLGGVGCPLGLAGTITH

21linker_HSA-cMyc
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLGKRLVRLRDGTRSYFGAFMVSSAGG

GSSGGSSAGGGSSGGSDAHKSEVAHRFKDLGEENFKALVLI

AFAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKS

LHTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQH

KDDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRH

PYFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRD

EGKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAE

FAEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICEN

QDSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADF

VESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRL

AKTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQ

NCELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLG

KVGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSD

RVTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADI

CTLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAA

FVEKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLIS

EEDL

29
ProC1485/
CAGGGACAGTCCGGATCTAGGCATCCATGTCGGCATGAC

ProC_mLm-
CCACATATCATATGCTACAAATTCGGTGGAGGATCTTCTG

16_mhLIGHT_
GAGGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGA

21linker_HSA-cMyc
CAATATTGGTGGCTCCCAAGAACGCCGATCACACGAAGT

DNA
GAACCCTGCTGCTCACTTGACTGGAGCTAACTCCAGCCTT

ACGGGGAGCGGGGGTCCTTTGCTCTGGGAAACGCAGCTG

GGTCTCGCGTTTCTTAGAGGGCTGAGTTATCACGATGGCG

CCTTGGTCGTCACGAAGACTGGGTACTACTATATTTATAG

TAAGGTACAGTTGGGGGGAGTGGGGTGCCCTCTCGGCCT

GGCTGGGACGATCACGCATGGGCTCTACAAGCGCACGCC

TAGGTATCCGGAGGAGTTGGAACTGTTGGTCTCACAGCA

GTCCCCGTGCGGGCGAGCGACTTCCTCCAGTAGAGTGTG

GTGGGACTCTAGCTTTCTCGGGGGAGTGGTTCATCTTGAG

GCAGGAGAGGAAGTGGTGGTACGGGTTTTGGGCAAGAGA

TTGGTGAGACTGCGGGATGGTACAAGATCTTATTTTGGTG

CTTTCATGGTCAGCTCTGCGGGGGGAGGAAGCTCCGGGG

GTAGTTCCGCCGGCGGCGGATCTAGTGGCGGTTCTGATGC

TCATAAAAGTGAGGTCGCGCACAGATTCAAAGACCTCGG

CGAGGAAAACTTTAAAGCCCTCGTATTGATAGCTTTCGCC

CAGTACCTCCAGCAGTGCCCATTCGAGGATCACGTGAAA

CTCGTGAATGAAGTAACGGAATTTGCCAAAACGTGCGTG

GCCGACGAGAGTGCCGAAAATTGCGACAAGTCACTTCAC

ACCCTTTTTGGTGACAAATTGTGTACTGTGGCGACGCTTA

GGGAAACATACGGAGAAATGGCCGATTGCTGTGCCAAAC

AAGAGCCTGAAAGAAACGAATGCTTTCTTCAGCACAAAG

ACGATAACCCTAACTTGCCGAGACTGGTGAGACCTGAAG

TAGACGTCATGTGTACCGCGTTCCATGACAACGAAGAGA

CTTTCTTGAAAAAATACCTTTATGAAATAGCACGGAGGC

ACCCTTATTTTTACGCTCCAGAGCTCCTCTTCTTTGCTAAA

CGGTACAAAGCGGCGTTTACCGAATGTTGCCAAGCTGCG

GATAAAGCTGCATGTCTTCTCCCGAAGTTGGATGAGCTGA

GAGATGAGGGTAAAGCGTCTTCCGCTAAACAACGACTTA

AATGCGCTTCTCTGCAGAAATTTGGCGAACGAGCGTTCA

AAGCCTGGGCCGTTGCGCGCCTTTCACAGCGGTTTCCGAA

AGCCGAGTTCGCCGAGGTTTCAAAGCTGGTTACGGACTT

GACAAAGGTGCATACAGAATGCTGCCACGGAGACCTGCT

GGAGTGCGCCGATGATCGCGCTGATTTGGCTAAATATATT

TGCGAAAATCAGGACAGCATCAGCTCCAAGTTGAAGGAG

TGTTGTGAAAAACCGCTGCTGGAGAAGTCACACTGCATA

GCCGAGGTGGAAAACGACGAGATGCCGGCAGACCTCCCC

AGCCTTGCCGCGGATTTCGTCGAATCAAAGGATGTATGC

AAAAATTACGCGGAAGCAAAAGATGTATTTCTGGGAATG

TTCCTGTACGAGTACGCTAGGCGACATCCCGACTACAGC

GTTGTTCTGCTCTTGAGACTTGCGAAGACGTACGAGACTA

CGCTCGAGAAGTGCTGTGCAGCTGCGGACCCCCATGAGT

GTTATGCTAAAGTCTTCGACGAATTTAAGCCTTTGGTGGA

AGAGCCACAGAACCTGATCAAACAAAATTGTGAACTGTT

CGAACAATTGGGGGAGTATAAATTTCAGAACGCTCTCCTT

GTTCGGTATACAAAAAAAGTACCGCAGGTAAGTACGCCG

ACACTCGTGGAAGTAAGCAGGAACCTCGGAAAGGTTGGA

TCAAAATGCTGCAAGCATCCGGAGGCTAAGCGCATGCCA

TGCGCTGAGGATTATCTTTCAGTGGTCCTGAACCAATTGT

GCGTGTTGCACGAGAAAACTCCAGTAAGCGATAGAGTTA

CCAAATGTTGTACAGAGAGCCTGGTTAATCGACGACCTT

GCTTCAGCGCCTTGGAAGTCGATGAGACGTATGTGCCGA

AGGAATTTAACGCCGAAACTTTCACTTTTCATGCAGATAT

CTGTACATTGAGCGAAAAGGAAAGGCAAATTAAAAAACA

AACTGCGCTTGTGGAATTGGTCAAGCACAAGCCTAAAGC

CACAAAGGAACAGCTCAAAGCGGTAATGGACGATTTTGC

GGCGTTCGTAGAGAAGTGTTGCAAGGCGGACGATAAAGA

AACGTGCTTTGCTGAGGAGGGAAAAAAGCTTGTTGCTGC

CAGTCAAGCGGCGCTTGGCTTGAGTGGTGGAGAACAAAA

ACTCATTTCCGAGGAAGATCTTTGA

30
ProC1487/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

16_mhLIGHT_
RGLSYHDGALVVTKTGYYYIYSKVQLGGVGCPLGLAGTITH

1204DNI_HSA-cMyc
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLGKRLVRLRDGTRSYFGAFMVSSAGG

GSSGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIA

FAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSL

HTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHK

DDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHP

YFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDE

GKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEF

AEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQ

DSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFV

ESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLA

KTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQN

CELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGK

VGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDR

VTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADIC

TLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAF

VEKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISE

EDL

31
ProC1487/
CAGGGACAGTCCGGATCTAGGCATCCATGTCGGCATGAC

ProC_mLm-
CCACATATCATATGCTACAAATTCGGTGGAGGATCTTCTG

16_mhLIGHT_
GAGGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGA

1204DNI_HSA-cMyc
CAATATTGGTGGCTCCCAAGAACGCCGATCACACGAAGT

DNA
GAACCCTGCTGCTCACTTGACTGGAGCTAACTCCAGCCTT

ACGGGGAGCGGGGGTCCTTTGCTCTGGGAAACGCAGCTG

GGTCTCGCGTTTCTTAGAGGGCTGAGTTATCACGATGGCG

CCTTGGTCGTCACGAAGACTGGGTACTACTATATTTATAG

TAAGGTACAGTTGGGGGGAGTGGGGTGCCCTCTCGGCCT

GGCTGGGACGATCACGCATGGGCTCTACAAGCGCACGCC

TAGGTATCCGGAGGAGTTGGAACTGTTGGTCTCACAGCA

GTCCCCGTGCGGGCGAGCGACTTCCTCCAGTAGAGTGTG

GTGGGACTCTAGCTTTCTCGGGGGAGTGGTTCATCTTGAG

GCAGGAGAGGAAGTGGTGGTACGGGTTTTGGGCAAGAGA

TTGGTGAGACTGCGGGATGGTACAAGATCTTATTTTGGTG

CTTTCATGGTCTCCAGCGCCGGGGGCGGAAGCAGCGGCG

GCAGCTTAAGCGGCAGAAGCGACAACATCGGCAGCGATG

CTCATAAAAGTGAGGTCGCGCACAGATTCAAAGACCTCG

GCGAGGAAAACTTTAAAGCCCTCGTATTGATAGCTTTCGC

CCAGTACCTCCAGCAGTGCCCATTCGAGGATCACGTGAA

ACTCGTGAATGAAGTAACGGAATTTGCCAAAACGTGCGT

GGCCGACGAGAGTGCCGAAAATTGCGACAAGTCACTTCA

CACCCTTTTTGGTGACAAATTGTGTACTGTGGCGACGCTT

AGGGAAACATACGGAGAAATGGCCGATTGCTGTGCCAAA

CAAGAGCCTGAAAGAAACGAATGCTTTCTTCAGCACAAA

GACGATAACCCTAACTTGCCGAGACTGGTGAGACCTGAA

GTAGACGTCATGTGTACCGCGTTCCATGACAACGAAGAG

ACTTTCTTGAAAAAATACCTTTATGAAATAGCACGGAGG

CACCCTTATTTTTACGCTCCAGAGCTCCTCTTCTTTGCTAA

ACGGTACAAAGCGGCGTTTACCGAATGTTGCCAAGCTGC

GGATAAAGCTGCATGTCTTCTCCCGAAGTTGGATGAGCTG

AGAGATGAGGGTAAAGCGTCTTCCGCTAAACAACGACTT

AAATGCGCTTCTCTGCAGAAATTTGGCGAACGAGCGTTC

AAAGCCTGGGCCGTTGCGCGCCTTTCACAGCGGTTTCCGA

AAGCCGAGTTCGCCGAGGTTTCAAAGCTGGTTACGGACT

TGACAAAGGTGCATACAGAATGCTGCCACGGAGACCTGC

TGGAGTGCGCCGATGATCGCGCTGATTTGGCTAAATATAT

TTGCGAAAATCAGGACAGCATCAGCTCCAAGTTGAAGGA

GTGTTGTGAAAAACCGCTGCTGGAGAAGTCACACTGCAT

AGCCGAGGTGGAAAACGACGAGATGCCGGCAGACCTCCC

CAGCCTTGCCGCGGATTTCGTCGAATCAAAGGATGTATGC

AAAAATTACGCGGAAGCAAAAGATGTATTTCTGGGAATG

TTCCTGTACGAGTACGCTAGGCGACATCCCGACTACAGC

GTTGTTCTGCTCTTGAGACTTGCGAAGACGTACGAGACTA

CGCTCGAGAAGTGCTGTGCAGCTGCGGACCCCCATGAGT

GTTATGCTAAAGTCTTCGACGAATTTAAGCCTTTGGTGGA

AGAGCCACAGAACCTGATCAAACAAAATTGTGAACTGTT

CGAACAATTGGGGGAGTATAAATTTCAGAACGCTCTCCTT

GTTCGGTATACAAAAAAAGTACCGCAGGTAAGTACGCCG

ACACTCGTGGAAGTAAGCAGGAACCTCGGAAAGGTTGGA

TCAAAATGCTGCAAGCATCCGGAGGCTAAGCGCATGCCA

TGCGCTGAGGATTATCTTTCAGTGGTCCTGAACCAATTGT

GCGTGTTGCACGAGAAAACTCCAGTAAGCGATAGAGTTA

CCAAATGTTGTACAGAGAGCCTGGTTAATCGACGACCTT

GCTTCAGCGCCTTGGAAGTCGATGAGACGTATGTGCCGA

AGGAATTTAACGCCGAAACTTTCACTTTTCATGCAGATAT

CTGTACATTGAGCGAAAAGGAAAGGCAAATTAAAAAACA

AACTGCGCTTGTGGAATTGGTCAAGCACAAGCCTAAAGC

CACAAAGGAACAGCTCAAAGCGGTAATGGACGATTTTGC

GGCGTTCGTAGAGAAGTGTTGCAAGGCGGACGATAAAGA

AACGTGCTTTGCTGAGGAGGGAAAAAAGCTTGTTGCTGC

CAGTCAAGCGGCGCTTGGCTTGAGTGGTGGAGAACAAAA

ACTCATTTCCGAGGAAGATCTTTGA

32
ProC1493/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_LIGHT-3HB-
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

1204DNI-HSA-His
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

Protein
HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGGGS

GGGSGGSGEIAALKQEIAALKKEIAALKWEIAALKQGYYGG

SGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIAFA

QYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLHT

LFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKDD

NPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPYF

YAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSHHHHHH

33
ProC1493/
CAAGAGCGAAGATCCCATGAAGTAAACCCTGCAGCTCAC

ProC_LIGHT-3HB-
CTTACAGGAGCCAACAGCAGTCTGACAGGTTCTGGGGGC

1204DNI-HSA-His
CCCTTGTTGTGGGAGACGCAACTGGGGCTTGCATTCCTCC

DNA
GAGGGCTCAGTTACCACGACGGCGCGCTTGTTGTTACAA

AAGCAGGATACTACTATATTTACTCAAAGGTGCAGCTGG

GTGGAGTGGGATGTCCATTGGGCCTGGCCTCAACTATAA

CCCATGGCCTCTATAAAAGAACGCCCCGGTATCCTGAGG

AGCTGGAGCTGTTGGTCTCACAGCAGTCACCGTGCGGCA

GAGCCACATCATCCTCTCGCGTATGGTGGGACTCTTCCTT

CCTGGGAGGTGTAGTCCATCTCGAGGCAGGTGAAGAAGT

CGTAGTTCGCGTACTCGATGAACGCCTGGTTCGGCTGAGG

GATGGGACTAGGAGCTATTTCGGCGCATTTATGGTATCTT

CTGCAGGTGGAGGAAGTGGTGGCGGTTCCGGTGGTTCAG

GGGAAATCGCGGCACTCAAACAAGAGATAGCGGCTTTGA

AAAAGGAGATCGCAGCCCTGAAATGGGAAATAGCGGCCT

TGAAGCAGGGCTACTATGGCGGCAGCGGCGGCAGCCTAA

GCGGACGGTCCGACAATATCGGCAGCGATGCACATAAAA

GTGAGGTGGCCCACCGCTTTAAAGACCTCGGCGAGGAGA

ACTTCAAGGCACTCGTACTTATTGCCTTTGCACAATACCT

GCAGCAATGTCCGTTTGAAGATCATGTCAAGCTCGTAAAT

GAAGTGACAGAGTTCGCTAAGACCTGTGTAGCTGACGAA

AGTGCCGAAAACTGCGACAAATCATTGCATACATTGTTC

GGCGACAAGCTTTGTACAGTTGCCACGCTCCGCGAGACA

TACGGCGAAATGGCCGATTGTTGTGCGAAACAGGAACCC

GAAAGAAATGAGTGCTTCTTGCAACACAAAGACGATAAT

CCCAATCTTCCGCGACTGGTGAGACCCGAAGTAGATGTA

ATGTGCACAGCTTTTCATGACAATGAGGAAACCTTTCTTA

AAAAATATCTGTACGAAATCGCCCGCCGACACCCGTATTT

CTATGCCCCAGAGCTGTTGTTTTTCGCAAAGCGCTACAAG

GCAGCGTTTACCGAATGCTGCCAGGCCGCTGATAAAGCC

GCTTGTCTGCTGCCTAAGCTTGATGAGCTTCGCGACGAGG

GTAAGGCTTCCAGCGCTAAACAACGCCTGAAGTGTGCAT

CTTTGCAAAAATTTGGTGAACGAGCCTTCAAGGCTTGGGC

TGTTGCCAGGCTGAGTCAACGGTTCCCGAAGGCGGAGTT

TGCGGAGGTTTCCAAGTTGGTAACGGACCTGACAAAGGT

ACATACCGAATGCTGCCATGGCGACCTGTTGGAGTGCGC

CGATGATCGAGCGGATCTTGCCAAGTATATTTGCGAAAA

CCAAGACTCCATTTCCAGTAAACTTAAGGAGTGTTGTGAG

AAACCTCTCCTTGAAAAGAGCCATTGTATAGCGGAGGTC

GAAAACGATGAAATGCCCGCTGATCTGCCGTCACTCGCT

GCTGACTTCGTTGAATCCAAGGATGTATGTAAAAACTATG

CCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTTGTATGA

ATACGCCCGACGGCATCCTGACTATTCAGTTGTGCTCCTT

CTTCGATTGGCTAAAACTTATGAGACGACACTTGAAAAG

TGTTGTGCCGCCGCCGACCCACATGAGTGCTACGCTAAG

GTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACCGCAGA

ATCTCATTAAGCAAAATTGTGAGCTCTTTGAACAACTCGG

TGAATACAAATTTCAGAACGCGCTTCTGGTTAGATATACG

AAGAAAGTGCCACAGGTGAGCACCCCTACATTGGTTGAG

GTCAGTAGGAACCTCGGCAAGGTGGGATCTAAGTGCTGC

AAACACCCGGAGGCAAAGAGAATGCCTTGCGCTGAGGAT

TATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTCTTCACG

AAAAGACTCCCGTCAGCGACCGAGTCACGAAGTGCTGTA

CCGAGAGCCTTGTTAATAGACGACCTTGCTTCTCCGCGCT

TGAGGTGGATGAGACCTACGTCCCAAAGGAATTCAACGC

CGAGACGTTCACTTTCCATGCCGATATTTGCACCTTGTCA

GAAAAGGAGCGACAGATAAAAAAGCAAACTGCTTTGGTG

GAGCTGGTTAAGCATAAGCCTAAAGCGACGAAGGAACAG

CTCAAAGCCGTAATGGATGATTTCGCTGCCTTCGTGGAGA

AATGTTGTAAGGCCGATGACAAGGAAACCTGCTTCGCTG

AAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGGCGGCAC

TTGGTTTGAGCCACCACCACCATCACCACtga

34
ProC1490/
EIAALKQEIAALKKEIAALKWEIAALKQGYYGGSGGSQERR

ProC_3HB-LIGHT-
SHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRGLSYH

1204DNI-HSA-cMyc
DGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGLYKRT

Protein
PRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVVHLEA

GEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGGGSSGGS

LSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLIAFAQYL

QQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLHTLFGD

KLCTVATLRETYGEMADCCAKQEPERNECFLQHKDDNPNL

PRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPYFYAPE

LLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEGKASS

AKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFAEVSK

LVTDLTKVHTECCHGDLLECADDRADLAKYICENQDSISSK

LKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVESKDV

CKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAKTYET

TLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNCELFE

QLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKVGSK

CCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRVTKC

CTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICTLSE

KERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFVEKC

CKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISEEDL

35
ProC1490/
GAAATCGCGGCACTCAAACAAGAGATAGCGGCTTTGAAA

ProC_3HB-LIGHT-
AAGGAGATCGCAGCCCTGAAATGGGAAATAGCGGCCTTG

1204DNI-HSA-cMyc
AAGCAGGGCTACTATGGGGGATCCGGGGGTTCACAGGAG

DNA
CGACGGTCCCATGAGGTGAATCCGGCAGCGCATTTGACG

GGGGCCAACTCATCCCTGACAGGTTCAGGTGGCCCTCTGT

TGTGGGAAACTCAGCTCGGACTGGCCTTCCTTAGAGGTTT

GTCATATCATGACGGAGCACTTGTAGTCACCAAAGCTGG

GTATTACTACATATACTCTAAGGTCCAGCTGGGTGGGGTG

GGCTGTCCACTTGGCTTGGCATCTACGATCACGCATGGGT

TGTACAAAAGAACTCCACGATATCCAGAAGAACTCGAAT

TGCTTGTCTCCCAACAATCTCCTTGTGGCAGGGCTACGTC

CAGTTCCCGAGTGTGGTGGGATTCAAGTTTTCTCGGGGGC

GTAGTCCATCTTGAAGCAGGGGAGGAAGTGGTCGTCCGA

GTGCTGGACGAACGGTTGGTTAGGCTTCGGGATGGGACA

AGAAGTTATTTTGGGGCCTTCATGGTATCCAGCGCCGGGG

GCGGAAGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGAC

AACATCGGCAGCGATGCTCATAAAAGTGAGGTCGCGCAC

AGATTCAAAGACCTCGGCGAGGAAAACTTTAAAGCCCTC

GTATTGATAGCTTTCGCCCAGTACCTCCAGCAGTGCCCAT

TCGAGGATCACGTGAAACTCGTGAATGAAGTAACGGAAT

TTGCCAAAACGTGCGTGGCCGACGAGAGTGCCGAAAATT

GCGACAAGTCACTTCACACCCTTTTTGGTGACAAATTGTG

TACTGTGGCGACGCTTAGGGAAACATACGGAGAAATGGC

CGATTGCTGTGCCAAACAAGAGCCTGAAAGAAACGAATG

CTTTCTTCAGCACAAAGACGATAACCCTAACTTGCCGAGA

CTGGTGAGACCTGAAGTAGACGTCATGTGTACCGCGTTCC

ATGACAACGAAGAGACTTTCTTGAAAAAATACCTTTATG

AAATAGCACGGAGGCACCCTTATTTTTACGCTCCAGAGCT

CCTCTTCTTTGCTAAACGGTACAAAGCGGCGTTTACCGAA

TGTTGCCAAGCTGCGGATAAAGCTGCATGTCTTCTCCCGA

AGTTGGATGAGCTGAGAGATGAGGGTAAAGCGTCTTCCG

CTAAACAACGACTTAAATGCGCTTCTCTGCAGAAATTTGG

CGAACGAGCGTTCAAAGCCTGGGCCGTTGCGCGCCTTTC

ACAGCGGTTTCCGAAAGCCGAGTTCGCCGAGGTTTCAAA

GCTGGTTACGGACTTGACAAAGGTGCATACAGAATGCTG

CCACGGAGACCTGCTGGAGTGCGCCGATGATCGCGCTGA

TTTGGCTAAATATATTTGCGAAAATCAGGACAGCATCAG

CTCCAAGTTGAAGGAGTGTTGTGAAAAACCGCTGCTGGA

GAAGTCACACTGCATAGCCGAGGTGGAAAACGACGAGAT

GCCGGCAGACCTCCCCAGCCTTGCCGCGGATTTCGTCGA

ATCAAAGGATGTATGCAAAAATTACGCGGAAGCAAAAGA

TGTATTTCTGGGAATGTTCCTGTACGAGTACGCTAGGCGA

CATCCCGACTACAGCGTTGTTCTGCTCTTGAGACTTGCGA

AGACGTACGAGACTACGCTCGAGAAGTGCTGTGCAGCTG

CGGACCCCCATGAGTGTTATGCTAAAGTCTTCGACGAATT

TAAGCCTTTGGTGGAAGAGCCACAGAACCTGATCAAACA

AAATTGTGAACTGTTCGAACAATTGGGGGAGTATAAATT

TCAGAACGCTCTCCTTGTTCGGTATACAAAAAAAGTACCG

CAGGTAAGTACGCCGACACTCGTGGAAGTAAGCAGGAAC

CTCGGAAAGGTTGGATCAAAATGCTGCAAGCATCCGGAG

GCTAAGCGCATGCCATGCGCTGAGGATTATCTTTCAGTGG

TCCTGAACCAATTGTGCGTGTTGCACGAGAAAACTCCAGT

AAGCGATAGAGTTACCAAATGTTGTACAGAGAGCCTGGT

TAATCGACGACCTTGCTTCAGCGCCTTGGAAGTCGATGAG

ACGTATGTGCCGAAGGAATTTAACGCCGAAACTTTCACTT

TTCATGCAGATATCTGTACATTGAGCGAAAAGGAAAGGC

AAATTAAAAAACAAACTGCGCTTGTGGAATTGGTCAAGC

ACAAGCCTAAAGCCACAAAGGAACAGCTCAAAGCGGTA

ATGGACGATTTTGCGGCGTTCGTAGAGAAGTGTTGCAAG

GCGGACGATAAAGAAACGTGCTTTGCTGAGGAGGGAAAA

AAGCTTGTTGCTGCCAGTCAAGCGGCGCTTGGCTTGAGTG

GTGGAGAACAAAAACTCATTTCCGAGGAAGATCTTTGA

36
ProC1494/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm16-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

LIGHT-3HB-
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

1204DNI-HSA-His
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGG

GSGGGSGGSGEIAALKQEIAALKKEIAALKWEIAALKQGYY

GGSGGSLSGRSDNIGSDAHKSEVAHRFKDLGEENFKALVLI

AFAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKS

LHTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQH

KDDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRH

PYFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRD

EGKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAE

FAEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICEN

QDSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADF

VESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRL

AKTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQ

NCELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLG

KVGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSD

RVTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADI

CTLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAA

FVEKCCKADDKETCFAEEGKKLVAASQAALGLSHHHHHH

37
ProC1494/
CAAGGACAGAGCGGCTCACGGCATCCTTGTAGACACGAC

ProC_mLm16-
CCACACATCATCTGTTACAAGTTTGGAGGCGGCAGCAGC

LIGHT-3HB-
GGCGGCTCTATCAGCTCTGGCCTTCTGAGCGGTCGGAGCG

1204DNI-HSA-His
ACAACATCGGAGGCAGCCAAGAGCGAAGATCCCATGAA

DNA
GTAAACCCTGCAGCTCACCTTACAGGAGCCAACAGCAGT

CTGACAGGTTCTGGGGGCCCCTTGTTGTGGGAGACGCAA

CTGGGGCTTGCATTCCTCCGAGGGCTCAGTTACCACGACG

GCGCGCTTGTTGTTACAAAAGCAGGATACTACTATATTTA

CTCAAAGGTGCAGCTGGGTGGAGTGGGATGTCCATTGGG

CCTGGCCTCAACTATAACCCATGGCCTCTATAAAAGAAC

GCCCCGGTATCCTGAGGAGCTGGAGCTGTTGGTCTCACA

GCAGTCACCGTGCGGCAGAGCCACATCATCCTCTCGCGT

ATGGTGGGACTCTTCCTTCCTGGGAGGTGTAGTCCATCTC

GAGGCAGGTGAAGAAGTCGTAGTTCGCGTACTCGATGAA

CGCCTGGTTCGGCTGAGGGATGGGACTAGGAGCTATTTC

GGCGCATTTATGGTATCTTCTGCAGGTGGAGGAAGTGGT

GGCGGTTCCGGTGGTTCAGGGGAAATCGCGGCACTCAAA

CAAGAGATAGCGGCTTTGAAAAAGGAGATCGCAGCCCTG

AAATGGGAAATAGCGGCCTTGAAGCAGGGCTACTATGGC

GGCAGCGGCGGCAGCCTAAGCGGACGGTCCGACAATATC

GGCAGCGATGCACATAAAAGTGAGGTGGCCCACCGCTTT

AAAGACCTCGGCGAGGAGAACTTCAAGGCACTCGTACTT

ATTGCCTTTGCACAATACCTGCAGCAATGTCCGTTTGAAG

ATCATGTCAAGCTCGTAAATGAAGTGACAGAGTTCGCTA

AGACCTGTGTAGCTGACGAAAGTGCCGAAAACTGCGACA

AATCATTGCATACATTGTTCGGCGACAAGCTTTGTACAGT

TGCCACGCTCCGCGAGACATACGGCGAAATGGCCGATTG

TTGTGCGAAACAGGAACCCGAAAGAAATGAGTGCTTCTT

GCAACACAAAGACGATAATCCCAATCTTCCGCGACTGGT

GAGACCCGAAGTAGATGTAATGTGCACAGCTTTTCATGA

CAATGAGGAAACCTTTCTTAAAAAATATCTGTACGAAAT

CGCCCGCCGACACCCGTATTTCTATGCCCCAGAGCTGTTG

TTTTTCGCAAAGCGCTACAAGGCAGCGTTTACaGAATGCT

GCCAGGCCGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCT

TGATGAGCTTCGCGACGAGGGTAAGGCTTCCAGCGCTAA

ACAACGCCTGAAGTGTGCATCTTTGCAAAAATTTGGTGA

ACGAGCCTTCAAGGCTTGGGCTGTTGCCAGGCTGAGTCA

ACGGTTCCCGAAGGCGGAGTTTGCGGAGGTTTCCAAGTT

GGTAACGGACCTGACAAAGGTACATACCGAATGCTGCCA

TGGCGACCTGTTGGAGTGCGCCGATGATCGAGCGGATCT

TGCCAAGTATATTTGCGAAAACCAAGACTCCATTTCCAGT

AAACTTAAGGAGTGTTGTGAGAAACCTCTCCTTGAAAAG

AGCCATTGTATAGCGGAGGTCGAAAACGATGAAATGCCC

GCTGATCTGCCGTCACTCGCTGCTGACTTCGTTGAATCCA

AGGATGTATGTAAAAACTATGCCGAAGCTAAGGACGTCT

TTCTTGGAATGTTCTTGTATGAATACGCCCGACGGCATCC

TGACTATTCAGTTGTGCTCCTTCTTCGATTGGCTAAAACTT

ATGAGACGACACTTGAAAAGTGTTGTGCCGCCGCCGACC

CACATGAGTGCTACGCTAAGGTTTTCGACGAATTTAAGCC

CTTGGTTGAAGAACCGCAGAATCTCATTAAGCAAAATTG

TGAGCTCTTTGAACAACTCGGTGAATACAAATTTCAGAAC

GCGCTTCTGGTTAGATATACGAAGAAAGTGCCACAGGTG

AGCACCCCTACATTGGTTGAGGTCAGTAGGAACCTCGGC

AAGGTGGGATCTAAGTGCTGCAAACACCCGGAGGCAAAG

AGAATGCCTTGCGCTGAGGATTATCTCTCAGTGGTTCTGA

ATCAGCTTTGCGTTCTTCACGAAAAGACTCCCGTCAGCGA

CCGAGTCACGAAGTGCTGTACCGAGAGCCTTGTTAATAG

ACGACCTTGCTTCTCCGCGCTTGAGGTGGATGAGACCTAC

GTCCCAAAGGAATTCAACGCCGAGACGTTCACTTTCCATG

CCGATATTTGCACCTTGTCAGAAAAGGAGCGACAGATAA

AAAAGCAAACTGCTTTGGTGGAGCTGGTTAAGCATAAGC

CTAAAGCGACGAAGGAACAGCTCAAAGCCGTAATGGATG

ATTTCGCTGCCTTCGTGGAGAAATGTTGTAAGGCCGATGA

CAAGGAAACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGT

CGCCGCTAGTCAGGCGGCACTTGGTTTGAGCCACCACCA

CCATCACCACtga

38
ProC2006/
GSGEQKLISEEDLGDAHKSEVAHRFKDLGEENFKALVLIAF

ProC_cMyc-HSA-
AQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLH

mLm16-1490DNI-
TLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKD

LIGHT-3HB
DNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPY

Protein
FYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLGGGSSGGSGS

QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGG

GSGGGSGGSGEIAALKQEIAALKKEIAALKWEIAALKQGYY

GG

39
ProC2006/
GGCTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTT

ProC_cMyc-HSA-
GGCGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAA

mLm16-1490DNI-
GACCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATT

LIGHT-3HB
GCCTTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATC

DNA
ATGTCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGA

CCTGTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAAT

CATTGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGC

CACGCTCCGCGAGACATACGGCGAAATGGCCGATTGTTG

TGCGAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCA

ACACAAAGACGATAATCCCAATCTTCCGCGACTGGTGAG

ACCCGAAGTAGATGTAATGTGCACAGCTTTTCATGACAAT

GAGGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCC

CGCCGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTT

TCGCAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCA

GGCCGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGAT

GAGCTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAA

CGCCTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGA

GCCTTCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGT

TCCCGAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAA

CGGACCTGACAAAGGTACATACCGAATGCTGCCATGGCG

ACCTGTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCA

AGTATATTTGCGAAAACCAAGACTCCATTTCCAGTAAACT

TAAGGAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCA

TTGTATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGA

TCTGCCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGAT

GTATGTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTG

GAATGTTCTTGTATGAATACGCCCGACGGCATCCTGACTA

TTCAGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAG

ACGACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACAT

GAGTGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGG

TTGAAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGC

TCTTTGAACAACTCGGTGAATACAAATTTCAGAACGCGCT

TCTGGTTAGATATACGAAGAAAGTGCCACAGGTGAGCAC

CCCTACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGT

GGGATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAAT

GCCTTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAG

CTTTGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAG

TCACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGAC

CTTGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCC

AAAGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGA

TATTTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAA

GCAAACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAA

AGCGACGAAGGAACAGCTCAAAGCCGTAATGGATGATTT

CGCTGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAA

GGAAACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGC

CGCTAGTCAGGCGGCACTTGGTTTGGGGGGCGGAAGCAG

CGGCGGCAGCGGCAGCCAAGGCCAGAGCGGCAGCAGGC

ACCCTTGTAGACACGATCCTCACATCATCTGTTACAAGTT

TGGAGGAGGCAGTAGCGGTGGCAGTATTAGCAGCGGACT

GCTGAGTGGCAGAAGCGACAACATCGGCGGCAGCCAGG

AGAGACGGAGCCACGAGGTGAACCCCGCTGCCCACCTGA

CCGGCGCCAACAGCAGTCTGACCGGCAGCGGCGGCCCTC

TGCTGTGGGAGACACAGCTGGGCCTGGCCTTTCTGAGAG

GCCTGTCCTACCACGACGGCGCCCTGGTCGTGACCAAGG

CCGGCTACTACTACATCTACAGCAAGGTGCAGCTGGGAG

GCGTGGGCTGCCCTCTGGGCCTGGCATCTACCATCACGCA

CGGCCTGTACAAGCGGACCCCTAGATATCCTGAGGAACT

GGAACTCCTGGTGTCCCAGCAGAGCCCTTGCGGCAGAGC

TACAAGCAGCTCAAGAGTGTGGTGGGACAGCAGCTTCCT

GGGCGGAGTGGTCCACCTGGAAGCTGGAGAAGAAGTGGT

GGTCCGGGTGCTGGACGAGAGACTCGTGAGGCTGAGAGA

CGGAACAAGAAGCTACTTCGGCGCTTTTATGGTGTCTTCT

GCAGGTGGAGGAAGTGGTGGCGGTTCCGGTGGTTCAGGG

GAAATCGCGGCACTCAAACAAGAGATAGCGGCTTTGAAA

AAGGAGATCGCAGCCCTGAAATGGGAAATAGCGGCCTTG

AAGCAGGGCTACTATGGCGGCtga

40
ProC1497/
GSGEQKLISEEDLGDAHKSEVAHRFKDLGEENFKALVLIAF

ProC_cMyc-HSA-
AQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLH

21GS-1204DNI-
TLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKD

LIGHT
DNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPY

Protein
FYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSSAGGGSSGG

SLSGRSDNIGSQERRSHEVNPAAHLTGANSSLTGSGGPLLW

ETQLGLAFLRGLSYHDGALVVTKAGYYYIYSKVQLGGVGC

PLGLASTITHGLYKRTPRYPEELELLVSQQSPCGRATSSSRV

WWDSSFLGGVVHLEAGEEVVVRVLDERLVRLRDGTRSYFG

AFMV

41
ProC1497/
GGCTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTT

ProC_cMyc-HSA-
GGCGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAA

21GS-1204DNI-
GACCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATT

LIGHT
GCCTTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATC

DNA
ATGTCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGA

CCTGTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAAT

CATTGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGC

CACGCTCCGCGAGACATACGGCGAAATGGCCGATTGTTG

TGCGAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCA

ACACAAAGACGATAATCCCAATCTTCCGCGACTGGTGAG

ACCCGAAGTAGATGTAATGTGCACAGCTTTTCATGACAAT

GAGGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCC

CGCCGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTT

TCGCAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCA

GGCCGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGAT

GAGCTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAA

CGCCTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGA

GCCTTCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGT

TCCCGAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAA

CGGACCTGACAAAGGTACATACCGAATGCTGCCATGGCG

ACCTGTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCA

AGTATATTTGCGAAAACCAAGACTCCATTTCCAGTAAACT

TAAGGAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCA

TTGTATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGA

TCTGCCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGAT

GTATGTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTG

GAATGTTCTTGTATGAATACGCCCGACGGCATCCTGACTA

TTCAGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAG

ACGACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACAT

GAGTGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGG

TTGAAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGC

TCTTTGAACAACTCGGTGAATACAAATTTCAGAACGCGCT

TCTGGTTAGATATACGAAGAAAGTGCCACAGGTGAGCAC

CCCTACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGT

GGGATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAAT

GCCTTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAG

CTTTGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAG

TCACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGAC

CTTGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCC

AAAGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGA

TATTTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAA

GCAAACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAA

AGCGACGAAGGAACAGCTCAAAGCCGTAATGGATGATTT

CGCTGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAA

GGAAACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGC

CGCTAGTCAGGCGGCACTTGGTTTGTCCAGCGCCGGGGG

CGGAAGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGACA

ACATCGGCAGCCAGGAGAGACGGAGCCACGAGGTGAAC

CCCGCTGCCCACCTGACCGGCGCCAACAGCAGTCTGACC

GGCAGCGGCGGCCCTCTGCTGTGGGAGACACAGCTGGGC

CTGGCCTTTCTGAGAGGCCTGTCCTACCACGACGGCGCCC

TGGTCGTGACCAAGGCCGGCTACTACTACATCTACAGCA

AGGTGCAGCTGGGAGGCGTGGGCTGCCCTCTGGGCCTGG

CATCTACCATCACGCACGGCCTGTACAAGCGGACCCCTA

GATATCCTGAGGAACTGGAACTCCTGGTGTCCCAGCAGA

GCCCTTGCGGCAGAGCTACAAGCAGCTCAAGAGTGTGGT

GGGACAGCAGCTTCCTGGGCGGAGTGGTCCACCTGGAAG

CTGGAGAAGAAGTGGTGGTCCGGGTGCTGGACGAGAGAC

TCGTGAGGCTGAGAGACGGAACAAGAAGCTACTTCGGCG

CTTTTATGGTGtga

42
ProC1489/
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

ProC_LIGHT-
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

1490DNI-mLm16-
YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

HSA-cMyc
HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVGGGSISSG

Protein
LLSGRSDNIGGGSSGGSRHPCRHDPHIICYKFSGGGSGGGSG

DAHKSEVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVK

LVNEVTEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRE

TYGEMADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDV

MCTAFHDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKA

AFTECCQAADKAACLLPKLDELRDEGKASSAKQRLKCASL

QKFGERAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHT

ECCHGDLLECADDRADLAKYICENQDSISSKLKECCEKPLLE

KSHCIAEVENDEMPADLPSLAADFVESKDVCKNYAEAKDV

FLGMFLYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADP

HECYAKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNAL

LVRYTKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMP

CAEDYLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCF

SALEVDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALV

ELVKHKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAE

EGKKLVAASQAALGLSEQKLISEEDL

43
ProC1489/
CAAGAGCGAAGATCCCATGAAGTAAACCCTGCAGCTCAC

ProC_LIGHT-
CTTACAGGAGCCAACAGCAGTCTGACAGGTTCTGGGGGC

1490DNI-mLm16-
CCCTTGTTGTGGGAGACGCAACTGGGGCTTGCATTCCTCC

HSA-cMyc
GAGGGCTCAGTTACCACGACGGCGCGCTTGTTGTTACAA

DNA
AAGCAGGATACTACTATATTTACTCAAAGGTGCAGCTGG

GTGGAGTGGGATGTCCATTGGGCCTGGCCTCAACTATAA

CCCATGGCCTCTATAAAAGAACGCCCCGGTATCCTGAGG

AGCTGGAGCTGTTGGTCTCACAGCAGTCACCGTGCGGCA

GAGCCACATCATCCTCTCGCGTATGGTGGGACTCTTCCTT

CCTGGGAGGTGTAGTCCATCTCGAGGCAGGTGAAGAAGT

CGTAGTTCGCGTACTCGATGAACGCCTGGTTCGGCTGAGG

GATGGGACTAGGAGCTATTTCGGCGCATTTATGGTAGGC

GGCGGCTCTATCTCCTCCGGCCTGCTGAGCGGCAGAAGC

GACAACATCGGCGGAGGCAGCTCCGGCGGCTCTAGACAC

CCTTGTAGACACGATCCTCACATCATCTGTTACAAGTTTT

CTGGTGGAGGAAGTGGTGGCGGTTCCGGTGATGCACATA

AAAGTGAGGTGGCCCACCGCTTTAAAGACCTCGGCGAGG

AGAACTTCAAGGCACTCGTACTTATTGCCTTTGCACAATA

CCTGCAGCAATGTCCGTTTGAAGATCATGTCAAGCTCGTA

AATGAAGTGACAGAGTTCGCTAAGACCTGTGTAGCTGAC

GAAAGTGCCGAAAACTGCGACAAATCATTGCATACATTG

TTCGGCGACAAGCTTTGTACAGTTGCCACGCTCCGCGAGA

CATACGGCGAAATGGCCGATTGTTGTGCGAAACAGGAAC

CCGAAAGAAATGAGTGCTTCTTGCAACACAAAGACGATA

ATCCCAATCTTCCGCGACTGGTGAGACCCGAAGTAGATG

TAATGTGCACAGCTTTTCATGACAATGAGGAAACCTTTCT

TAAAAAATATCTGTACGAAATCGCCCGCCGACACCCGTA

TTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGCGCTAC

AAGGCAGCGTTTACAGAATGCTGCCAGGCCGCTGATAAA

GCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCGCGACG

AGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAAGTGTG

CATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAGGCTTG

GGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAGGCGGA

GTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTGACAAA

GGTACATACCGAATGCTGCCATGGCGACCTGTTGGAGTG

CGCCGATGATCGAGCGGATCTTGCCAAGTATATTTGCGA

AAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTGTTGT

GAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCGGAG

GTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCACTC

GCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAAACT

ATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTTGTA

TGAATACGCCCGACGGCATCCTGACTATTCAGTTGTGCTC

CTTCTTCGATTGGCTAAAACTTATGAGACGACACTTGAAA

AGTGTTGTGCCGCCGCCGACCCACATGAGTGCTACGCTA

AGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACCGCA

GAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACAACTC

GGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGATATA

CGAAGAAAGTGCCACAGGTGAGCACCCCTACATTGGTTG

AGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAGTGCT

GCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCTGAGG

ATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTCTTCAC

GAAAAGACTCCCGTCAGCGACCGAGTCACGAAGTGCTGT

ACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTCCGCGC

TTGAGGTGGATGAGACCTACGTCCCAAAGGAATTCAACG

CCGAGACGTTCACTTTCCATGCCGATATTTGCACCTTGTC

AGAAAAGGAGCGACAGATAAAAAAGCAAACTGCTTTGGT

GGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAGGAACA

GCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCGTGGAG

AAATGTTGTAAGGCCGATGACAAGGAAACCTGCTTCGCT

GAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGGCGGCA

CTTGGTTTGAGCGAACAAAAACTCATTTCCGAGGAAGAT

CTTtga

44
ProC1488/
GSGEQKLISEEDLGDAHKSEVAHRFKDLGEENFKALVLIAF

ProC_cMyc-HSA-
AQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLH

mLm16-1490DNI-
TLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKD

LIGHT
DNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPY

Protein
FYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLGGGSSGGSGS

QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMV

45
ProC1488/
GGCTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTT

ProC_cMyc-HSA-
GGCGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAA

mLm16-1490DNI-
GACCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATT

LIGHT
GCCTTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATC

DNA
ATGTCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGA

CCTGTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAAT

CATTGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGC

CACGCTCCGCGAGACATACGGCGAAATGGCCGATTGTTG

TGCGAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCA

ACACAAAGACGATAATCCCAATCTTCCGCGACTGGTGAG

ACCCGAAGTAGATGTAATGTGCACAGCTTTTCATGACAAT

GAGGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCC

CGCCGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTT

TCGCAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCA

GGCCGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGAT

GAGCTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAA

CGCCTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGA

GCCTTCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGT

TCCCGAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAA

CGGACCTGACAAAGGTACATACCGAATGCTGCCATGGCG

ACCTGTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCA

AGTATATTTGCGAAAACCAAGACTCCATTTCCAGTAAACT

TAAGGAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCA

TTGTATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGA

TCTGCCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGAT

GTATGTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTG

GAATGTTCTTGTATGAATACGCCCGACGGCATCCTGACTA

TTCAGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAG

ACGACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACAT

GAGTGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGG

TTGAAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGC

TCTTTGAACAACTCGGTGAATACAAATTTCAGAACGCGCT

TCTGGTTAGATATACGAAGAAAGTGCCACAGGTGAGCAC

CCCTACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGT

GGGATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAAT

GCCTTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAG

CTTTGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAG

TCACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGAC

CTTGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCC

AAAGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGA

TATTTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAA

GCAAACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAA

AGCGACGAAGGAACAGCTCAAAGCCGTAATGGATGATTT

CGCTGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAA

GGAAACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGC

CGCTAGTCAGGCGGCACTTGGTTTGGGGGGCGGAAGCAG

CGGCGGCAGCGGCAGCCAAGGCCAGAGCGGCAGCAGGC

ACCCTTGTAGACACGATCCTCACATCATCTGTTACAAGTT

TGGAGGAGGCAGTAGCGGTGGCAGTATTAGCAGCGGACT

GCTGAGTGGCAGAAGCGACAACATCGGCGGCAGCCAGG

AGAGACGGAGCCACGAGGTGAACCCCGCTGCCCACCTGA

CCGGCGCCAACAGCAGTCTGACCGGCAGCGGCGGCCCTC

TGCTGTGGGAGACACAGCTGGGCCTGGCCTTTCTGAGAG

GCCTGTCCTACCACGACGGCGCCCTGGTCGTGACCAAGG

CCGGCTACTACTACATCTACAGCAAGGTGCAGCTGGGAG

GCGTGGGCTGCCCTCTGGGCCTGGCATCTACCATCACGCA

CGGCCTGTACAAGCGGACCCCTAGATATCCTGAGGAACT

GGAACTCCTGGTGTCCCAGCAGAGCCCTTGCGGCAGAGC

TACAAGCAGCTCAAGAGTGTGGTGGGACAGCAGCTTCCT

GGGCGGAGTGGTCCACCTGGAAGCTGGAGAAGAAGTGGT

GGTCCGGGTGCTGGACGAGAGACTCGTGAGGCTGAGAGA

CGGAACAAGAAGCTACTTCGGCGCTTTTATGGTGtga

46
ProC1498/
GSGEQKLISEEDLGDAHKSEVAHRFKDLGEENFKALVLIAF

ProC_cMyc-HSA-
AQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSLH

21GS-1204DNI-
TLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHKD

LIGHT-mLm16
DNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHPY

Protein
FYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDEG

KASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEFA

EVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQD

SISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFVE

SKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLAK

TYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQNC

ELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKV

GSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRV

TKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADICT

LSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAFV

EKCCKADDKETCFAEEGKKLVAASQAALGLSSAGGGSSGG

SLSGRSDNIGSQERRSHEVNPAAHLTGANSSLTGSGGPLLW

ETQLGLAFLRGLSYHDGALVVTKAGYYYIYSKVQLGGVGC

PLGLASTITHGLYKRTPRYPEELELLVSQQSPCGRATSSSRV

WWDSSFLGGVVHLEAGEEVVVRVLDERLVRLRDGTRSYFG

AFMVGGGSISSGLLSGRSDNIGGGSSGGSRHPCRHDPHIICY

KF

47
ProC1498/
GGCTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTT

ProC_cMyc-HSA-
GGCGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAA

21GS-1204DNI-
GACCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATT

LIGHT-mLm16
GCCTTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATC

DNA
ATGTCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGA

CCTGTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAAT

CATTGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGC

CACGCTCCGCGAGACATACGGCGAAATGGCCGATTGTTG

TGCGAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCA

ACACAAAGACGATAATCCCAATCTTCCGCGACTGGTGAG

ACCCGAAGTAGATGTAATGTGCACAGCTTTTCATGACAAT

GAGGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCC

CGCCGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTT

TCGCAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCA

GGCCGCTGATAAAGCCGCTTGTCTtCTGCCTAAGCTTGAT

GAGCTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAA

CGCCTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGA

GCCTTCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGT

TCCCGAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAA

CGGACCTGACAAAGGTACATACCGAATGCTGCCATGGCG

ACCTGTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCA

AGTATATTTGCGAAAACCAAGACTCCATTTCCAGTAAACT

TAAGGAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCA

TTGTATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGA

TCTGCCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGAT

GTATGTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTG

GAATGTTCTTGTATGAATACGCCCGACGGCATCCTGACTA

TTCAGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAG

ACGACACTTGAAAAGTGTTGTGCCGCtGCtGACCCACATG

AGTGCTACGCTAAGGTTTTCGACGAATTTAAGCCaTTGGT

TGAAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGCT

CTTTGAACAACTCGGTGAATACAAATTTCAGAACGCGCTT

CTGGTTAGATATACGAAGAAAGTGCCACAGGTGAGCACC

CCTACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTG

GGATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATG

CCTTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGC

TTTGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGT

CACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACC

TTGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCA

AAGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGAT

ATTTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAG

CAAACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAA

GCGACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTC

GCTGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAG

GAAACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCC

GCTAGTCAGGCGGCACTTGGTTTGTCCAGCGCCGGGGGC

GGAAGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGACAA

CATCGGCAGCCAGGAGAGACGGAGCCACGAGGTGAACC

CCGCTGCCCACCTGACCGGCGCCAACAGCAGTCTGACCG

GCAGCGGCGGCCCTCTGCTGTGGGAGACACAGCTGGGCC

TGGCCTTTCTGAGAGGCCTGTCCTACCACGACGGCGCCCT

GGTCGTGACCAAGGCCGGCTACTACTACATCTACAGCAA

GGTGCAGCTGGGAGGCGTGGGCTGCCCTCTGGGCCTGGC

ATCTACCATCACGCACGGCCTGTACAAGCGGACCCCTAG

ATATCCTGAGGAACTGGAACTCCTGGTGTCCCAGCAGAG

CCCTTGCGGCAGAGCTACAAGCAGCTCAAGAGTGTGGTG

GGACAGCAGCTTCCTGGGCGGAGTGGTCCACCTGGAAGC

TGGAGAAGAAGTGGTGGTCCGGGTGCTGGACGAGAGACT

CGTGAGGCTGAGAGACGGAACAAGAAGCTACTTCGGCGC

TTTTATGGTGGGCGGAGGCTCCATTTCTAGCGGCCTGCTG

AGCGGCAGAAGCGATAACATCGGCGGaGGAAGCAGCGGA

GGCAGCAGACACCCCTGCAGACACGATCCTCACATCATC

TGCTACAAGTTCtga

48
ProC1162/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

16_1490_LIGHT_
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

11linker_HSA-cMyc
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGG

GSSGGSDAHKSEVAHRFKDLGEENFKALVLIAFAQYLQQCP

FEDHVKLVNEVTEFAKTCVADESAENCDKSLHTLFGDKLCT

VATLRETYGEMADCCAKQEPERNECFLQHKDDNPNLPRLV

RPEVDVMCTAFHDNEETFLKKYLYEIARRHPYFYAPELLFF

AKRYKAAFTECCQAADKAACLLPKLDELRDEGKASSAKQR

LKCASLQKFGERAFKAWAVARLSQRFPKAEFAEVSKLVTD

LTKVHTECCHGDLLECADDRADLAKYICENQDSISSKLKEC

CEKPLLEKSHCIAEVENDEMPADLPSLAADFVESKDVCKNY

AEAKDVFLGMFLYEYARRHPDYSVVLLLRLAKTYETTLEK

CCAAADPHECYAKVFDEFKPLVEEPQNLIKQNCELFEQLGE

YKFQNALLVRYTKKVPQVSTPTLVEVSRNLGKVGSKCCKH

PEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDRVTKCCTESL

VNRRPCFSALEVDETYVPKEFNAETFTFHADICTLSEKERQI

KKQTALVELVKHKPKATKEQLKAVMDDFAAFVEKCCKAD

DKETCFAEEGKKLVAASQAALGLSGGEQKLISEEDL

49
ProC1162/
CAAGGGCAATCCGGATCTCGGCATCCGTGTCGGCATGAC

ProC_mLm-
CCTCACATCATATGCTATAAGTTTGGGGGGGGATCCTCAG

16_1490_LIGHT_
GTGGTTCCATTTCTTCTGGTTTGTTGTCTGGAAGATCAGA

11linker_HSA-cMyc
CAACATCGGCGGATCTCAAGAAAGACGCTCTCATGAGGT

DNA
GAATCCTGCCGCGCACCTTACTGGGGCAAACTCCAGTCT

GACCGGATCAGGTGGGCCATTGCTTTGGGAGACACAGTT

GGGACTGGCATTCCTTCGAGGCCTCAGCTACCATGATGGC

GCCCTGGTCGTAACGAAAGCTGGGTATTACTATATATATA

GCAAAGTCCAACTGGGGGGGGTTGGGTGTCCCCTGGGGC

TCGCGTCAACCATCACCCACGGACTCTATAAGAGAACAC

CAAGATACCCAGAAGAGTTGGAACTTCTCGTGTCTCAAC

AAAGTCCATGTGGGAGGGCAACATCTTCTTCACGCGTAT

GGTGGGATTCATCCTTTCTCGGTGGCGTTGTCCATCTTGA

AGCAGGGGAGGAAGTTGTTGTCAGAGTCTTGGATGAAAG

ACTCGTGAGATTGCGGGATGGTACTAGATCCTACTTCGGC

GCGTTCATGGTCTCCTCAGCGGGAGGTGGGAGTAGTGGC

GGCTCAGACGCCCATAAATCCGAAGTGGCACATCGATTT

AAGGACCTCGGGGAGGAGAACTTCAAAGCTCTGGTACTC

ATCGCCTTTGCTCAGTACTTGCAGCAATGCCCCTTCGAGG

ATCATGTCAAACTCGTGAACGAGGTTACGGAGTTCGCTA

AAACATGTGTTGCTGACGAGTCTGCAGAGAACTGTGACA

AATCCCTCCACACGCTGTTCGGTGATAAACTGTGTACGGT

GGCTACCCTCAGGGAAACCTACGGAGAGATGGCCGATTG

TTGCGCCAAACAGGAGCCTGAGAGGAACGAATGCTTTCT

TCAACACAAGGATGACAATCCTAACTTGCCTAGGCTGGTT

CGGCCCGAGGTCGATGTGATGTGCACAGCGTTTCACGAC

AACGAAGAAACATTCCTGAAGAAATACTTGTACGAGATT

GCTAGGCGACACCCATATTTCTACGCGCCGGAGCTTCTCT

TCTTTGCGAAGCGCTACAAGGCTGCATTTACAGAGTGCTG

CCAAGCCGCTGATAAGGCGGCCTGTCTTCTCCCCAAGCTC

GATGAACTCCGAGATGAAGGGAAAGCTTCATCAGCGAAA

CAAAGATTGAAATGTGCTTCCCTCCAAAAGTTTGGAGAA

CGAGCCTTTAAGGCTTGGGCAGTGGCACGGCTCAGTCAG

CGCTTTCCTAAGGCTGAATTTGCCGAAGTGTCCAAGCTTG

TAACGGATCTCACTAAAGTTCATACTGAATGCTGCCACGG

AGACCTTCTCGAATGCGCGGACGATCGCGCGGACTTGGC

GAAATATATATGCGAGAATCAAGATAGTATCAGCAGTAA

ACTCAAAGAGTGCTGCGAGAAGCCTCTCCTCGAAAAGAG

CCACTGTATCGCCGAGGTGGAAAATGATGAGATGCCTGC

GGACTTGCCATCCCTTGCCGCAGACTTTGTCGAATCAAAA

GACGTTTGCAAGAATTACGCGGAGGCAAAAGATGTATTC

CTTGGCATGTTCTTGTACGAATACGCACGGCGCCACCCTG

ACTATTCAGTAGTGTTGCTCTTGAGACTCGCTAAAACATA

CGAAACGACGCTTGAGAAATGTTGCGCAGCAGCCGATCC

CCACGAGTGTTACGCAAAGGTGTTCGACGAGTTTAAACC

CCTCGTTGAAGAACCTCAAAACCTGATAAAACAAAATTG

TGAGTTGTTCGAGCAGTTGGGAGAGTACAAGTTTCAGAA

TGCTCTCCTGGTTCGGTACACCAAGAAGGTCCCACAAGTG

TCCACGCCCACCCTCGTAGAGGTATCACGGAACCTTGGC

AAGGTCGGTAGCAAGTGCTGCAAACACCCAGAAGCTAAG

CGCATGCCATGCGCTGAAGACTATCTGTCTGTGGTGCTTA

ATCAATTGTGTGTACTGCATGAGAAAACTCCTGTGTCCGA

CCGGGTTACCAAGTGCTGTACCGAGTCACTCGTCAACCG

GCGACCTTGTTTTTCTGCGCTGGAGGTTGATGAGACGTAT

GTTCCGAAAGAATTCAACGCCGAGACTTTCACCTTCCATG

CTGATATATGCACACTCAGTGAAAAAGAACGACAAATAA

AGAAGCAAACCGCATTGGTCGAGCTGGTCAAGCATAAAC

CCAAAGCTACAAAAGAACAATTGAAGGCTGTTATGGATG

ACTTTGCCGCGTTCGTAGAGAAATGCTGCAAGGCAGATG

ATAAAGAGACATGTTTCGCCGAAGAGGGCAAGAAACTGG

TGGCCGCCTCTCAAGCTGCACTTGGGCTCTCTGGAGGCGA

ACAAAAGCTTATAAGCGAAGAGGACTTGTGA

50
ProC1163/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

16_1490_LIGHT_
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

21linker_HSA-cMyc
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

Protein
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVSSAGG

GSSGGSSAGGGSSGGSDAHKSEVAHRFKDLGEENFKALVLI

AFAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKS

LHTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQH

KDDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRH

PYFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRD

EGKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAE

FAEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICEN

QDSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADF

VESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRL

AKTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQ

NCELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLG

KVGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSD

RVTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADI

CTLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAA

FVEKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLIS

EEDL

51
ProC1163/
CAGGGACAGTCCGGATCTAGGCATCCATGTCGGCATGAC

ProC_mLm-
CCACATATCATATGCTACAAATTCGGTGGAGGATCTTCTG

16_1490_LIGHT_
GAGGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGA

21linker_HSA-cMyc
CAATATTGGTGGCTCCCAGGAGAGGAGATCACATGAAGT

DNA
CAACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGTCTT

ACAGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGCTG

GGACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGGG

GCGTTGGTCGTTACTAAAGCCGGGTATTACTATATATACT

CTAAGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTCT

TGCGTCTACAATTACACATGGTCTGTATAAGAGGACTCCC

AGATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCAAT

CTCCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTGGT

GGGACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAGGC

GGGAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGCCT

TGTACGACTTCGGGACGGTACAAGAAGCTACTTTGGGGC

TTTCATGGTATCTTCTGCAGGGGGGGGGTCATCCGGCGGA

AGTTCAGCGGGGGGGGGATCCTCCGGTGGCAGTGATGCA

CATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTCGGC

GAGGAGAACTTCAAGGCACTCGTACTTATTGCCTTTGCAC

AATACCTGCAGCAATGTCCGTTTGAAGATCATGTCAAGCT

CGTAAATGAAGTGACAGAGTTCGCTAAGACCTGTGTAGC

TGACGAAAGTGCCGAAAACTGCGACAAATCATTGCATAC

ATTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTCCGC

GAGACATACGGCGAAATGGCCGATTGTTGTGCGAAACAG

GAACCCGAAAGAAATGAGTGCTTCTTGCAACACAAAGAC

GATAATCCCAATCTTCCGCGACTGGTGAGACCCGAAGTA

GATGTAATGTGCACAGCTTTTCATGACAATGAGGAAACC

TTTCTTAAAAAATATCTGTACGAAATCGCCCGCCGACACC

CGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGCG

CTACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGCTGA

TAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCGC

GACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAAG

TGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAGG

CTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAGG

CGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTGA

CAAAGGTACATACCGAATGCTGCCATGGCGACCTGTTGG

AGTGCGCCGATGATCGAGCGGATCTTGCCAAGTATATTTG

CGAAAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTG

TTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCG

GAGGTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCA

CTCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAA

ACTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTT

GTATGAATACGCCCGACGGCATCCTGACTATTCAGTTGTG

CTCCTTCTTCGATTGGCTAAAACTTATGAGACGACACTTG

AAAAGTGTTGTGCCGCCGCCGACCCACATGAGTGCTACG

CTAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACC

GCAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACA

ACTCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGA

TATACGAAGAAAGTGCCACAGGTGAGCACCCCTACATTG

GTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAG

TGCTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCT

GAGGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTC

TTCACGAAAAGACTCCCGTCAGCGACCGAGTCACGAAGT

GCTGTACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTC

CGCGCTTGAGGTGGATGAGACCTACGTCCCAAAGGAATT

CAACGCCGAGACGTTCACTTTCCATGCCGATATTTGCACC

TTGTCAGAAAAGGAGCGACAGATAAAAAAGCAAACTGCT

TTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAG

GAACAGCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCG

TGGAGAAATGTTGTAAGGCCGATGACAAGGAAACCTGCT

TCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGG

CGGCACTTGGTTTGTCAGGTGGGGAGCAGAAACTTATCTC

CGAAGAGGATTTGTAA

52
ProC1164/
QGQSGSRHPCRHDPHIICYKFGGGSSGGSISSGLLSGRSDNIG

ProC_mLm-
GSQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFL

16_1490_LIGHT_
RGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITH

IgG4 WT hinge_HSA-
GLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGG

cMyc
VVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMVESKYG

Protein
PPCPSCPAPEFLGGPSDAHKSEVAHRFKDLGEENFKALVLIA

FAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAENCDKSL

HTLFGDKLCTVATLRETYGEMADCCAKQEPERNECFLQHK

DDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEIARRHP

YFYAPELLFFAKRYKAAFTECCQAADKAACLLPKLDELRDE

GKASSAKQRLKCASLQKFGERAFKAWAVARLSQRFPKAEF

AEVSKLVTDLTKVHTECCHGDLLECADDRADLAKYICENQ

DSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSLAADFV

ESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVVLLLRLA

KTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQNLIKQN

CELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEVSRNLGK

VGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEKTPVSDR

VTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFTFHADIC

TLSEKERQIKKQTALVELVKHKPKATKEQLKAVMDDFAAF

VEKCCKADDKETCFAEEGKKLVAASQAALGLSGGEQKLISE

EDL

53
ProC1164/
CAAGGCCAGAGTGGGAGTAGGCATCCATGTCGCCATGAT

ProC_mLm-
CCTCACATTATATGCTATAAATTTGGTGGGGGAAGCAGTG

16_1490_LIGHT_
GTGGGTCCATCAGTAGTGGGCTGTTGTCCGGTCGGAGTG

IgG4 WT hinge_HSA-
ATAATATTGGAGGCTCCCAGGAACGCAGGAGTCATGAAG

cMyc
TTAACCCGGCGGCACATCTTACGGGTGCGAACTCTAGTCT

DNA
TACCGGGAGTGGGGGGCCCCTGCTTTGGGAGACACAGCT

TGGGCTCGCTTTCCTCAGGGGACTCTCTTACCATGATGGC

GCACTGGTAGTAACCAAAGCTGGATACTATTATATTTACT

CTAAAGTTCAATTGGGGGGCGTTGGCTGCCCACTCGGCCT

CGCATCTACTATCACCCATGGGTTGTATAAGCGGACCCCT

AGATACCCTGAGGAACTTGAGCTTTTGGTTTCTCAACAGT

CACCTTGCGGTAGGGCTACCTCATCAAGCCGCGTTTGGTG

GGACAGTTCATTTCTCGGGGGCGTAGTCCATCTGGAGGC

AGGTGAGGAAGTAGTGGTTCGAGTGCTCGACGAGCGCCT

CGTACGACTCCGGGATGGGACGAGAAGTTATTTCGGCGC

CTTTATGGTAGAGTCAAAATACGGGCCTCCCTGTCCCTCT

TGTCCGGCACCCGAATTTCTTGGCGGGCCCTCTGATGCCC

ACAAGTCTGAAGTTGCGCATAGATTTAAAGACCTCGGAG

AGGAGAATTTTAAAGCACTCGTGCTTATCGCATTTGCGCA

GTACCTGCAGCAGTGCCCTTTCGAGGACCACGTCAAGCTT

GTCAACGAGGTGACAGAATTCGCCAAAACATGTGTCGCC

GATGAGTCTGCCGAGAACTGTGACAAAAGTTTGCATACC

CTGTTCGGCGACAAACTCTGCACTGTAGCAACTCTTAGGG

AAACATACGGGGAAATGGCAGACTGTTGCGCGAAACAGG

AGCCAGAACGAAACGAATGTTTCTTGCAGCACAAGGATG

ATAACCCTAATCTCCCGAGGTTGGTCAGGCCCGAAGTCG

ACGTAATGTGCACGGCTTTCCATGACAATGAGGAAACCT

TCCTCAAGAAGTACCTCTACGAAATAGCACGAAGACATC

CGTATTTCTATGCTCCTGAGCTGCTCTTTTTCGCTAAACGC

TATAAGGCCGCATTCACGGAGTGTTGTCAAGCCGCCGAT

AAGGCTGCTTGCCTTCTGCCCAAGTTGGACGAACTGCGCG

ATGAGGGGAAAGCATCATCAGCAAAGCAACGCCTGAAAT

GCGCTAGTTTGCAAAAATTCGGGGAACGCGCCTTCAAAG

CTTGGGCTGTCGCGCGGCTCTCACAGAGGTTCCCCAAGG

CTGAGTTCGCCGAAGTTTCCAAGCTGGTTACTGATTTGAC

CAAAGTGCACACAGAATGTTGCCACGGCGACCTGCTTGA

GTGTGCGGATGACCGCGCAGATCTCGCGAAGTATATATG

CGAAAACCAGGATTCAATTAGCTCTAAATTGAAAGAATG

TTGTGAGAAACCTCTGCTTGAAAAGTCACACTGCATTGCG

GAGGTGGAAAATGATGAAATGCCCGCAGATCTCCCCTCT

TTGGCAGCGGACTTCGTGGAGAGTAAAGACGTCTGTAAG

AATTACGCCGAGGCGAAGGATGTATTCCTGGGGATGTTT

CTCTATGAATACGCTCGCAGACATCCTGACTACTCTGTGG

TGCTGCTGTTGCGCCTCGCTAAGACCTACGAAACAACCCT

GGAAAAATGTTGTGCCGCAGCTGATCCACACGAATGCTA

TGCTAAAGTCTTTGATGAATTTAAGCCTTTGGTTGAGGAG

CCCCAGAACCTGATAAAACAGAACTGTGAATTGTTCGAG

CAACTTGGAGAGTATAAATTCCAAAACGCGCTTCTCGTGC

GGTACACCAAGAAGGTGCCTCAAGTCAGTACTCCAACCC

TTGTGGAGGTAAGTCGCAATCTCGGTAAAGTTGGCAGTA

AATGTTGTAAGCATCCTGAAGCGAAGCGCATGCCTTGTG

CAGAGGACTATCTGTCAGTAGTTCTTAACCAGCTGTGTGT

GCTTCATGAGAAAACACCCGTGTCCGACAGGGTGACAAA

GTGTTGCACTGAGAGTCTCGTGAACCGGAGACCTTGTTTC

TCCGCCCTGGAAGTGGACGAAACCTATGTGCCGAAGGAA

TTCAATGCTGAAACGTTTACGTTCCATGCCGACATCTGCA

CGCTTAGCGAGAAAGAGAGACAGATAAAGAAGCAAACC

GCCTTGGTGGAACTCGTTAAGCACAAGCCAAAAGCAACC

AAAGAACAACTCAAAGCGGTCATGGACGATTTCGCTGCA

TTTGTAGAGAAATGCTGCAAAGCGGATGACAAGGAGACG

TGTTTCGCTGAAGAGGGAAAAAAGCTCGTGGCAGCATCC

CAGGCTGCACTTGGTCTGTCTGGTGGTGAGCAAAAACTG

ATTTCAGAGGAGGATTTGTGA

54
human LIGHT
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

protomer
LSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTITHGL

YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

HLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMV

55
mouse-human
QERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLAFLRG

LIGHT protomer
LSYHDGALVVTKTGYYYIYSKVQLGGVGCPLGLAGTITHGL

YKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFLGGVV

HLEAGEEVVVRVLGKRLVRLRDGTRSYFGAFMV

56
HSA
DAHKSEVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVK

LVNEVTEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRE

TYGEMADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDV

MCTAFHDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKA

AFTECCQAADKAACLLPKLDELRDEGKASSAKQRLKCASL

QKFGERAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHT

ECCHGDLLECADDRADLAKYICENQDSISSKLKECCEKPLLE

KSHCIAEVENDEMPADLPSLAADFVESKDVCKNYAEAKDV

FLGMFLYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADP

HECYAKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNAL

LVRYTKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMP

CAEDYLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCF

SALEVDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALV

ELVKHKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAE

EGKKLVAASQAALGL

57
3HB-Trimerization
EIAALKQEIAALKKEIAALKWEIAALKQGYY

three helix bundle

58
His
HHHHHH

59
cMyc
EQKLISEEDL

60
Strep
SAWSHPQFEK

61
mLm16
RHPCRHDPHIICYKF

62
1490DNI
ISSGLLSGRSDNI

63
1204DNI
LSGRSDNI

64
Linker (11)
SSAGGGSSGGS

65
Linker (21)
SSAGGGSSGGSSAGGGSSGGS

66
Linker (10)
SGGGSGGGSG

67
Linker (11c)
GGGSSGGSGS

68
Linker (8)
GGGSSGGS

69
Linker (11b)
SGGGSGGGSGS

Linker (3a)
GGS

Linker (3b)
SGG

Linker (3c)
GSG

Linker(2)
GS

Linker(1b)
G

75
Linker(4)
GGGS

76
Header
QGQSGS

77
Linker (IgG4 WT
ESKYGPPCPSCPAPEFLGGPS

hinge)

78
signal peptide
METDTLLLWVLLLWVPGSTG

79
Full length human
MEESVVRPSVFVVDGQTDIPFTRLGRSHRRQSCSVARVGLG

LIGHT
LLLLLMGAGLAVQGWFLLQLHWRLGEMVTRLPDGPAGSW

EQLIQERRSHEVNPAAHLTGANSSLTGSGGPLLWETQLGLA

FLRGLSYHDGALVVTKAGYYYIYSKVQLGGVGCPLGLASTI

THGLYKRTPRYPEELELLVSQQSPCGRATSSSRVWWDSSFL

GGVVHLEAGEEVVVRVLDERLVRLRDGTRSYFGAFMV

Linker (1a)
S

81
1490DNI-SER to
ISSGLLSGRCDNI

CYS

82
ProC1189/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_LIGHT-10GS-
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYS

His
KVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPC

Protein with signal
GRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRL

sequence
RDGTRSYFGAFMVSGGGSGGGSGHHHHHH

83
ProC1189/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_LIGHT-10GS-
GGAACGGCGCTCCCACGAGGTCAATCCGGCGGCTCATTT

His
GACTGGAGCCAACTCTAGTCTTACCGGGAGCGGCGGTCC

DNA with coding
ATTGCTGTGGGAGACGCAACTTGGATTGGCTTTTCTTCGG

sequence for signal
GGATTGTCTTACCACGATGGAGCACTCGTTGTTACGAAAG

peptide
CCGGTTACTACTACATTTATTCTAAGGTCCAGTTGGGTGG

AGTTGGCTGTCCCCTGGGACTTGCAAGCACTATCACTCAC

GGACTGTACAAGAGGACACCCCGATACCCCGAGGAACTC

GAGCTGCTTGTGAGCCAACAGTCTCCATGTGGGCGCGCA

ACTAGTTCTTCACGGGTGTGGTGGGACTCCAGTTTCCTGG

GAGGTGTTGTTCATCTCGAGGCAGGTGAAGAAGTAGTTG

TCAGGGTACTTGATGAACGGCTTGTTAGACTCCGGGATG

GAACGAGGTCCTATTTCGGTGCGTTCATGGTAAGCGGGG

GCGGAAGTGGGGGCGGGTCAGGTCATCATCACCACCATC

ATTGA

84
ProC1193/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

16_1490_LIGHT_
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

10GS His
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

Protein with signal
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

sequence
RLRDGTRSYFGAFMVSGGGSGGGSGHHHHHH

85
ProC1193/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm-
AGGACAAAGTGGTTCCCGACACCCGTGCAGGCATGACCC

16_1490_LIGHT_
ACATATAATCTGTTATAAGTTTGGTGGAGGCTCCTCCGGC

10GS His
GGGTCTATCAGTTCCGGTCTCCTCAGCGGTCGCAGTGATA

DNA with coding
ATATCGGCGGTTCTCAGGAACGCAGGTCACACGAGGTAA

sequence for signal
ATCCAGCCGCCCATTTGACTGGCGCTAATAGTTCTCTTAC

peptide
GGGTAGCGGTGGCCCTCTTCTGTGGGAAACGCAGTTGGG

CTTGGCTTTCCTTAGAGGTCTCAGCTATCACGACGGCGCC

CTCGTCGTTACAAAGGCCGGGTACTATTATATTTATTCTA

AGGTACAGCTTGGCGGGGTGGGGTGCCCGCTGGGTCTTG

CATCTACGATCACTCATGGTCTCTACAAAAGAACACCAA

GGTATCCAGAAGAACTTGAGCTCCTCGTTAGCCAACAGT

CCCCCTGCGGACGGGCTACTTCCTCTAGCCGGGTATGGTG

GGATAGCAGTTTCCTTGGGGGGGTCGTGCATCTCGAGGCT

GGAGAGGAGGTAGTAGTCAGGGTCTTGGATGAGAGATTG

GTAAGGCTTCGAGACGGTACAAGATCATACTTTGGGGCC

TTCATGGTGAGCGGGGGTGGCAGCGGCGGTGGCAGCGGG

CATCATCACCATCACCATTGA

86
ProC1188/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_LIGHT-10GS-
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYS

Strep
KVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPC

Protein with signal
GRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRL

sequence
RDGTRSYFGAFMVSGGGSGGGSGSAWSHPQFEK

87
ProC1188/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_LIGHT-10GS-
GGAACGCAGGTCCCATGAAGTAAACCCGGCGGCCCATCT

Strep
TACGGGTGCAAATTCAAGCTTGACAGGCAGCGGAGGGCC

DNA with coding
GCTCCTGTGGGAGACGCAACTTGGGCTTGCGTTTCTCCGG

sequence for signal
GGCCTGTCATATCACGACGGTGCTCTTGTGGTAACGAAA

peptide
GCAGGGTACTATTATATATATAGCAAGGTTCAGTTGGGTG

GGGTTGGATGCCCGCTTGGACTCGCGTCCACTATTACTCA

CGGGTTGTATAAGAGGACACCGCGATACCCAGAGGAGCT

GGAACTCCTTGTTTCACAGCAGTCTCCTTGCGGGAGAGCC

ACATCTTCATCCAGGGTCTGGTGGGACTCTTCTTTCTTGG

GCGGCGTTGTTCATCTGGAAGCGGGGGAAGAGGTTGTAG

TGAGGGTACTCGACGAGAGGCTGGTGAGGCTGCGAGACG

GGACCCGCTCATATTTCGGAGCCTTCATGGTATCAGGAGG

GGGCTCCGGTGGGGGGTCAGGAAGCGCATGGTCACACCC

TCAGTTCGAGAAATGA

88
ProC1192/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm16_1490_
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

LIGHT-10GS-Strep
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

Protein with signal
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

sequence
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

RLRDGTRSYFGAFMVSGGGSGGGSGSAWSHPQFEK

89
ProC1192/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm16_1490_
AGGACAGAGTGGAAGTCGACACCCTTGTAGGCACGACCC

LIGHT-10GS-Strep
ACATATAATCTGCTATAAATTTGGTGGGGGTTCCAGCGGT

DNA with coding
GGAAGTATCAGCTCCGGCCTTCTTAGTGGCAGGAGTGAC

sequence for signal
AATATTGGCGGATCTCAAGAGCGACGCAGTCACGAGGTA

peptide
AATCCTGCAGCACACTTGACAGGTGCTAACAGCTCACTTA

CCGGAAGTGGGGGGCCGCTGTTGTGGGAGACGCAGCTCG

GGTTGGCCTTTCTTCGAGGGCTCTCTTATCACGACGGTGC

ATTGGTGGTGACCAAAGCAGGGTATTACTACATATACTCT

AAGGTGCAACTGGGTGGAGTAGGTTGTCCATTGGGGCTC

GCCTCTACAATAACTCATGGTCTGTATAAGCGAACCCCGC

GGTATCCCGAAGAGCTTGAACTCCTCGTCAGCCAGCAAT

CTCCCTGTGGTCGGGCAACATCATCTAGCAGAGTGTGGTG

GGACTCCTCTTTTTTGGGTGGTGTAGTACATCTGGAAGCG

GGCGAAGAAGTGGTCGTCCGAGTGCTTGACGAACGACTC

GTTAGACTGCGAGACGGAACTCGGAGCTACTTTGGAGCT

TTTATGGTTAGCGGTGGTGGTTCAGGAGGTGGGAGTGGG

AGTGCATGGTCACACCCGCAATTCGAGAAATGA

90
ProC1491/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_LIGHT-
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYS

1204DNI-HSA-His
KVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPC

Protein with signal
GRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRL

sequence
RDGTRSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHKSEV

AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLSHHHHHH

91
ProC1491/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_LIGHT-
GGAGAGGAGATCACATGAAGTCAACCCGGCCGCCCATCT

1204DNI-HSA-His
TACTGGTGCCAATAGTAGTCTTACAGGTTCTGGCGGACCC

DNA with coding
TTGCTTTGGGAGACCCAGCTGGGACTGGCTTTCCTTAGAG

sequence for signal
GCCTGAGTTATCACGACGGGGCGTTGGTCGTTACTAAAG

peptide
CCGGGTATTACTATATATACTCTAAGGTTCAGCTCGGCGG

TGTAGGATGCCCACTGGGTCTTGCGTCTACAATTACACAT

GGTCTGTATAAGAGGACTCCCAGATATCCAGAAGAACTG

GAATTGCTTGTTTCCCAGCAATCTCCGTGCGGACGCGCAA

CGAGCTCCAGTAGGGTGTGGTGGGACTCCAGCTTCCTGG

GTGGCGTTGTCCATTTGGAGGCGGGAGAGGAAGTAGTGG

TGCGGGTCCTTGATGAACGCCTTGTACGACTTCGGGACGG

TACAAGAAGCTACTTTGGGGCTTTCATGGTATCCAGCGCC

GGGGGCGGAAGCAGCGGCGGCAGCTTAAGCGGCAGAAG

CGACAACATCGGCAGCGATGCACATAAAAGTGAGGTGGC

CCACCGCTTTAAAGACCTCGGCGAGGAGAACTTCAAGGC

ACTCGTACTTATTGCCTTTGCACAATACCTGCAGCAATGT

CCGTTTGAAGATCATGTCAAGCTCGTAAATGAAGTGACA

GAGTTCGCTAAGACCTGTGTAGCTGACGAAAGTGCCGAA

AACTGCGACAAATCATTGCATACATTGTTCGGCGACAAG

CTTTGTACAGTTGCCACGCTCCGCGAGACATACGGCGAA

ATGGCCGATTGTTGTGCGAAACAGGAACCCGAAAGAAAT

GAGTGCTTCTTGCAACACAAAGACGATAATCCCAATCTTC

CGCGACTGGTGAGACCCGAAGTAGATGTAATGTGCACAG

CTTTTCATGACAATGAGGAAACCTTTCTTAAAAAATATCT

GTACGAAATCGCCCGCCGACACCCGTATTTCTATGCCCCA

GAGCTGTTGTTTTTCGCAAAGCGCTACAAGGCAGCGTTTA

CCGAATGCTGCCAGGCCGCTGATAAAGCCGCTTGTCTGCT

GCCTAAGCTTGATGAGCTTCGCGACGAGGGTAAGGCTTC

CAGCGCTAAACAACGCCTGAAGTGTGCATCTTTGCAAAA

ATTTGGTGAACGAGCCTTCAAGGCTTGGGCTGTTGCCAGG

CTGAGTCAACGGTTCCCGAAGGCGGAGTTTGCGGAGGTT

TCCAAGTTGGTAACGGACCTGACAAAGGTACATACCGAA

TGCTGCCATGGCGACCTGTTGGAGTGCGCCGATGATCGA

GCGGATCTTGCCAAGTATATTTGCGAAAACCAAGACTCC

ATTTCCAGTAAACTTAAGGAGTGTTGTGAGAAACCTCTCC

TTGAAAAGAGCCATTGTATAGCGGAGGTCGAAAACGATG

AAATGCCCGCTGATCTGCCGTCACTCGCTGCTGACTTCGT

TGAATCCAAGGATGTATGTAAAAACTATGCCGAAGCTAA

GGACGTCTTTCTTGGAATGTTCTTGTATGAATACGCCCGA

CGGCATCCTGACTATTCAGTTGTGCTCCTTCTTCGATTGG

CTAAAACTTATGAGACGACACTTGAAAAGTGTTGTGCCG

CCGCCGACCCACATGAGTGCTACGCTAAGGTTTTCGACG

AATTTAAGCCCTTGGTTGAAGAACCGCAGAATCTCATTAA

GCAAAATTGTGAGCTCTTTGAACAACTCGGTGAATACAA

ATTTCAGAACGCGCTTCTGGTTAGATATACGAAGAAAGT

GCCACAGGTGAGCACCCCTACATTGGTTGAGGTCAGTAG

GAACCTCGGCAAGGTGGGATCTAAGTGCTGCAAACACCC

GGAGGCAAAGAGAATGCCTTGCGCTGAGGATTATCTCTC

AGTGGTTCTGAATCAGCTTTGCGTTCTTCACGAAAAGACT

CCCGTCAGCGACCGAGTCACGAAGTGCTGTACCGAGAGC

CTTGTTAATAGACGACCTTGCTTCTCCGCGCTTGAGGTGG

ATGAGACCTACGTCCCAAAGGAATTCAACGCCGAGACGT

TCACTTTCCATGCCGATATTTGCACCTTGTCAGAAAAGGA

GCGACAGATAAAAAAGCAAACTGCTTTGGTGGAGCTGGT

TAAGCATAAGCCTAAAGCGACGAAGGAACAGCTCAAAGC

CGTAATGGATGATTTCGCTGCCTTCGTGGAGAAATGTTGT

AAGGCCGATGACAAGGAAACCTGCTTCGCTGAAGAGGGT

AAAAAGCTCGTCGCCGCTAGTCAGGCGGCACTTGGTTTG

AGCCACCATCACCACCACCACtga

92
ProC1492/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm16-
GGGSSGGSISSGLLSGRCDNIGGSQERRSHEVNPAAHLTGAN

LIGHT-1204DNI-
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

HSA-His (1490DNI
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

has S to C mutation)
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

Protein with signal
RLRDGTRSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHKS

sequence
EVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEV

TEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSHHHHHH

93
ProC1492/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm16-
GGGCCAGTCTGGATCCAGACACCCATGCAGACACGACCC

LIGHT-1204DNI-
CCACATCATCTGTTACAAATTCGGCGGAGGCAGCTCCGG

HSA-His (1490DNI
CGGCAGCATCTCCAGCGGACTGCTGAGCGGCAGAtGCGA

has S to C mutation)
TAACATCGGCGGAAGCCAGGAGAGGAGATCACATGAAGT

DNA with coding
CAACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGTCTT

sequence for signal
ACAGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGCTG

peptide
GGACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGGG

GCGTTGGTCGTTACTAAAGCCGGGTATTACTATATATACT

CTAAGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTCT

TGCGTCTACAATTACACATGGTCTGTATAAGAGGACTCCC

AGATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCAAT

CTCCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTGGT

GGGACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAGGC

GGGAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGCCT

TGTACGACTTCGGGACGGTACAAGAAGCTACTTTGGGGC

TTTCATGGTATCCAGCGCCGGGGGCGGAAGCAGCGGCGG

CAGCTTAAGCGGCAGAAGCGACAACATCGGCAGCGATGC

ACATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTCGG

CGAGGAGAACTTCAAGGCACTCGTACTTATTGCCTTTGCA

CAATACCTGCAGCAATGTCCGTTTGAAGATCATGTCAAGC

TCGTAAATGAAGTGACAGAGTTCGCTAAGACCTGTGTAG

CTGACGAAAGTGCCGAAAACTGCGACAAATCATTGCATA

CATTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTCCG

CGAGACATACGGCGAAATGGCCGATTGTTGTGCGAAACA

GGAACCCGAAAGAAATGAGTGCTTCTTGCAACACAAAGA

CGATAATCCCAATCTTCCGCGACTGGTGAGACCCGAAGT

AGATGTAATGTGCACAGCTTTTCATGACAATGAGGAAAC

CTTTCTTAAAAAATATCTGTACGAAATCGCCCGCCGACAC

CCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGC

GCTACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGCTG

ATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCG

CGACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAA

GTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAG

GCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAG

GCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTG

ACAAAGGTACATACCGAATGtTGCCATGGCGACCTGTTGG

AGTGCGCCGATGATCGAGCGGATCTTGCCAAGTATATTTG

CGAAAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTG

TTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCG

GAGGTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCA

CTCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAA

ACTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTT

GTATGAATACGCCCGACGGCATCCTGACTATTCAGTTGTG

CTCCTTCTTCGATTGGCTAAAACTTATGAGACGACACTTG

AAAAGTGTTGTGCCGCGGCGGACCCACATGAGTGCTACG

CTAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACC

GCAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACA

ACTCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGA

TATACGAAGAAAGTGCCACAGGTGAGCACCCCTACATTG

GTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAG

TGCTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCT

GAGGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTC

TTCACGAAAAGACTCCCGTCAGCGACCGAGTCACGAAGT

GCTGTACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTC

CGCGCTTGAGGTGGATGAGACCTACGTCCCAAAGGAATT

CAACGCCGAGACGTTCACTTTCCATGCCGATATTTGCACC

TTGTCAGAAAAGGAGCGACAGATAAAAAAGCAAACTGCT

TTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAG

GAACAGCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCG

TGGAGAAATGTTGTAAGGCCGATGACAAGGAAACCTGCT

TCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGG

CGGCACTTGGTTTGAGCCACCATCACCACCACCACtga

94
ProC1655/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm16-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

LIGHT-1204DNI-
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

HSA-His 1490
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

Protein with signal
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

sequence
RLRDGTRSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHKS

EVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEV

TEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSHHHHHH

95
ProC1655/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm16-
GGGCCAGTCTGGATCCAGACACCCATGCAGACACGACCC

LIGHT-1204DNI-
CCACATCATCTGTTACAAATTCGGCGGAGGCAGCTCCGG

HSA-His 1490
CGGCAGCATCTCCAGCGGACTGCTGAGCGGCAGAAGCGA

DNA with coding
TAACATCGGCGGAAGCCAGGAGAGGAGATCACATGAAGT

sequence for signal
CAACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGTCTT

peptide
ACAGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGCTG

GGACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGGG

GCGTTGGTCGTTACTAAAGCCGGGTATTACTATATATACT

CTAAGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTCT

TGCGTCTACAATTACACATGGTCTGTATAAGAGGACTCCC

AGATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCAAT

CTCCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTGGT

GGGACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAGGC

GGGAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGCCT

TGTACGACTTCGGGACGGTACAAGAAGCTACTTTGGGGC

TTTCATGGTATCCAGCGCCGGGGGCGGAAGCAGCGGCGG

CAGCTTAAGCGGCAGAAGCGAtAACATCGGCAGCGATGC

ACATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTCGG

CGAGGAGAACTTCAAGGCACTCGTACTTATTGCCTTTGCA

CAATACCTGCAGCAATGTCCGTTTGAAGATCATGTCAAGC

TCGTAAATGAAGTGACAGAGTTCGCTAAGACCTGTGTAG

CTGACGAAAGTGCCGAAAACTGCGACAAATCATTGCATA

CATTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTCCG

CGAGACATACGGCGAAATGGCCGATTGTTGTGCGAAACA

GGAACCCGAAAGAAATGAGTGCTTCTTGCAACACAAAGA

CGATAATCCCAATCTTCCGCGACTGGTGAGACCCGAAGT

AGATGTAATGTGCACAGCTTTTCATGACAATGAGGAAAC

CTTTCTTAAAAAATATCTGTACGAAATCGCCCGCCGACAC

CCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGC

GCTACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGCTG

ATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCG

CGACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAA

GTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAG

GCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAG

GCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTG

ACAAAGGTACATACCGAATGUTGCCATGGCGACCTGTTGG

AGTGCGCCGATGATCGAGCGGATCTTGCCAAGTATATTTG

CGAAAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTG

TTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCG

GAGGTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCA

CTCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAA

ACTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTT

GTATGAATACGCCCGACGGCATCCTGACTATTCAGTTGTG

CTCCTTCTTCGATTGGCTAAAACTTATGAGACGACACTTG

AAAAGTGTTGTGCCGCGGCGGACCCACATGAGTGCTACG

CTAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACC

GCAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACA

ACTCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGA

TATACGAAGAAAGTGCCACAGGTGAGCACCCCTACATTG

GTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAG

TGCTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCT

GAGGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTC

TTCACGAAAAGACTCCCGTCAGCGACCGAGTCACGAAGT

GCTGTACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTC

CGCGCTTGAGGTGGATGAGACCTACGTCCCAAAGGAATT

CAACGCCGAGACGTTCACTTTCCATGCCGATATTTGCACC

TTGTCAGAAAAGGAGCGACAGATAAAAAAGCAAACTGCT

TTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAG

GAACAGCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCG

TGGAGAAATGTTGTAAGGCCGATGACAAGGAAACCTGCT

TCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGG

CGGCACTTGGTTTGAGCCACCATCACCACCACCACtga

96
ProC1499/
METDTLLLWVLLLWVPGSTGDAHKSEVAHRFKDLGEENFK

ProC_HSA-21GS-
ALVLIAFAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAEN

1204DNI-LIGHT
CDKSLHTLFGDKLCTVATLRETYGEMADCCAKQEPERNEC

Protein with signal
FLQHKDDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEI

sequence
ARRHPYFYAPELLFFAKRYKAAFTECCQAADKAACLLPKL

DELRDEGKASSAKQRLKCASLQKFGERAFKAWAVARLSQR

FPKAEFAEVSKLVTDLTKVHTECCHGDLLECADDRADLAK

YICENQDSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSL

AADFVESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVV

LLLRLAKTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQ

NLIKQNCELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEV

SRNLGKVGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEK

TPVSDRVTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFT

FHADICTLSEKERQIKKQTALVELVKHKPKATKEQLKAVMD

DFAAFVEKCCKADDKETCFAEEGKKLVAASQAALGLSSAG

GGSSGGSLSGRSDNIGSQERRSHEVNPAAHLTGANSSLTGSG

GPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYSKVQL

GGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPCGRAT

SSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRLRDGT

RSYFGAFMV

97
ProC1499/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcGA

ProC_HSA-21GS-
TGCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCT

1204DNI-LIGHT
CGGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCCTTT

DNA with coding
GCACAATACCTGCAGCAATGTCCGTTTGAAGATCATGTCA

sequence for signal
AGCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCTGTG

peptide
TAGCTGACGAAAGTGCCGAAAACTGCGACAAATCATTGC

ATACATTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCT

CCGCGAGACATACGGCGAAATGGCCGATTGTTGTGCGAA

ACAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACACAA

AGACGATAATCCCAATCTTCCGCGACTGGTGAGACCCGA

AGTAGATGTAATGTGCACAGCTTTTCATGACAATGAGGA

AACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGCCGA

CACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAA

AGCGCTACAAGGCAGCGTTTACaGAATGCTGtCAGGCCGC

TGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTT

CGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTG

AAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCA

AGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGA

AGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACC

TGACAAAGGTACATACCGAATGCTGCCATGGCGACCTGT

TGGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTATA

TTTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAGG

AGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGTAT

AGCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTGCC

GTCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTATGT

AAAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAATG

TTCTTGTATGAATACGCCCGACGGCATCCTGACTATTCAG

TTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACGAC

ACTTGAAAAGTGTTGTGCCGCCGCCGACCCACATGAGTG

CTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAA

GAACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCTTTG

AACAACTCGGTGAATACAAATTTCAGAACGCGCTTCTGG

TTAGATATACGAAGAAAGTGCCACAGGTGAGCACCCCTA

CATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGAT

CTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATGCCTT

GCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTTTG

CGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGTCAC

GAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACCTTG

CTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCAAAG

GAATTCAACGCCGAGACGTTCACTTTCCATGCCGATATTT

GCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCAA

ACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCG

ACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTCGCT

GCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAGGAA

ACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCT

AGTCAGGCGGCACTTGGTTTGTCCAGCGCCGGGGGCGGA

AGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGACAACAT

CGGCAGCCAGGAGAGACGGAGCCACGAGGTGAACCCCG

CTGCCCACCTGACCGGCGCCAACAGCAGTCTGACCGGCA

GCGGCGGCCCTCTGCTGTGGGAGACACAGCTGGGCCTGG

CCTTTCTGAGAGGCCTGTCCTACCACGACGGCGCCCTGGT

CGTGACCAAGGCCGGCTACTACTACATCTACAGCAAGGT

GCAGCTGGGAGGCGTGGGCTGCCCTCTGGGCCTGGCATC

TACCATCACGCACGGCCTGTACAAGCGGACCCCTAGATA

TCCTGAGGAACTGGAACTCCTGGTGTCCCAGCAGAGCCC

TTGCGGCAGAGCTACAAGCAGCTCAAGAGTGTGGTGGGA

CAGCAGCTTCCTGGGCGGAGTGGTCCACCTGGAAGCTGG

AGAAGAAGTGGTGGTCCGGGTGCTGGACGAGAGACTCGT

GAGGCTGAGAGACGGAACAAGAAGCTACTTCGGCGCTTT

TATGGTGtga

98
ProC1495/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_LIGHT-
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYS

1204DNI-HSA-cmyc
KVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPC

Protein with signal
GRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRL

sequence
RDGTRSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHKSEV

AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLSGGEQKLISEEDL

99
ProC1495/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_LIGHT-
GGAGAGGAGATCACATGAAGTCAACCCGGCCGCCCATCT

1204DNI-HSA-cmyc
TACTGGTGCCAATAGTAGTCTTACAGGTTCTGGCGGACCC

DNA with coding
TTGCTTTGGGAGACCCAGCTGGGACTGGCTTTCCTTAGAG

sequence for signal
GCCTGAGTTATCACGACGGGGCGTTGGTCGTTACTAAAG

peptide
CCGGGTATTACTATATATACTCTAAGGTTCAGCTCGGCGG

TGTAGGATGCCCACTGGGTCTTGCGTCTACAATTACACAT

GGTCTGTATAAGAGGACTCCCAGATATCCAGAAGAACTG

GAATTGCTTGTTTCCCAGCAATCTCCGTGCGGACGCGCAA

CGAGCTCCAGTAGGGTGTGGTGGGACTCCAGCTTCCTGG

GTGGCGTTGTCCATTTGGAGGCGGGAGAGGAAGTAGTGG

TGCGGGTCCTTGATGAACGCCTTGTACGACTTCGGGACGG

TACAAGAAGCTACTTTGGGGCTTTCATGGTATCCAGCGCC

GGGGGCGGAAGCAGCGGCGGCAGCTTAAGCGGCAGAAG

CGACAACATCGGCAGCGATGCACATAAAAGTGAGGTGGC

CCACCGCTTTAAAGACCTCGGCGAGGAGAACTTCAAGGC

ACTCGTACTTATTGCCTTTGCACAATACCTGCAGCAATGT

CCGTTTGAAGATCATGTCAAGCTCGTAAATGAAGTGACA

GAGTTCGCTAAGACCTGTGTAGCTGACGAAAGTGCCGAA

AACTGCGACAAATCATTGCATACATTGTTCGGCGACAAG

CTTTGTACAGTTGCCACGCTCCGCGAGACATACGGCGAA

ATGGCCGATTGTTGTGCGAAACAGGAACCCGAAAGAAAT

GAGTGCTTCTTGCAACACAAAGACGATAATCCCAATCTTC

CGCGACTGGTGAGACCCGAAGTAGATGTAATGTGCACAG

CTTTTCATGACAATGAGGAAACCTTTCTTAAAAAATATCT

GTACGAAATCGCCCGCCGACACCCGTATTTCTATGCCCCA

GAGCTGTTGTTTTTCGCAAAGCGCTACAAGGCAGCGTTTA

CCGAATGCTGCCAGGCCGCTGATAAAGCCGCTTGTCTGCT

GCCTAAGCTTGATGAGCTTCGCGACGAGGGTAAGGCTTC

CAGCGCTAAACAACGCCTGAAGTGTGCATCTTTGCAAAA

ATTTGGTGAACGAGCCTTCAAGGCTTGGGCTGTTGCCAGG

CTGAGTCAACGGTTCCCGAAGGCGGAGTTTGCGGAGGTT

TCCAAGTTGGTAACGGACCTGACAAAGGTACATACCGAA

TGCTGCCATGGCGACCTGTTGGAGTGCGCCGATGATCGA

GCGGATCTTGCCAAGTATATTTGCGAAAACCAAGACTCC

ATTTCCAGTAAACTTAAGGAGTGTTGTGAGAAACCTCTCC

TTGAAAAGAGCCATTGTATAGCGGAGGTCGAAAACGATG

AAATGCCCGCTGATCTGCCGTCACTCGCTGCTGACTTCGT

TGAATCCAAGGATGTATGTAAAAACTATGCCGAAGCTAA

GGACGTCTTTCTTGGAATGTTCTTGTATGAATACGCCCGA

CGGCATCCTGACTATTCAGTTGTGCTCCTTCTTCGATTGG

CTAAAACTTATGAGACGACACTTGAAAAGTGTTGTGCCG

CCGCCGACCCACATGAGTGCTACGCTAAGGTTTTCGACG

AATTTAAGCCCTTGGTTGAAGAACCGCAGAATCTCATTAA

GCAAAATTGTGAGCTCTTTGAACAACTCGGTGAATACAA

ATTTCAGAACGCGCTTCTGGTTAGATATACGAAGAAAGT

GCCACAGGTGAGCACCCCTACATTGGTTGAGGTCAGTAG

GAACCTCGGCAAGGTGGGATCTAAGTGCTGCAAACACCC

GGAGGCAAAGAGAATGCCTTGCGCTGAGGATTATCTCTC

AGTGGTTCTGAATCAGCTTTGCGTTCTTCACGAAAAGACT

CCCGTCAGCGACCGAGTCACGAAGTGCTGTACCGAGAGC

CTTGTTAATAGACGACCTTGCTTCTCCGCGCTTGAGGTGG

ATGAGACCTACGTCCCAAAGGAATTCAACGCCGAGACGT

TCACTTTCCATGCCGATATTTGCACCTTGTCAGAAAAGGA

GCGACAGATAAAAAAGCAAACTGCTTTGGTGGAGCTGGT

TAAGCATAAGCCTAAAGCGACGAAGGAACAGCTCAAAGC

CGTAATGGATGATTTCGCTGCCTTCGTGGAGAAATGTTGT

AAGGCCGATGACAAGGAAACCTGCTTCGCTGAAGAGGGT

AAAAAGCTCGTCGCCGCTAGTCAGGCGGCACTTGGTTTG

AGTGGTGGAGAACAAAAACTCATTTCCGAGGAAGATCTTt

ga

100
ProC1496/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm16-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

LIGHT-1204DNI-
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

HSA-cMyc
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

Protein with signal
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

sequence
RLRDGTRSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHKS

EVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEV

TEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSGGEQKLISEEDL

101
ProC1496/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm16-
GGGACAGTCCGGATCTAGGCATCCATGTCGGCATGACCC

LIGHT-1204DNI-
ACATATCATATGCTACAAATTCGGTGGAGGATCTTCTGGA

HSA-cMyc
GGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGACA

DNA with coding
ATATTGGTGGCTCCCAGGAGAGGAGATCACATGAAGTCA

sequence for signal
ACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGTCTTAC

peptide
AGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGCTGGG

ACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGGGGCG

TTGGTCGTTACTAAAGCCGGGTATTACTATATATACTCTA

AGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTCTTGC

GTCTACAATTACACATGGTCTGTATAAGAGGACTCCCAG

ATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCAATCT

CCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTGGTGG

GACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAGGCGG

GAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGCCTTG

TACGACTTCGGGACGGTACAAGAAGCTACTTTGGGGCTTT

CATGGTATCCAGCGCCGGGGGCGGAAGCAGCGGCGGCA

GCTTAAGCGGCAGAAGCGACAACATCGGCAGCGATGCAC

ATAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTCGGCG

AGGAGAACTTCAAGGCACTCGTACTTATTGCCTTTGCACA

ATACCTGCAGCAATGTCCGTTTGAAGATCATGTCAAGCTC

GTAAATGAAGTGACAGAGTTCGCTAAGACCTGTGTAGCT

GACGAAAGTGCCGAAAACTGCGACAAATCATTGCATACA

TTGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTCCGCG

AGACATACGGCGAAATGGCCGATTGTTGTGCGAAACAGG

AACCCGAAAGAAATGAGTGCTTCTTGCAACACAAAGACG

ATAATCCCAATCTTCCGCGACTGGTGAGACCCGAAGTAG

ATGTAATGTGCACAGCTTTTCATGACAATGAGGAAACCTT

TCTTAAAAAATATCTGTACGAAATCGCCCGCCGACACCC

GTATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGCGC

TACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGCTGAT

AAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCGCG

ACGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAAGT

GTGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAGGC

TTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAGGC

GGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTGAC

AAAGGTACATACCGAATGCTGtCATGGCGACCTGTTGGAG

TGCGCCGATGATCGAGCGGATCTTGCCAAGTATATTTGCG

AAAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTGTT

GTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCGG

AGGTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCAC

TCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAAA

CTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTTG

TATGAATACGCCCGACGGCATCCTGACTATTCAGTTGTGC

TCCTTCTTCGATTGGCTAAAACTTATGAGACGACACTTGA

AAAGTGTTGTGCCGCCGCCGACCCACATGAGTGCTACGC

TAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACCG

CAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACAAC

TCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGATA

TACGAAGAAAGTGCCACAGGTGAGCACCCCTACATTGGT

TGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAGTG

CTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCTGA

GGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTCTTC

ACGAAAAGACTCCCGTCAGCGACCGAGTCACGAAGTGCT

GTACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTCCGC

GCTTGAGGTGGATGAGACCTACGTCCCAAAGGAATTCAA

CGCCGAGACGTTCACTTTCCATGCCGATATTTGCACCTTG

TCAGAAAAGGAGCGACAGATAAAAAAGCAAACTGCTTTG

GTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAGGAA

CAGCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCGTGG

AGAAATGTTGTAAGGCCGATGACAAGGAAACCTGCTTCG

CTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGGCGG

CACTTGGTTTGAGTGGTGGAGAACAAAAACTCATTTCCG

AGGAAGATCTTtga

102
ProC1184/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_LIGHT_
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYS

21linker_HSA-cMyc
KVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPC

Protein with signal
GRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRL

sequence
RDGTRSYFGAFMVSSAGGGSSGGSSAGGGSSGGSDAHKSE

VAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVT

EFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSGGEQKLISEEDL

103
ProC1184/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_LIGHT_
GGAGAGGCGCTCTCATGAAGTAAACCCCGCCGCGCACCT

21linker_HSA-cMyc
TACCGGTGCGAATTCCAGCCTTACGGGCTCCGGGGGCCC

DNA with coding
TCTTCTGTGGGAAACCCAACTCGGGCTGGCGTTTCTCAGG

sequence for signal
GGTCTCAGTTACCACGACGGCGCGCTTGTCGTTACTAAAG

peptide
CGGGCTACTACTATATCTACTCCAAGGTACAGCTCGGTGG

TGTAGGATGTCCGCTTGGGCTTGCCTCTACCATCACGCAC

GGTCTCTATAAAAGAACCCCAAGATACCCCGAAGAGTTG

GAACTGCTTGTTTCTCAACAGTCCCCTTGTGGTCGGGCAA

CCAGTTCATCTCGGGTGTGGTGGGATAGTAGCTTTCTCGG

AGGAGTAGTCCACCTGGAAGCTGGGGAAGAGGTAGTCGT

CCGGGTACTCGATGAACGGCTCGTGCGCCTCCGAGATGG

GACCCGGTCTTACTTTGGGGCTTTCATGGTTAGCTCTGCG

GGGGGAGGAAGCTCCGGGGGTAGTTCCGCCGGCGGCGGA

TCTAGTGGCGGTTCTGATGCTCATAAAAGTGAGGTCGCGC

ACAGATTCAAAGACCTCGGCGAGGAAAACTTTAAAGCCC

TCGTATTGATAGCTTTCGCCCAGTACCTCCAGCAGTGCCC

ATTCGAGGATCACGTGAAACTCGTGAATGAAGTAACGGA

ATTTGCCAAAACGTGCGTGGCCGACGAGAGTGCCGAAAA

TTGCGACAAGTCACTTCACACCCTTTTTGGTGACAAATTG

TGTACTGTGGCGACGCTTAGGGAAACATACGGAGAAATG

GCCGATTGCTGTGCCAAACAAGAGCCTGAAAGAAACGAA

TGCTTTCTTCAGCACAAAGACGATAACCCTAACTTGCCGA

GACTGGTGAGACCTGAAGTAGACGTCATGTGTACCGCGT

TCCATGACAACGAAGAGACTTTCTTGAAAAAATACCTTTA

TGAAATAGCACGGAGGCACCCTTATTTTTACGCTCCAGAG

CTCCTCTTCTTTGCTAAACGGTACAAAGCGGCGTTTACCG

AATGTTGCCAAGCTGCGGATAAAGCTGCATGTCTTCTCCC

GAAGTTGGATGAGCTGAGAGATGAGGGTAAAGCGTCTTC

CGCTAAACAACGACTTAAATGCGCTTCTCTGCAGAAATTT

GGCGAACGAGCGTTCAAAGCCTGGGCCGTTGCGCGCCTT

TCACAGCGGTTTCCGAAAGCCGAGTTCGCCGAGGTTTCA

AAGCTGGTTACGGACTTGACAAAGGTGCATACAGAATGC

TGCCACGGAGACCTGCTGGAGTGCGCCGATGATCGCGCT

GATTTGGCTAAATATATTTGCGAAAATCAGGACAGCATC

AGCTCCAAGTTGAAGGAGTGTTGTGAAAAACCGCTGCTG

GAGAAGTCACACTGCATAGCCGAGGTGGAAAACGACGA

GATGCCGGCAGACCTCCCCAGCCTTGCCGCGGATTTCGTC

GAATCAAAGGATGTATGCAAAAATTACGCGGAAGCAAAA

GATGTATTTCTGGGAATGTTCCTGTACGAGTACGCTAGGC

GACATCCCGACTACAGCGTTGTTCTGCTCTTGAGACTTGC

GAAGACGTACGAGACTACGCTCGAGAAGTGCTGTGCAGC

TGCGGACCCCCATGAGTGTTATGCTAAAGTCTTCGACGAA

TTTAAGCCTTTGGTGGAAGAGCCACAGAACCTGATCAAA

CAAAATTGTGAACTGTTCGAACAATTGGGGGAGTATAAA

TTTCAGAACGCTCTCCTTGTTCGGTATACAAAAAAAGTAC

CGCAGGTAAGTACGCCGACACTCGTGGAAGTAAGCAGGA

ACCTCGGAAAGGTTGGATCAAAATGCTGCAAGCATCCGG

AGGCTAAGCGCATGCCATGCGCTGAGGATTATCTTTCAGT

GGTCCTGAACCAATTGTGCGTGTTGCACGAGAAAACTCC

AGTAAGCGATAGAGTTACCAAATGTTGTACAGAGAGCCT

GGTTAATCGACGACCTTGCTTCAGCGCCTTGGAAGTCGAT

GAGACGTATGTGCCGAAGGAATTTAACGCCGAAACTTTC

ACTTTTCATGCAGATATCTGTACATTGAGCGAAAAGGAA

AGGCAAATTAAAAAACAAACTGCGCTTGTGGAATTGGTC

AAGCACAAGCCTAAAGCCACAAAGGAACAGCTCAAAGC

GGTAATGGACGATTTTGCGGCGTTCGTAGAGAAGTGTTG

CAAGGCGGACGATAAAGAAACGTGCTTTGCTGAGGAGGG

AAAAAAGCTTGTTGCTGCCAGTCAAGCGGCGCTTGGCTT

GAGTGGTGGAGAACAAAAACTCATTTCCGAGGAAGATCT

TTGA

104
ProC1486/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_mhLIGHT_
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKTGYYYIYS

1204DNI HSA-cMyc
KVQLGGVGCPLGLAGTITHGLYKRTPRYPEELELLVSQQSP

Protein with signal
CGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLGKRLVR

sequence
LRDGTRSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHKSE

VAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVT

EFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSGGEQKLISEEDL

105
ProC1486/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mhLIGHT_
AGAACGCCGATCACACGAAGTGAACCCTGCTGCTCACTT

1204DNI HSA-cMyc
GACTGGAGCTAACTCCAGCCTTACGGGGAGCGGGGGTCC

DNA with coding
TTTGCTCTGGGAAACGCAGCTGGGTCTCGCGTTTCTTAGA

sequence for signal
GGGCTGAGTTATCACGATGGCGCCTTGGTCGTCACGAAG

peptide
ACTGGGTACTACTATATTTATAGTAAGGTACAGTTGGGGG

GAGTGGGGTGCCCTCTCGGCCTGGCTGGGACGATCACGC

ATGGGCTCTACAAGCGCACGCCTAGGTATCCGGAGGAGT

TGGAACTGTTGGTCTCACAGCAGTCCCCGTGCGGGCGAG

CGACTTCCTCCAGTAGAGTGTGGTGGGACTCTAGCTTTCT

CGGGGGAGTGGTTCATCTTGAGGCAGGAGAGGAAGTGGT

GGTACGGGTTTTGGGCAAGAGATTGGTGAGACTGCGGGA

TGGTACAAGATCTTATTTTGGTGCTTTCATGGTCTCCAGC

GCCGGGGGCGGAAGCAGCGGCGGCAGCTTAAGCGGCAG

AAGCGACAACATCGGCAGCGATGCTCATAAAAGTGAGGT

CGCGCACAGATTCAAAGACCTCGGCGAGGAAAACTTTAA

AGCCCTCGTATTGATAGCTTTCGCCCAGTACCTCCAGCAG

TGCCCATTCGAGGATCACGTGAAACTCGTGAATGAAGTA

ACGGAATTTGCCAAAACGTGCGTGGCCGACGAGAGTGCC

GAAAATTGCGACAAGTCACTTCACACCCTTTTTGGTGACA

AATTGTGTACTGTGGCGACGCTTAGGGAAACATACGGAG

AAATGGCCGATTGCTGTGCCAAACAAGAGCCTGAAAGAA

ACGAATGCTTTCTTCAGCACAAAGACGATAACCCTAACTT

GCCGAGACTGGTGAGACCTGAAGTAGACGTCATGTGTAC

CGCGTTCCATGACAACGAAGAGACTTTCTTGAAAAAATA

CCTTTATGAAATAGCACGGAGGCACCCTTATTTTTACGCT

CCAGAGCTCCTCTTCTTTGCTAAACGGTACAAAGCGGCGT

TTACCGAATGTTGCCAAGCTGCGGATAAAGCTGCATGTCT

TCTCCCGAAGTTGGATGAGCTGAGAGATGAGGGTAAAGC

GTCTTCCGCTAAACAACGACTTAAATGCGCTTCTCTGCAG

AAATTTGGCGAACGAGCGTTCAAAGCCTGGGCCGTTGCG

CGCCTTTCACAGCGGTTTCCGAAAGCCGAGTTCGCCGAG

GTTTCAAAGCTGGTTACGGACTTGACAAAGGTGCATACA

GAATGCTGCCACGGAGACCTGCTGGAGTGCGCCGATGAT

CGCGCTGATTTGGCTAAATATATTTGCGAAAATCAGGAC

AGCATCAGCTCCAAGTTGAAGGAGTGTTGTGAAAAACCG

CTGCTGGAGAAGTCACACTGCATAGCCGAGGTGGAAAAC

GACGAGATGCCGGCAGACCTCCCCAGCCTTGCCGCGGAT

TTCGTCGAATCAAAGGATGTATGCAAAAATTACGCGGAA

GCAAAAGATGTATTTCTGGGAATGTTCCTGTACGAGTACG

CTAGGCGACATCCCGACTACAGCGTTGTTCTGCTCTTGAG

ACTTGCGAAGACGTACGAGACTACGCTCGAGAAGTGCTG

TGCAGCTGCGGACCCCCATGAGTGTTATGCTAAAGTCTTC

GACGAATTTAAGCCTTTGGTGGAAGAGCCACAGAACCTG

ATCAAACAAAATTGTGAACTGTTCGAACAATTGGGGGAG

TATAAATTTCAGAACGCTCTCCTTGTTCGGTATACAAAAA

AAGTACCGCAGGTAAGTACGCCGACACTCGTGGAAGTAA

GCAGGAACCTCGGAAAGGTTGGATCAAAATGCTGCAAGC

ATCCGGAGGCTAAGCGCATGCCATGCGCTGAGGATTATC

TTTCAGTGGTCCTGAACCAATTGTGCGTGTTGCACGAGAA

AACTCCAGTAAGCGATAGAGTTACCAAATGTTGTACAGA

GAGCCTGGTTAATCGACGACCTTGCTTCAGCGCCTTGGAA

GTCGATGAGACGTATGTGCCGAAGGAATTTAACGCCGAA

ACTTTCACTTTTCATGCAGATATCTGTACATTGAGCGAAA

AGGAAAGGCAAATTAAAAAACAAACTGCGCTTGTGGAAT

TGGTCAAGCACAAGCCTAAAGCCACAAAGGAACAGCTCA

AAGCGGTAATGGACGATTTTGCGGCGTTCGTAGAGAAGT

GTTGCAAGGCGGACGATAAAGAAACGTGCTTTGCTGAGG

AGGGAAAAAAGCTTGTTGCTGCCAGTCAAGCGGCGCTTG

GCTTGAGTGGTGGAGAACAAAAACTCATTTCCGAGGAAG

ATCTTTGA

106
ProC1483/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_mhLIGHT_
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKTGYYYIYS

21linker_HSA-cMyc
KVQLGGVGCPLGLAGTITHGLYKRTPRYPEELELLVSQQSP

Protein with signal
CGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLGKRLVR

sequence
LRDGTRSYFGAFMVSSAGGGSSGGSSAGGGSSGGSDAHKSE

VAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVT

EFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSGGEQKLISEEDL

107
ProC1483/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mhLIGHT_
AGAACGCCGATCACACGAAGTGAACCCTGCTGCTCACTT

21linker_HSA-cMyc
GACTGGAGCTAACTCCAGCCTTACGGGGAGCGGGGGTCC

DNA with coding
TTTGCTCTGGGAAACGCAGCTGGGTCTCGCGTTTCTTAGA

sequence for signal
GGGCTGAGTTATCACGATGGCGCCTTGGTCGTCACGAAG

peptide
ACTGGGTACTACTATATTTATAGTAAGGTACAGTTGGGGG

GAGTGGGGTGCCCTCTCGGCCTGGCTGGGACGATCACGC

ATGGGCTCTACAAGCGCACGCCTAGGTATCCGGAGGAGT

TGGAACTGTTGGTCTCACAGCAGTCCCCGTGCGGGCGAG

CGACTTCCTCCAGTAGAGTGTGGTGGGACTCTAGCTTTCT

CGGGGGAGTGGTTCATCTTGAGGCAGGAGAGGAAGTGGT

GGTACGGGTTTTGGGCAAGAGATTGGTGAGACTGCGGGA

TGGTACAAGATCTTATTTTGGTGCTTTCATGGTCAGCTCT

GCGGGGGGAGGAAGCTCCGGGGGTAGTTCCGCCGGCGGC

GGATCTAGTGGCGGTTCTGATGCTCATAAAAGTGAGGTC

GCGCACAGATTCAAAGACCTCGGCGAGGAAAACTTTAAA

GCCCTCGTATTGATAGCTTTCGCCCAGTACCTCCAGCAGT

GCCCATTCGAGGATCACGTGAAACTCGTGAATGAAGTAA

CGGAATTTGCCAAAACGTGCGTGGCCGACGAGAGTGCCG

AAAATTGCGACAAGTCACTTCACACCCTTTTTGGTGACAA

ATTGTGTACTGTGGCGACGCTTAGGGAAACATACGGAGA

AATGGCCGATTGCTGTGCCAAACAAGAGCCTGAAAGAAA

CGAATGCTTTCTTCAGCACAAAGACGATAACCCTAACTTG

CCGAGACTGGTGAGACCTGAAGTAGACGTCATGTGTACC

GCGTTCCATGACAACGAAGAGACTTTCTTGAAAAAATAC

CTTTATGAAATAGCACGGAGGCACCCTTATTTTTACGCTC

CAGAGCTCCTCTTCTTTGCTAAACGGTACAAAGCGGCGTT

TACCGAATGTTGCCAAGCTGCGGATAAAGCTGCATGTCTT

CTCCCGAAGTTGGATGAGCTGAGAGATGAGGGTAAAGCG

TCTTCCGCTAAACAACGACTTAAATGCGCTTCTCTGCAGA

AATTTGGCGAACGAGCGTTCAAAGCCTGGGCCGTTGCGC

GCCTTTCACAGCGGTTTCCGAAAGCCGAGTTCGCCGAGGT

TTCAAAGCTGGTTACGGACTTGACAAAGGTGCATACAGA

ATGCTGCCACGGAGACCTGCTGGAGTGCGCCGATGATCG

CGCTGATTTGGCTAAATATATTTGCGAAAATCAGGACAG

CATCAGCTCCAAGTTGAAGGAGTGTTGTGAAAAACCGCT

GCTGGAGAAGTCACACTGCATAGCCGAGGTGGAAAACGA

CGAGATGCCGGCAGACCTCCCCAGCCTTGCCGCGGATTT

CGTCGAATCAAAGGATGTATGCAAAAATTACGCGGAAGC

AAAAGATGTATTTCTGGGAATGTTCCTGTACGAGTACGCT

AGGCGACATCCCGACTACAGCGTTGTTCTGCTCTTGAGAC

TTGCGAAGACGTACGAGACTACGCTCGAGAAGTGCTGTG

CAGCTGCGGACCCCCATGAGTGTTATGCTAAAGTCTTCGA

CGAATTTAAGCCTTTGGTGGAAGAGCCACAGAACCTGAT

CAAACAAAATTGTGAACTGTTCGAACAATTGGGGGAGTA

TAAATTTCAGAACGCTCTCCTTGTTCGGTATACAAAAAAA

GTACCGCAGGTAAGTACGCCGACACTCGTGGAAGTAAGC

AGGAACCTCGGAAAGGTTGGATCAAAATGCTGCAAGCAT

CCGGAGGCTAAGCGCATGCCATGCGCTGAGGATTATCTTT

CAGTGGTCCTGAACCAATTGTGCGTGTTGCACGAGAAAA

CTCCAGTAAGCGATAGAGTTACCAAATGTTGTACAGAGA

GCCTGGTTAATCGACGACCTTGCTTCAGCGCCTTGGAAGT

CGATGAGACGTATGTGCCGAAGGAATTTAACGCCGAAAC

TTTCACTTTTCATGCAGATATCTGTACATTGAGCGAAAAG

GAAAGGCAAATTAAAAAACAAACTGCGCTTGTGGAATTG

GTCAAGCACAAGCCTAAAGCCACAAAGGAACAGCTCAA

AGCGGTAATGGACGATTTTGCGGCGTTCGTAGAGAAGTG

TTGCAAGGCGGACGATAAAGAAACGTGCTTTGCTGAGGA

GGGAAAAAAGCTTGTTGCTGCCAGTCAAGCGGCGCTTGG

CTTGAGTGGTGGAGAACAAAAACTCATTTCCGAGGAAGA

TCTTTGA

108
ProC1485/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

16_mhLIGHT_
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKTGYYYI

21linker_HSA-cMyc
YSKVQLGGVGCPLGLAGTITHGLYKRTPRYPEELELLVSQQ

Protein with signal
SPCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLGKRL

sequence
VRLRDGTRSYFGAFMVSSAGGGSSGGSSAGGGSSGGSDAH

KSEVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVN

EVTEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYG

EMADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCT

AFHDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFT

ECCQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKF

GERAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECC

HGDLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSH

CIAEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLG

MFLYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHE

CYAKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLV

RYTKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCA

EDYLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSA

LEVDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVEL

VKHKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEE

GKKLVAASQAALGLSGGEQKLISEEDL

109
ProC1485/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm-
GGGACAGTCCGGATCTAGGCATCCATGTCGGCATGACCC

16_mhLIGHT_
ACATATCATATGCTACAAATTCGGTGGAGGATCTTCTGGA

21linker_HSA-cMyc
GGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGACA

DNA with coding
ATATTGGTGGCTCCCAAGAACGCCGATCACACGAAGTGA

sequence for signal
ACCCTGCTGCTCACTTGACTGGAGCTAACTCCAGCCTTAC

peptide
GGGGAGCGGGGGTCCTTTGCTCTGGGAAACGCAGCTGGG

TCTCGCGTTTCTTAGAGGGCTGAGTTATCACGATGGCGCC

TTGGTCGTCACGAAGACTGGGTACTACTATATTTATAGTA

AGGTACAGTTGGGGGGAGTGGGGTGCCCTCTCGGCCTGG

CTGGGACGATCACGCATGGGCTCTACAAGCGCACGCCTA

GGTATCCGGAGGAGTTGGAACTGTTGGTCTCACAGCAGT

CCCCGTGCGGGCGAGCGACTTCCTCCAGTAGAGTGTGGT

GGGACTCTAGCTTTCTCGGGGGAGTGGTTCATCTTGAGGC

AGGAGAGGAAGTGGTGGTACGGGTTTTGGGCAAGAGATT

GGTGAGACTGCGGGATGGTACAAGATCTTATTTTGGTGCT

TTCATGGTCAGCTCTGCGGGGGGAGGAAGCTCCGGGGGT

AGTTCCGCCGGCGGCGGATCTAGTGGCGGTTCTGATGCTC

ATAAAAGTGAGGTCGCGCACAGATTCAAAGACCTCGGCG

AGGAAAACTTTAAAGCCCTCGTATTGATAGCTTTCGCCCA

GTACCTCCAGCAGTGCCCATTCGAGGATCACGTGAAACT

CGTGAATGAAGTAACGGAATTTGCCAAAACGTGCGTGGC

CGACGAGAGTGCCGAAAATTGCGACAAGTCACTTCACAC

CCTTTTTGGTGACAAATTGTGTACTGTGGCGACGCTTAGG

GAAACATACGGAGAAATGGCCGATTGCTGTGCCAAACAA

GAGCCTGAAAGAAACGAATGCTTTCTTCAGCACAAAGAC

GATAACCCTAACTTGCCGAGACTGGTGAGACCTGAAGTA

GACGTCATGTGTACCGCGTTCCATGACAACGAAGAGACT

TTCTTGAAAAAATACCTTTATGAAATAGCACGGAGGCAC

CCTTATTTTTACGCTCCAGAGCTCCTCTTCTTTGCTAAACG

GTACAAAGCGGCGTTTACCGAATGTTGCCAAGCTGCGGA

TAAAGCTGCATGTCTTCTCCCGAAGTTGGATGAGCTGAGA

GATGAGGGTAAAGCGTCTTCCGCTAAACAACGACTTAAA

TGCGCTTCTCTGCAGAAATTTGGCGAACGAGCGTTCAAA

GCCTGGGCCGTTGCGCGCCTTTCACAGCGGTTTCCGAAAG

CCGAGTTCGCCGAGGTTTCAAAGCTGGTTACGGACTTGAC

AAAGGTGCATACAGAATGCTGCCACGGAGACCTGCTGGA

GTGCGCCGATGATCGCGCTGATTTGGCTAAATATATTTGC

GAAAATCAGGACAGCATCAGCTCCAAGTTGAAGGAGTGT

TGTGAAAAACCGCTGCTGGAGAAGTCACACTGCATAGCC

GAGGTGGAAAACGACGAGATGCCGGCAGACCTCCCCAGC

CTTGCCGCGGATTTCGTCGAATCAAAGGATGTATGCAAA

AATTACGCGGAAGCAAAAGATGTATTTCTGGGAATGTTC

CTGTACGAGTACGCTAGGCGACATCCCGACTACAGCGTT

GTTCTGCTCTTGAGACTTGCGAAGACGTACGAGACTACGC

TCGAGAAGTGCTGTGCAGCTGCGGACCCCCATGAGTGTT

ATGCTAAAGTCTTCGACGAATTTAAGCCTTTGGTGGAAGA

GCCACAGAACCTGATCAAACAAAATTGTGAACTGTTCGA

ACAATTGGGGGAGTATAAATTTCAGAACGCTCTCCTTGTT

CGGTATACAAAAAAAGTACCGCAGGTAAGTACGCCGACA

CTCGTGGAAGTAAGCAGGAACCTCGGAAAGGTTGGATCA

AAATGCTGCAAGCATCCGGAGGCTAAGCGCATGCCATGC

GCTGAGGATTATCTTTCAGTGGTCCTGAACCAATTGTGCG

TGTTGCACGAGAAAACTCCAGTAAGCGATAGAGTTACCA

AATGTTGTACAGAGAGCCTGGTTAATCGACGACCTTGCTT

CAGCGCCTTGGAAGTCGATGAGACGTATGTGCCGAAGGA

ATTTAACGCCGAAACTTTCACTTTTCATGCAGATATCTGT

ACATTGAGCGAAAAGGAAAGGCAAATTAAAAAACAAAC

TGCGCTTGTGGAATTGGTCAAGCACAAGCCTAAAGCCAC

AAAGGAACAGCTCAAAGCGGTAATGGACGATTTTGCGGC

GTTCGTAGAGAAGTGTTGCAAGGCGGACGATAAAGAAAC

GTGCTTTGCTGAGGAGGGAAAAAAGCTTGTTGCTGCCAG

TCAAGCGGCGCTTGGCTTGAGTGGTGGAGAACAAAAACT

CATTTCCGAGGAAGATCTTTGA

110
ProC1487/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

16_mhLIGHT_
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKTGYYYI

1204DNI_HSA-cMyc
YSKVQLGGVGCPLGLAGTITHGLYKRTPRYPEELELLVSQQ

Protein with signal
SPCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLGKRL

sequence
VRLRDGTRSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHK

SEVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNE

VTEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGE

MADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTA

FHDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSGGEQKLISEEDL

111
ProC1487/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm-
GGGACAGTCCGGATCTAGGCATCCATGTCGGCATGACCC

16_mhLIGHT_
ACATATCATATGCTACAAATTCGGTGGAGGATCTTCTGGA

1204DNI_HSA-cMyc
GGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGACA

DNA with coding
ATATTGGTGGCTCCCAAGAACGCCGATCACACGAAGTGA

sequence for signal
ACCCTGCTGCTCACTTGACTGGAGCTAACTCCAGCCTTAC

peptide
GGGGAGCGGGGGTCCTTTGCTCTGGGAAACGCAGCTGGG

TCTCGCGTTTCTTAGAGGGCTGAGTTATCACGATGGCGCC

TTGGTCGTCACGAAGACTGGGTACTACTATATTTATAGTA

AGGTACAGTTGGGGGGAGTGGGGTGCCCTCTCGGCCTGG

CTGGGACGATCACGCATGGGCTCTACAAGCGCACGCCTA

GGTATCCGGAGGAGTTGGAACTGTTGGTCTCACAGCAGT

CCCCGTGCGGGCGAGCGACTTCCTCCAGTAGAGTGTGGT

GGGACTCTAGCTTTCTCGGGGGAGTGGTTCATCTTGAGGC

AGGAGAGGAAGTGGTGGTACGGGTTTTGGGCAAGAGATT

GGTGAGACTGCGGGATGGTACAAGATCTTATTTTGGTGCT

TTCATGGTCTCCAGCGCCGGGGGCGGAAGCAGCGGCGGC

AGCTTAAGCGGCAGAAGCGACAACATCGGCAGCGATGCT

CATAAAAGTGAGGTCGCGCACAGATTCAAAGACCTCGGC

GAGGAAAACTTTAAAGCCCTCGTATTGATAGCTTTCGCCC

AGTACCTCCAGCAGTGCCCATTCGAGGATCACGTGAAAC

TCGTGAATGAAGTAACGGAATTTGCCAAAACGTGCGTGG

CCGACGAGAGTGCCGAAAATTGCGACAAGTCACTTCACA

CCCTTTTTGGTGACAAATTGTGTACTGTGGCGACGCTTAG

GGAAACATACGGAGAAATGGCCGATTGCTGTGCCAAACA

AGAGCCTGAAAGAAACGAATGCTTTCTTCAGCACAAAGA

CGATAACCCTAACTTGCCGAGACTGGTGAGACCTGAAGT

AGACGTCATGTGTACCGCGTTCCATGACAACGAAGAGAC

TTTCTTGAAAAAATACCTTTATGAAATAGCACGGAGGCA

CCCTTATTTTTACGCTCCAGAGCTCCTCTTCTTTGCTAAAC

GGTACAAAGCGGCGTTTACCGAATGTTGCCAAGCTGCGG

ATAAAGCTGCATGTCTTCTCCCGAAGTTGGATGAGCTGAG

AGATGAGGGTAAAGCGTCTTCCGCTAAACAACGACTTAA

ATGCGCTTCTCTGCAGAAATTTGGCGAACGAGCGTTCAA

AGCCTGGGCCGTTGCGCGCCTTTCACAGCGGTTTCCGAAA

GCCGAGTTCGCCGAGGTTTCAAAGCTGGTTACGGACTTG

ACAAAGGTGCATACAGAATGCTGCCACGGAGACCTGCTG

GAGTGCGCCGATGATCGCGCTGATTTGGCTAAATATATTT

GCGAAAATCAGGACAGCATCAGCTCCAAGTTGAAGGAGT

GTTGTGAAAAACCGCTGCTGGAGAAGTCACACTGCATAG

CCGAGGTGGAAAACGACGAGATGCCGGCAGACCTCCCCA

GCCTTGCCGCGGATTTCGTCGAATCAAAGGATGTATGCA

AAAATTACGCGGAAGCAAAAGATGTATTTCTGGGAATGT

TCCTGTACGAGTACGCTAGGCGACATCCCGACTACAGCG

TTGTTCTGCTCTTGAGACTTGCGAAGACGTACGAGACTAC

GCTCGAGAAGTGCTGTGCAGCTGCGGACCCCCATGAGTG

TTATGCTAAAGTCTTCGACGAATTTAAGCCTTTGGTGGAA

GAGCCACAGAACCTGATCAAACAAAATTGTGAACTGTTC

GAACAATTGGGGGAGTATAAATTTCAGAACGCTCTCCTT

GTTCGGTATACAAAAAAAGTACCGCAGGTAAGTACGCCG

ACACTCGTGGAAGTAAGCAGGAACCTCGGAAAGGTTGGA

TCAAAATGCTGCAAGCATCCGGAGGCTAAGCGCATGCCA

TGCGCTGAGGATTATCTTTCAGTGGTCCTGAACCAATTGT

GCGTGTTGCACGAGAAAACTCCAGTAAGCGATAGAGTTA

CCAAATGTTGTACAGAGAGCCTGGTTAATCGACGACCTT

GCTTCAGCGCCTTGGAAGTCGATGAGACGTATGTGCCGA

AGGAATTTAACGCCGAAACTTTCACTTTTCATGCAGATAT

CTGTACATTGAGCGAAAAGGAAAGGCAAATTAAAAAACA

AACTGCGCTTGTGGAATTGGTCAAGCACAAGCCTAAAGC

CACAAAGGAACAGCTCAAAGCGGTAATGGACGATTTTGC

GGCGTTCGTAGAGAAGTGTTGCAAGGCGGACGATAAAGA

AACGTGCTTTGCTGAGGAGGGAAAAAAGCTTGTTGCTGC

CAGTCAAGCGGCGCTTGGCTTGAGTGGTGGAGAACAAAA

ACTCATTTCCGAGGAAGATCTTTGA

112
ProC1493/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_LIGHT-3HB-
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYS

1204DNI-HSA-His
KVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPC

Protein with signal
GRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRL

sequence
RDGTRSYFGAFMVSSAGGGSGGGSGGSGEIAALKQEIAALK

KEIAALKWEIAALKQGYYGGSGGSLSGRSDNIGSDAHKSEV

AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLSHHHHHH

113
ProC1493/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_LIGHT-3HB-
AGAGCGAAGATCCCATGAAGTAAACCCTGCAGCTCACCT

1204DNI-HSA-His
TACAGGAGCCAACAGCAGTCTGACAGGTTCTGGGGGCCC

DNA with coding
CTTGTTGTGGGAGACGCAACTGGGGCTTGCATTCCTCCGA

sequence for signal
GGGCTCAGTTACCACGACGGCGCGCTTGTTGTTACAAAA

peptide
GCAGGATACTACTATATTTACTCAAAGGTGCAGCTGGGT

GGAGTGGGATGTCCATTGGGCCTGGCCTCAACTATAACC

CATGGCCTCTATAAAAGAACGCCCCGGTATCCTGAGGAG

CTGGAGCTGTTGGTCTCACAGCAGTCACCGTGCGGCAGA

GCCACATCATCCTCTCGCGTATGGTGGGACTCTTCCTTCC

TGGGAGGTGTAGTCCATCTCGAGGCAGGTGAAGAAGTCG

TAGTTCGCGTACTCGATGAACGCCTGGTTCGGCTGAGGG

ATGGGACTAGGAGCTATTTCGGCGCATTTATGGTATCTTC

TGCAGGTGGAGGAAGTGGTGGCGGTTCCGGTGGTTCAGG

GGAAATCGCGGCACTCAAACAAGAGATAGCGGCTTTGAA

AAAGGAGATCGCAGCCCTGAAATGGGAAATAGCGGCCTT

GAAGCAGGGCTACTATGGCGGCAGCGGCGGCAGCCTAAG

CGGACGGTCCGACAATATCGGCAGCGATGCACATAAAAG

TGAGGTGGCCCACCGCTTTAAAGACCTCGGCGAGGAGAA

CTTCAAGGCACTCGTACTTATTGCCTTTGCACAATACCTG

CAGCAATGTCCGTTTGAAGATCATGTCAAGCTCGTAAATG

AAGTGACAGAGTTCGCTAAGACCTGTGTAGCTGACGAAA

GTGCCGAAAACTGCGACAAATCATTGCATACATTGTTCG

GCGACAAGCTTTGTACAGTTGCCACGCTCCGCGAGACAT

ACGGCGAAATGGCCGATTGTTGTGCGAAACAGGAACCCG

AAAGAAATGAGTGCTTCTTGCAACACAAAGACGATAATC

CCAATCTTCCGCGACTGGTGAGACCCGAAGTAGATGTAA

TGTGCACAGCTTTTCATGACAATGAGGAAACCTTTCTTAA

AAAATATCTGTACGAAATCGCCCGCCGACACCCGTATTTC

TATGCCCCAGAGCTGTTGTTTTTCGCAAAGCGCTACAAGG

CAGCGTTTACCGAATGCTGCCAGGCCGCTGATAAAGCCG

CTTGTCTGCTGCCTAAGCTTGATGAGCTTCGCGACGAGGG

TAAGGCTTCCAGCGCTAAACAACGCCTGAAGTGTGCATC

TTTGCAAAAATTTGGTGAACGAGCCTTCAAGGCTTGGGCT

GTTGCCAGGCTGAGTCAACGGTTCCCGAAGGCGGAGTTT

GCGGAGGTTTCCAAGTTGGTAACGGACCTGACAAAGGTA

CATACCGAATGCTGCCATGGCGACCTGTTGGAGTGCGCC

GATGATCGAGCGGATCTTGCCAAGTATATTTGCGAAAAC

CAAGACTCCATTTCCAGTAAACTTAAGGAGTGTTGTGAG

AAACCTCTCCTTGAAAAGAGCCATTGTATAGCGGAGGTC

GAAAACGATGAAATGCCCGCTGATCTGCCGTCACTCGCT

GCTGACTTCGTTGAATCCAAGGATGTATGTAAAAACTATG

CCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTTGTATGA

ATACGCCCGACGGCATCCTGACTATTCAGTTGTGCTCCTT

CTTCGATTGGCTAAAACTTATGAGACGACACTTGAAAAG

TGTTGTGCCGCCGCCGACCCACATGAGTGCTACGCTAAG

GTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACCGCAGA

ATCTCATTAAGCAAAATTGTGAGCTCTTTGAACAACTCGG

TGAATACAAATTTCAGAACGCGCTTCTGGTTAGATATACG

AAGAAAGTGCCACAGGTGAGCACCCCTACATTGGTTGAG

GTCAGTAGGAACCTCGGCAAGGTGGGATCTAAGTGCTGC

AAACACCCGGAGGCAAAGAGAATGCCTTGCGCTGAGGAT

TATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTCTTCACG

AAAAGACTCCCGTCAGCGACCGAGTCACGAAGTGCTGTA

CCGAGAGCCTTGTTAATAGACGACCTTGCTTCTCCGCGCT

TGAGGTGGATGAGACCTACGTCCCAAAGGAATTCAACGC

CGAGACGTTCACTTTCCATGCCGATATTTGCACCTTGTCA

GAAAAGGAGCGACAGATAAAAAAGCAAACTGCTTTGGTG

GAGCTGGTTAAGCATAAGCCTAAAGCGACGAAGGAACAG

CTCAAAGCCGTAATGGATGATTTCGCTGCCTTCGTGGAGA

AATGTTGTAAGGCCGATGACAAGGAAACCTGCTTCGCTG

AAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGGCGGCAC

TTGGTTTGAGCCACCACCACCATCACCACtga

114
ProC1490/
METDTLLLWVLLLWVPGSTGEIAALKQEIAALKKEIAALKW

ProC_3HB-LIGHT-
EIAALKQGYYGGSGGSQERRSHEVNPAAHLTGANSSLTGSG

1204DNI-HSA-cMyc
GPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYSKVQL

Protein with signal
GGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPCGRAT

sequence
SSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRLRDGT

RSYFGAFMVSSAGGGSSGGSLSGRSDNIGSDAHKSEVAHRF

KDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTEFAKT

CVADESAENCDKSLHTLFGDKLCTVATLRETYGEMADCCA

KQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFHDNEE

TFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECCQAAD

KAACLLPKLDELRDEGKASSAKQRLKCASLQKFGERAFKA

WAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGDLLEC

ADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIAEVEN

DEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFLYEYA

RRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYAKVFD

EFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYTKKVP

QVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDYLSVV

LNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEVDETY

VPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKHKPKA

TKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKLVAAS

QAALGLSGGEQKLISEEDL

115
ProC1490/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcGA

ProC_3HB-LIGHT-
AATCGCGGCACTCAAACAAGAGATAGCGGCTTTGAAAAA

1204DNI-HSA-cMyc
GGAGATCGCAGCCCTGAAATGGGAAATAGCGGCCTTGAA

DNA with coding
GCAGGGCTACTATGGGGGATCCGGGGGTTCACAGGAGCG

sequence for signal
ACGGTCCCATGAGGTGAATCCGGCAGCGCATTTGACGGG

peptide
GGCCAACTCATCCCTGACAGGTTCAGGTGGCCCTCTGTTG

TGGGAAACTCAGCTCGGACTGGCCTTCCTTAGAGGTTTGT

CATATCATGACGGAGCACTTGTAGTCACCAAAGCTGGGT

ATTACTACATATACTCTAAGGTCCAGCTGGGTGGGGTGG

GCTGTCCACTTGGCTTGGCATCTACGATCACGCATGGGTT

GTACAAAAGAACTCCACGATATCCAGAAGAACTCGAATT

GCTTGTCTCCCAACAATCTCCTTGTGGCAGGGCTACGTCC

AGTTCCCGAGTGTGGTGGGATTCAAGTTTTCTCGGGGGCG

TAGTCCATCTTGAAGCAGGGGAGGAAGTGGTCGTCCGAG

TGCTGGACGAACGGTTGGTTAGGCTTCGGGATGGGACAA

GAAGTTATTTTGGGGCCTTCATGGTATCCAGCGCCGGGGG

CGGAAGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGACA

ACATCGGCAGCGATGCTCATAAAAGTGAGGTCGCGCACA

GATTCAAAGACCTCGGCGAGGAAAACTTTAAAGCCCTCG

TATTGATAGCTTTCGCCCAGTACCTCCAGCAGTGCCCATT

CGAGGATCACGTGAAACTCGTGAATGAAGTAACGGAATT

TGCCAAAACGTGCGTGGCCGACGAGAGTGCCGAAAATTG

CGACAAGTCACTTCACACCCTTTTTGGTGACAAATTGTGT

ACTGTGGCGACGCTTAGGGAAACATACGGAGAAATGGCC

GATTGCTGTGCCAAACAAGAGCCTGAAAGAAACGAATGC

TTTCTTCAGCACAAAGACGATAACCCTAACTTGCCGAGAC

TGGTGAGACCTGAAGTAGACGTCATGTGTACCGCGTTCC

ATGACAACGAAGAGACTTTCTTGAAAAAATACCTTTATG

AAATAGCACGGAGGCACCCTTATTTTTACGCTCCAGAGCT

CCTCTTCTTTGCTAAACGGTACAAAGCGGCGTTTACCGAA

TGTTGCCAAGCTGCGGATAAAGCTGCATGTCTTCTCCCGA

AGTTGGATGAGCTGAGAGATGAGGGTAAAGCGTCTTCCG

CTAAACAACGACTTAAATGCGCTTCTCTGCAGAAATTTGG

CGAACGAGCGTTCAAAGCCTGGGCCGTTGCGCGCCTTTC

ACAGCGGTTTCCGAAAGCCGAGTTCGCCGAGGTTTCAAA

GCTGGTTACGGACTTGACAAAGGTGCATACAGAATGCTG

CCACGGAGACCTGCTGGAGTGCGCCGATGATCGCGCTGA

TTTGGCTAAATATATTTGCGAAAATCAGGACAGCATCAG

CTCCAAGTTGAAGGAGTGTTGTGAAAAACCGCTGCTGGA

GAAGTCACACTGCATAGCCGAGGTGGAAAACGACGAGAT

GCCGGCAGACCTCCCCAGCCTTGCCGCGGATTTCGTCGA

ATCAAAGGATGTATGCAAAAATTACGCGGAAGCAAAAGA

TGTATTTCTGGGAATGTTCCTGTACGAGTACGCTAGGCGA

CATCCCGACTACAGCGTTGTTCTGCTCTTGAGACTTGCGA

AGACGTACGAGACTACGCTCGAGAAGTGCTGTGCAGCTG

CGGACCCCCATGAGTGTTATGCTAAAGTCTTCGACGAATT

TAAGCCTTTGGTGGAAGAGCCACAGAACCTGATCAAACA

AAATTGTGAACTGTTCGAACAATTGGGGGAGTATAAATT

TCAGAACGCTCTCCTTGTTCGGTATACAAAAAAAGTACCG

CAGGTAAGTACGCCGACACTCGTGGAAGTAAGCAGGAAC

CTCGGAAAGGTTGGATCAAAATGCTGCAAGCATCCGGAG

GCTAAGCGCATGCCATGCGCTGAGGATTATCTTTCAGTGG

TCCTGAACCAATTGTGCGTGTTGCACGAGAAAACTCCAGT

AAGCGATAGAGTTACCAAATGTTGTACAGAGAGCCTGGT

TAATCGACGACCTTGCTTCAGCGCCTTGGAAGTCGATGAG

ACGTATGTGCCGAAGGAATTTAACGCCGAAACTTTCACTT

TTCATGCAGATATCTGTACATTGAGCGAAAAGGAAAGGC

AAATTAAAAAACAAACTGCGCTTGTGGAATTGGTCAAGC

ACAAGCCTAAAGCCACAAAGGAACAGCTCAAAGCGGTA

ATGGACGATTTTGCGGCGTTCGTAGAGAAGTGTTGCAAG

GCGGACGATAAAGAAACGTGCTTTGCTGAGGAGGGAAAA

AAGCTTGTTGCTGCCAGTCAAGCGGCGCTTGGCTTGAGTG

GTGGAGAACAAAAACTCATTTCCGAGGAAGATCTTTGA

116
ProC1494/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm16-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

LIGHT-3HB-
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

1204DNI-HSA-His
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

Protein with signal
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

sequence
RLRDGTRSYFGAFMVSSAGGGSGGGSGGSGEIAALKQEIAA

LKKEIAALKWEIAALKQGYYGGSGGSLSGRSDNIGSDAHKS

EVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEV

TEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSHHHHHH

117
ProC1494/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm16-
AGGACAGAGCGGCTCACGGCATCCTTGTAGACACGACCC

LIGHT-3HB-
ACACATCATCTGTTACAAGTTTGGAGGCGGCAGCAGCGG

1204DNI-HSA-His
CGGCTCTATCAGCTCTGGCCTTCTGAGCGGTCGGAGCGAC

DNA with coding
AACATCGGAGGCAGCCAAGAGCGAAGATCCCATGAAGTA

sequence for signal
AACCCTGCAGCTCACCTTACAGGAGCCAACAGCAGTCTG

peptide
ACAGGTTCTGGGGGCCCCTTGTTGTGGGAGACGCAACTG

GGGCTTGCATTCCTCCGAGGGCTCAGTTACCACGACGGC

GCGCTTGTTGTTACAAAAGCAGGATACTACTATATTTACT

CAAAGGTGCAGCTGGGTGGAGTGGGATGTCCATTGGGCC

TGGCCTCAACTATAACCCATGGCCTCTATAAAAGAACGC

CCCGGTATCCTGAGGAGCTGGAGCTGTTGGTCTCACAGC

AGTCACCGTGCGGCAGAGCCACATCATCCTCTCGCGTAT

GGTGGGACTCTTCCTTCCTGGGAGGTGTAGTCCATCTCGA

GGCAGGTGAAGAAGTCGTAGTTCGCGTACTCGATGAACG

CCTGGTTCGGCTGAGGGATGGGACTAGGAGCTATTTCGG

CGCATTTATGGTATCTTCTGCAGGTGGAGGAAGTGGTGGC

GGTTCCGGTGGTTCAGGGGAAATCGCGGCACTCAAACAA

GAGATAGCGGCTTTGAAAAAGGAGATCGCAGCCCTGAAA

TGGGAAATAGCGGCCTTGAAGCAGGGCTACTATGGCGGC

AGCGGCGGCAGCCTAAGCGGACGGTCCGACAATATCGGC

AGCGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAA

GACCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATT

GCCTTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATC

ATGTCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGA

CCTGTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAAT

CATTGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGC

CACGCTCCGCGAGACATACGGCGAAATGGCCGATTGTTG

TGCGAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCA

ACACAAAGACGATAATCCCAATCTTCCGCGACTGGTGAG

ACCCGAAGTAGATGTAATGTGCACAGCTTTTCATGACAAT

GAGGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCC

CGCCGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTT

TCGCAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGCCA

GGCCGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGAT

GAGCTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAA

CGCCTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGA

GCCTTCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGT

TCCCGAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAA

CGGACCTGACAAAGGTACATACCGAATGCTGCCATGGCG

ACCTGTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCA

AGTATATTTGCGAAAACCAAGACTCCATTTCCAGTAAACT

TAAGGAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCA

TTGTATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGA

TCTGCCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGAT

GTATGTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTG

GAATGTTCTTGTATGAATACGCCCGACGGCATCCTGACTA

TTCAGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAG

ACGACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACAT

GAGTGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGG

TTGAAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGC

TCTTTGAACAACTCGGTGAATACAAATTTCAGAACGCGCT

TCTGGTTAGATATACGAAGAAAGTGCCACAGGTGAGCAC

CCCTACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGT

GGGATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAAT

GCCTTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAG

CTTTGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAG

TCACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGAC

CTTGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCC

AAAGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGA

TATTTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAA

GCAAACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAA

AGCGACGAAGGAACAGCTCAAAGCCGTAATGGATGATTT

CGCTGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAA

GGAAACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGC

CGCTAGTCAGGCGGCACTTGGTTTGAGCCACCACCACCA

TCACCACtga

118
ProC2006/
METDTLLLWVLLLWVPGSTGGSGEQKLISEEDLGDAHKSEV

ProC_cMyc-HSA-
AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

mLm16-1490DNI-
FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

LIGHT-3HB
DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

Protein with signal
DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

sequence
QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLGGGSSGGSGSQGQSGSRHPCRHDPHIICYKF

GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

RLRDGTRSYFGAFMVSSAGGGSGGGSGGSGEIAALKQEIAA

LKKEIAALKWEIAALKQGYYGG

119
ProC2006/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcGG

ProC_cMyc-HSA-
CTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTTGG

mLm16-1490DNI-
CGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGA

LIGHT-3HB
CCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCC

DNA with coding
TTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATCATG

sequence for signal
TCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCT

peptide
GTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAATCAT

TGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGCCAC

GCTCCGCGAGACATACGGCGAAATGGCCGATTGTTGTGC

GAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACA

CAAAGACGATAATCCCAATCTTCCGCGACTGGTGAGACC

CGAAGTAGATGTAATGTGCACAGCTTTTCATGACAATGA

GGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGC

CGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCG

CAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCAGGC

CGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAG

CTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGC

CTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCT

TCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCC

GAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGA

CCTGACAAAGGTACATACCGAATGCTGCCATGGCGACCT

GTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTA

TATTTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAG

GAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGT

ATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTG

CCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTAT

GTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAA

TGTTCTTGTATGAATACGCCCGACGGCATCCTGACTATTC

AGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACG

ACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACATGAG

TGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTG

AAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCT

TTGAACAACTCGGTGAATACAAATTTCAGAACGCGCTTCT

GGTTAGATATACGAAGAAAGTGCCACAGGTGAGCACCCC

TACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGG

ATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATGCC

TTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTT

TGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGTC

ACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACCT

TGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCAA

AGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGATAT

TTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCA

AACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGC

GACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTCGC

TGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAGGA

AACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGC

TAGTCAGGCGGCACTTGGTTTGGGGGGCGGAAGCAGCGG

CGGCAGCGGCAGCCAAGGCCAGAGCGGCAGCAGGCACC

CTTGTAGACACGATCCTCACATCATCTGTTACAAGTTTGG

AGGAGGCAGTAGCGGTGGCAGTATTAGCAGCGGACTGCT

GAGTGGCAGAAGCGACAACATCGGCGGCAGCCAGGAGA

GACGGAGCCACGAGGTGAACCCCGCTGCCCACCTGACCG

GCGCCAACAGCAGTCTGACCGGCAGCGGCGGCCCTCTGC

TGTGGGAGACACAGCTGGGCCTGGCCTTTCTGAGAGGCC

TGTCCTACCACGACGGCGCCCTGGTCGTGACCAAGGCCG

GCTACTACTACATCTACAGCAAGGTGCAGCTGGGAGGCG

TGGGCTGCCCTCTGGGCCTGGCATCTACCATCACGCACGG

CCTGTACAAGCGGACCCCTAGATATCCTGAGGAACTGGA

ACTCCTGGTGTCCCAGCAGAGCCCTTGCGGCAGAGCTAC

AAGCAGCTCAAGAGTGTGGTGGGACAGCAGCTTCCTGGG

CGGAGTGGTCCACCTGGAAGCTGGAGAAGAAGTGGTGGT

CCGGGTGCTGGACGAGAGACTCGTGAGGCTGAGAGACGG

AACAAGAAGCTACTTCGGCGCTTTTATGGTGTCTTCTGCA

GGTGGAGGAAGTGGTGGCGGTTCCGGTGGTTCAGGGGAA

ATCGCGGCACTCAAACAAGAGATAGCGGCTTTGAAAAAG

GAGATCGCAGCCCTGAAATGGGAAATAGCGGCCTTGAAG

CAGGGCTACTATGGCGGCtga

120
ProC1497/
METDTLLLWVLLLWVPGSTGGSGEQKLISEEDLGDAHKSEV

ProC_cMyc-HSA-
AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

21GS-1204DNI-
FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

LIGHT
DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

Protein with signal
DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

sequence
QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLSSAGGGSSGGSLSGRSDNIGSQERRSHEVNP

AAHLTGANSSLTGSGGPLLWETQLGLAFLRGLSYHDGALV

VTKAGYYYIYSKVQLGGVGCPLGLASTITHGLYKRTPRYPE

ELELLVSQQSPCGRATSSSRVWWDSSFLGGVVHLEAGEEVV

VRVLDERLVRLRDGTRSYFGAFMV

121
ProC1497/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcGG

ProC_cMyc-HSA-
CTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTTGG

21GS-1204DNI-
CGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGA

LIGHT
CCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCC

DNA with coding
TTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATCATG

sequence for signal
TCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCT

peptide
GTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAATCAT

TGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGCCAC

GCTCCGCGAGACATACGGCGAAATGGCCGATTGTTGTGC

GAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACA

CAAAGACGATAATCCCAATCTTCCGCGACTGGTGAGACC

CGAAGTAGATGTAATGTGCACAGCTTTTCATGACAATGA

GGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGC

CGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCG

CAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCAGGC

CGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAG

CTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGC

CTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCT

TCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCC

GAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGA

CCTGACAAAGGTACATACCGAATGCTGCCATGGCGACCT

GTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTA

TATTTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAG

GAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGT

ATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTG

CCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTAT

GTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAA

TGTTCTTGTATGAATACGCCCGACGGCATCCTGACTATTC

AGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACG

ACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACATGAG

TGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTG

AAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCT

TTGAACAACTCGGTGAATACAAATTTCAGAACGCGCTTCT

GGTTAGATATACGAAGAAAGTGCCACAGGTGAGCACCCC

TACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGG

ATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATGCC

TTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTT

TGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGTC

ACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACCT

TGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCAA

AGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGATAT

TTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCA

AACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGC

GACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTCGC

TGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAGGA

AACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGC

TAGTCAGGCGGCACTTGGTTTGTCCAGCGCCGGGGGCGG

AAGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGACAACA

TCGGCAGCCAGGAGAGACGGAGCCACGAGGTGAACCCC

GCTGCCCACCTGACCGGCGCCAACAGCAGTCTGACCGGC

AGCGGCGGCCCTCTGCTGTGGGAGACACAGCTGGGCCTG

GCCTTTCTGAGAGGCCTGTCCTACCACGACGGCGCCCTGG

TCGTGACCAAGGCCGGCTACTACTACATCTACAGCAAGG

TGCAGCTGGGAGGCGTGGGCTGCCCTCTGGGCCTGGCAT

CTACCATCACGCACGGCCTGTACAAGCGGACCCCTAGAT

ATCCTGAGGAACTGGAACTCCTGGTGTCCCAGCAGAGCC

CTTGCGGCAGAGCTACAAGCAGCTCAAGAGTGTGGTGGG

ACAGCAGCTTCCTGGGCGGAGTGGTCCACCTGGAAGCTG

GAGAAGAAGTGGTGGTCCGGGTGCTGGACGAGAGACTCG

TGAGGCTGAGAGACGGAACAAGAAGCTACTTCGGCGCTT

TTATGGTGtga

122
ProC1489/
METDTLLLWVLLLWVPGSTGQERRSHEVNPAAHLTGANSS

ProC_LIGHT-
LTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYIYS

1490DNI-mLm16-
KVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQSPC

HSA-cMyc
GRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLVRL

Protein with signal
RDGTRSYFGAFMVGGGSISSGLLSGRSDNIGGGSSGGSRHPC

sequence
RHDPHIICYKFSGGGSGGGSGDAHKSEVAHRFKDLGEENFK

ALVLIAFAQYLQQCPFEDHVKLVNEVTEFAKTCVADESAEN

CDKSLHTLFGDKLCTVATLRETYGEMADCCAKQEPERNEC

FLQHKDDNPNLPRLVRPEVDVMCTAFHDNEETFLKKYLYEI

ARRHPYFYAPELLFFAKRYKAAFTECCQAADKAACLLPKL

DELRDEGKASSAKQRLKCASLQKFGERAFKAWAVARLSQR

FPKAEFAEVSKLVTDLTKVHTECCHGDLLECADDRADLAK

YICENQDSISSKLKECCEKPLLEKSHCIAEVENDEMPADLPSL

AADFVESKDVCKNYAEAKDVFLGMFLYEYARRHPDYSVV

LLLRLAKTYETTLEKCCAAADPHECYAKVFDEFKPLVEEPQ

NLIKQNCELFEQLGEYKFQNALLVRYTKKVPQVSTPTLVEV

SRNLGKVGSKCCKHPEAKRMPCAEDYLSVVLNQLCVLHEK

TPVSDRVTKCCTESLVNRRPCFSALEVDETYVPKEFNAETFT

FHADICTLSEKERQIKKQTALVELVKHKPKATKEQLKAVMD

DFAAFVEKCCKADDKETCFAEEGKKLVAASQAALGLSEQK

LISEEDL

123
ProC1489/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_LIGHT-
AGAGCGAAGATCCCATGAAGTAAACCCTGCAGCTCACCT

1490DNI-mLm16-
TACAGGAGCCAACAGCAGTCTGACAGGTTCTGGGGGCCC

HSA-cMyc
CTTGTTGTGGGAGACGCAACTGGGGCTTGCATTCCTCCGA

DNA with coding
GGGCTCAGTTACCACGACGGCGCGCTTGTTGTTACAAAA

sequence for signal
GCAGGATACTACTATATTTACTCAAAGGTGCAGCTGGGT

peptide
GGAGTGGGATGTCCATTGGGCCTGGCCTCAACTATAACC

CATGGCCTCTATAAAAGAACGCCCCGGTATCCTGAGGAG

CTGGAGCTGTTGGTCTCACAGCAGTCACCGTGCGGCAGA

GCCACATCATCCTCTCGCGTATGGTGGGACTCTTCCTTCC

TGGGAGGTGTAGTCCATCTCGAGGCAGGTGAAGAAGTCG

TAGTTCGCGTACTCGATGAACGCCTGGTTCGGCTGAGGG

ATGGGACTAGGAGCTATTTCGGCGCATTTATGGTAGGCG

GCGGCTCTATCTCCTCCGGCCTGCTGAGCGGCAGAAGCG

ACAACATCGGCGGAGGCAGCTCCGGCGGCTCTAGACACC

CTTGTAGACACGATCCTCACATCATCTGTTACAAGTTTTC

TGGTGGAGGAAGTGGTGGCGGTTCCGGTGATGCACATAA

AAGTGAGGTGGCCCACCGCTTTAAAGACCTCGGCGAGGA

GAACTTCAAGGCACTCGTACTTATTGCCTTTGCACAATAC

CTGCAGCAATGTCCGTTTGAAGATCATGTCAAGCTCGTAA

ATGAAGTGACAGAGTTCGCTAAGACCTGTGTAGCTGACG

AAAGTGCCGAAAACTGCGACAAATCATTGCATACATTGT

TCGGCGACAAGCTTTGTACAGTTGCCACGCTCCGCGAGA

CATACGGCGAAATGGCCGATTGTTGTGCGAAACAGGAAC

CCGAAAGAAATGAGTGCTTCTTGCAACACAAAGACGATA

ATCCCAATCTTCCGCGACTGGTGAGACCCGAAGTAGATG

TAATGTGCACAGCTTTTCATGACAATGAGGAAACCTTTCT

TAAAAAATATCTGTACGAAATCGCCCGCCGACACCCGTA

TTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGCGCTAC

AAGGCAGCGTTTACAGAATGCTGCCAGGCCGCTGATAAA

GCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCGCGACG

AGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAAGTGTG

CATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAGGCTTG

GGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAGGCGGA

GTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTGACAAA

GGTACATACCGAATGCTGCCATGGCGACCTGTTGGAGTG

CGCCGATGATCGAGCGGATCTTGCCAAGTATATTTGCGA

AAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTGTTGT

GAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCGGAG

GTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCACTC

GCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAAACT

ATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTTGTA

TGAATACGCCCGACGGCATCCTGACTATTCAGTTGTGCTC

CTTCTTCGATTGGCTAAAACTTATGAGACGACACTTGAAA

AGTGTTGTGCCGCCGCCGACCCACATGAGTGCTACGCTA

AGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACCGCA

GAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACAACTC

GGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGATATA

CGAAGAAAGTGCCACAGGTGAGCACCCCTACATTGGTTG

AGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAGTGCT

GCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCTGAGG

ATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTCTTCAC

GAAAAGACTCCCGTCAGCGACCGAGTCACGAAGTGCTGT

ACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTCCGCGC

TTGAGGTGGATGAGACCTACGTCCCAAAGGAATTCAACG

CCGAGACGTTCACTTTCCATGCCGATATTTGCACCTTGTC

AGAAAAGGAGCGACAGATAAAAAAGCAAACTGCTTTGGT

GGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAGGAACA

GCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCGTGGAG

AAATGTTGTAAGGCCGATGACAAGGAAACCTGCTTCGCT

GAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGGCGGCA

CTTGGTTTGAGCGAACAAAAACTCATTTCCGAGGAAGAT

CTTtga

124
ProC1488/
METDTLLLWVLLLWVPGSTGGSGEQKLISEEDLGDAHKSEV

ProC_cMyc-HSA-
AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

mLm16-1490DNI-
FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

LIGHT
DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

Protein with signal
DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

sequence
QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLGGGSSGGSGSQGQSGSRHPCRHDPHIICYKF

GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

RLRDGTRSYFGAFMV

125
ProC1488/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcGG

ProC_cMyc-HSA-
CTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTTGG

mLm16-1490DNI-
CGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGA

LIGHT
CCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCC

DNA with coding
TTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATCATG

sequence for signal
TCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCT

peptide
GTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAATCAT

TGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGCCAC

GCTCCGCGAGACATACGGCGAAATGGCCGATTGTTGTGC

GAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACA

CAAAGACGATAATCCCAATCTTCCGCGACTGGTGAGACC

CGAAGTAGATGTAATGTGCACAGCTTTTCATGACAATGA

GGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGC

CGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCG

CAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCAGGC

CGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAG

CTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGC

CTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCT

TCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCC

GAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGA

CCTGACAAAGGTACATACCGAATGCTGCCATGGCGACCT

GTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTA

TATTTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAG

GAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGT

ATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTG

CCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTAT

GTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAA

TGTTCTTGTATGAATACGCCCGACGGCATCCTGACTATTC

AGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACG

ACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACATGAG

TGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTG

AAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCT

TTGAACAACTCGGTGAATACAAATTTCAGAACGCGCTTCT

GGTTAGATATACGAAGAAAGTGCCACAGGTGAGCACCCC

TACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGG

ATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATGCC

TTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTT

TGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGTC

ACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACCT

TGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCAA

AGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGATAT

TTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCA

AACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGC

GACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTCGC

TGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAGGA

AACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGC

TAGTCAGGCGGCACTTGGTTTGGGGGGCGGAAGCAGCGG

CGGCAGCGGCAGCCAAGGCCAGAGCGGCAGCAGGCACC

CTTGTAGACACGATCCTCACATCATCTGTTACAAGTTTGG

AGGAGGCAGTAGCGGTGGCAGTATTAGCAGCGGACTGCT

GAGTGGCAGAAGCGACAACATCGGCGGCAGCCAGGAGA

GACGGAGCCACGAGGTGAACCCCGCTGCCCACCTGACCG

GCGCCAACAGCAGTCTGACCGGCAGCGGCGGCCCTCTGC

TGTGGGAGACACAGCTGGGCCTGGCCTTTCTGAGAGGCC

TGTCCTACCACGACGGCGCCCTGGTCGTGACCAAGGCCG

GCTACTACTACATCTACAGCAAGGTGCAGCTGGGAGGCG

TGGGCTGCCCTCTGGGCCTGGCATCTACCATCACGCACGG

CCTGTACAAGCGGACCCCTAGATATCCTGAGGAACTGGA

ACTCCTGGTGTCCCAGCAGAGCCCTTGCGGCAGAGCTAC

AAGCAGCTCAAGAGTGTGGTGGGACAGCAGCTTCCTGGG

CGGAGTGGTCCACCTGGAAGCTGGAGAAGAAGTGGTGGT

CCGGGTGCTGGACGAGAGACTCGTGAGGCTGAGAGACGG

AACAAGAAGCTACTTCGGCGCTTTTATGGTGtga

126
ProC1498/
METDTLLLWVLLLWVPGSTGGSGEQKLISEEDLGDAHKSEV

ProC_cMyc-HSA-
AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

21GS-1204DNI-
FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

LIGHT-mLm16
DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

Protein with signal
DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

sequence
QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLSSAGGGSSGGSLSGRSDNIGSQERRSHEVNP

AAHLTGANSSLTGSGGPLLWETQLGLAFLRGLSYHDGALV

VTKAGYYYIYSKVQLGGVGCPLGLASTITHGLYKRTPRYPE

ELELLVSQQSPCGRATSSSRVWWDSSFLGGVVHLEAGEEVV

VRVLDERLVRLRDGTRSYFGAFMVGGGSISSGLLSGRSDNI

GGGSSGGSRHPCRHDPHIICYKF

127
ProC1498/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcGG

ProC_cMyc-HSA-
CTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTTGG

21GS-1204DNI-
CGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGA

LIGHT-mLm16
CCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCC

DNA with coding
TTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATCATG

sequence for signal
TCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCT

peptide
GTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAATCAT

TGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGCCAC

GCTCCGCGAGACATACGGCGAAATGGCCGATTGTTGTGC

GAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACA

CAAAGACGATAATCCCAATCTTCCGCGACTGGTGAGACC

CGAAGTAGATGTAATGTGCACAGCTTTTCATGACAATGA

GGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGC

CGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCG

CAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCAGGC

CGCTGATAAAGCCGCTTGTCTtCTGCCTAAGCTTGATGAG

CTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGC

CTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCT

TCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCC

GAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGA

CCTGACAAAGGTACATACCGAATGCTGCCATGGCGACCT

GTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTA

TATTTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAG

GAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGT

ATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTG

CCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTAT

GTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAA

TGTTCTTGTATGAATACGCCCGACGGCATCCTGACTATTC

AGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACG

ACACTTGAAAAGTGTTGTGCCGCtGCtGACCCACATGAGT

GCTACGCTAAGGTTTTCGACGAATTTAAGCCaTTGGTTGA

AGAACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCTTT

GAACAACTCGGTGAATACAAATTTCAGAACGCGCTTCTG

GTTAGATATACGAAGAAAGTGCCACAGGTGAGCACCCCT

ACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGGA

TCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATGCCT

TGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTTT

GCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGTCA

CGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACCTT

GCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCAAA

GGAATTCAACGCCGAGACGTTCACTTTCCATGCCGATATT

TGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCAA

ACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGCG

ACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTCGCT

GCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAGGAA

ACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGCT

AGTCAGGCGGCACTTGGTTTGTCCAGCGCCGGGGGCGGA

AGCAGCGGCGGCAGCTTAAGCGGCAGAAGCGACAACAT

CGGCAGCCAGGAGAGACGGAGCCACGAGGTGAACCCCG

CTGCCCACCTGACCGGCGCCAACAGCAGTCTGACCGGCA

GCGGCGGCCCTCTGCTGTGGGAGACACAGCTGGGCCTGG

CCTTTCTGAGAGGCCTGTCCTACCACGACGGCGCCCTGGT

CGTGACCAAGGCCGGCTACTACTACATCTACAGCAAGGT

GCAGCTGGGAGGCGTGGGCTGCCCTCTGGGCCTGGCATC

TACCATCACGCACGGCCTGTACAAGCGGACCCCTAGATA

TCCTGAGGAACTGGAACTCCTGGTGTCCCAGCAGAGCCC

TTGCGGCAGAGCTACAAGCAGCTCAAGAGTGTGGTGGGA

CAGCAGCTTCCTGGGCGGAGTGGTCCACCTGGAAGCTGG

AGAAGAAGTGGTGGTCCGGGTGCTGGACGAGAGACTCGT

GAGGCTGAGAGACGGAACAAGAAGCTACTTCGGCGCTTT

TATGGTGGGCGGAGGCTCCATTTCTAGCGGCCTGCTGAGC

GGCAGAAGCGATAACATCGGCGGaGGAAGCAGCGGAGGC

AGCAGACACCCCTGCAGACACGATCCTCACATCATCTGC

TACAAGTTCtga

128
ProC1162/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

16_1490_LIGHT_
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

11linker_HSA-cMyc
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

Protein with signal
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

sequence
RLRDGTRSYFGAFMVSSAGGGSSGGSDAHKSEVAHRFKDL

GEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTEFAKTCVA

DESAENCDKSLHTLFGDKLCTVATLRETYGEMADCCAKQE

PERNECFLQHKDDNPNLPRLVRPEVDVMCTAFHDNEETFLK

KYLYEIARRHPYFYAPELLFFAKRYKAAFTECCQAADKAAC

LLPKLDELRDEGKASSAKQRLKCASLQKFGERAFKAWAVA

RLSQRFPKAEFAEVSKLVTDLTKVHTECCHGDLLECADDRA

DLAKYICENQDSISSKLKECCEKPLLEKSHCIAEVENDEMPA

DLPSLAADFVESKDVCKNYAEAKDVFLGMFLYEYARRHPD

YSVVLLLRLAKTYETTLEKCCAAADPHECYAKVFDEFKPLV

EEPQNLIKQNCELFEQLGEYKFQNALLVRYTKKVPQVSTPT

LVEVSRNLGKVGSKCCKHPEAKRMPCAEDYLSVVLNQLCV

LHEKTPVSDRVTKCCTESLVNRRPCFSALEVDETYVPKEFN

AETFTFHADICTLSEKERQIKKQTALVELVKHKPKATKEQLK

AVMDDFAAFVEKCCKADDKETCFAEEGKKLVAASQAALG

LSGGEQKLISEEDL

129
ProC1162/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm-
AGGGCAATCCGGATCTCGGCATCCGTGTCGGCATGACCC

16_1490_LIGHT_
TCACATCATATGCTATAAGTTTGGGGGGGGATCCTCAGGT

11linker_HSA-cMyc
GGTTCCATTTCTTCTGGTTTGTTGTCTGGAAGATCAGACA

DNA with coding
ACATCGGCGGATCTCAAGAAAGACGCTCTCATGAGGTGA

sequence for signal
ATCCTGCCGCGCACCTTACTGGGGCAAACTCCAGTCTGAC

peptide
CGGATCAGGTGGGCCATTGCTTTGGGAGACACAGTTGGG

ACTGGCATTCCTTCGAGGCCTCAGCTACCATGATGGCGCC

CTGGTCGTAACGAAAGCTGGGTATTACTATATATATAGCA

AAGTCCAACTGGGGGGGGTTGGGTGTCCCCTGGGGCTCG

CGTCAACCATCACCCACGGACTCTATAAGAGAACACCAA

GATACCCAGAAGAGTTGGAACTTCTCGTGTCTCAACAAA

GTCCATGTGGGAGGGCAACATCTTCTTCACGCGTATGGTG

GGATTCATCCTTTCTCGGTGGCGTTGTCCATCTTGAAGCA

GGGGAGGAAGTTGTTGTCAGAGTCTTGGATGAAAGACTC

GTGAGATTGCGGGATGGTACTAGATCCTACTTCGGCGCGT

TCATGGTCTCCTCAGCGGGAGGTGGGAGTAGTGGCGGCT

CAGACGCCCATAAATCCGAAGTGGCACATCGATTTAAGG

ACCTCGGGGAGGAGAACTTCAAAGCTCTGGTACTCATCG

CCTTTGCTCAGTACTTGCAGCAATGCCCCTTCGAGGATCA

TGTCAAACTCGTGAACGAGGTTACGGAGTTCGCTAAAAC

ATGTGTTGCTGACGAGTCTGCAGAGAACTGTGACAAATC

CCTCCACACGCTGTTCGGTGATAAACTGTGTACGGTGGCT

ACCCTCAGGGAAACCTACGGAGAGATGGCCGATTGTTGC

GCCAAACAGGAGCCTGAGAGGAACGAATGCTTTCTTCAA

CACAAGGATGACAATCCTAACTTGCCTAGGCTGGTTCGG

CCCGAGGTCGATGTGATGTGCACAGCGTTTCACGACAAC

GAAGAAACATTCCTGAAGAAATACTTGTACGAGATTGCT

AGGCGACACCCATATTTCTACGCGCCGGAGCTTCTCTTCT

TTGCGAAGCGCTACAAGGCTGCATTTACAGAGTGCTGCC

AAGCCGCTGATAAGGCGGCCTGTCTTCTCCCCAAGCTCG

ATGAACTCCGAGATGAAGGGAAAGCTTCATCAGCGAAAC

AAAGATTGAAATGTGCTTCCCTCCAAAAGTTTGGAGAAC

GAGCCTTTAAGGCTTGGGCAGTGGCACGGCTCAGTCAGC

GCTTTCCTAAGGCTGAATTTGCCGAAGTGTCCAAGCTTGT

AACGGATCTCACTAAAGTTCATACTGAATGCTGCCACGG

AGACCTTCTCGAATGCGCGGACGATCGCGCGGACTTGGC

GAAATATATATGCGAGAATCAAGATAGTATCAGCAGTAA

ACTCAAAGAGTGCTGCGAGAAGCCTCTCCTCGAAAAGAG

CCACTGTATCGCCGAGGTGGAAAATGATGAGATGCCTGC

GGACTTGCCATCCCTTGCCGCAGACTTTGTCGAATCAAAA

GACGTTTGCAAGAATTACGCGGAGGCAAAAGATGTATTC

CTTGGCATGTTCTTGTACGAATACGCACGGCGCCACCCTG

ACTATTCAGTAGTGTTGCTCTTGAGACTCGCTAAAACATA

CGAAACGACGCTTGAGAAATGTTGCGCAGCAGCCGATCC

CCACGAGTGTTACGCAAAGGTGTTCGACGAGTTTAAACC

CCTCGTTGAAGAACCTCAAAACCTGATAAAACAAAATTG

TGAGTTGTTCGAGCAGTTGGGAGAGTACAAGTTTCAGAA

TGCTCTCCTGGTTCGGTACACCAAGAAGGTCCCACAAGTG

TCCACGCCCACCCTCGTAGAGGTATCACGGAACCTTGGC

AAGGTCGGTAGCAAGTGCTGCAAACACCCAGAAGCTAAG

CGCATGCCATGCGCTGAAGACTATCTGTCTGTGGTGCTTA

ATCAATTGTGTGTACTGCATGAGAAAACTCCTGTGTCCGA

CCGGGTTACCAAGTGCTGTACCGAGTCACTCGTCAACCG

GCGACCTTGTTTTTCTGCGCTGGAGGTTGATGAGACGTAT

GTTCCGAAAGAATTCAACGCCGAGACTTTCACCTTCCATG

CTGATATATGCACACTCAGTGAAAAAGAACGACAAATAA

AGAAGCAAACCGCATTGGTCGAGCTGGTCAAGCATAAAC

CCAAAGCTACAAAAGAACAATTGAAGGCTGTTATGGATG

ACTTTGCCGCGTTCGTAGAGAAATGCTGCAAGGCAGATG

ATAAAGAGACATGTTTCGCCGAAGAGGGCAAGAAACTGG

TGGCCGCCTCTCAAGCTGCACTTGGGCTCTCTGGAGGCGA

ACAAAAGCTTATAAGCGAAGAGGACTTGTGA

130
ProC1163/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

16_1490_LIGHT_
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

i21lnker_HSA-cMyc
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

Protein with signal
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

sequence
RLRDGTRSYFGAFMVSSAGGGSSGGSSAGGGSSGGSDAHK

SEVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNE

VTEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGE

MADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTA

FHDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSGGEQKLISEEDL

131
ProC1163/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm-
GGGACAGTCCGGATCTAGGCATCCATGTCGGCATGACCC

16_1490_LIGHT_
ACATATCATATGCTACAAATTCGGTGGAGGATCTTCTGGA

21linker_HSA-cMyc
GGCTCAATTTCATCAGGACTCCTGTCCGGGCGCTCCGACA

DNA with coding
ATATTGGTGGCTCCCAGGAGAGGAGATCACATGAAGTCA

sequence for signal
ACCCGGCCGCCCATCTTACTGGTGCCAATAGTAGTCTTAC

peptide
AGGTTCTGGCGGACCCTTGCTTTGGGAGACCCAGCTGGG

ACTGGCTTTCCTTAGAGGCCTGAGTTATCACGACGGGGCG

TTGGTCGTTACTAAAGCCGGGTATTACTATATATACTCTA

AGGTTCAGCTCGGCGGTGTAGGATGCCCACTGGGTCTTGC

GTCTACAATTACACATGGTCTGTATAAGAGGACTCCCAG

ATATCCAGAAGAACTGGAATTGCTTGTTTCCCAGCAATCT

CCGTGCGGACGCGCAACGAGCTCCAGTAGGGTGTGGTGG

GACTCCAGCTTCCTGGGTGGCGTTGTCCATTTGGAGGCGG

GAGAGGAAGTAGTGGTGCGGGTCCTTGATGAACGCCTTG

TACGACTTCGGGACGGTACAAGAAGCTACTTTGGGGCTTT

CATGGTATCTTCTGCAGGGGGGGGGTCATCCGGCGGAAG

TTCAGCGGGGGGGGGATCCTCCGGTGGCAGTGATGCACA

TAAAAGTGAGGTGGCCCACCGCTTTAAAGACCTCGGCGA

GGAGAACTTCAAGGCACTCGTACTTATTGCCTTTGCACAA

TACCTGCAGCAATGTCCGTTTGAAGATCATGTCAAGCTCG

TAAATGAAGTGACAGAGTTCGCTAAGACCTGTGTAGCTG

ACGAAAGTGCCGAAAACTGCGACAAATCATTGCATACAT

TGTTCGGCGACAAGCTTTGTACAGTTGCCACGCTCCGCGA

GACATACGGCGAAATGGCCGATTGTTGTGCGAAACAGGA

ACCCGAAAGAAATGAGTGCTTCTTGCAACACAAAGACGA

TAATCCCAATCTTCCGCGACTGGTGAGACCCGAAGTAGA

TGTAATGTGCACAGCTTTTCATGACAATGAGGAAACCTTT

CTTAAAAAATATCTGTACGAAATCGCCCGCCGACACCCG

TATTTCTATGCCCCAGAGCTGTTGTTTTTCGCAAAGCGCT

ACAAGGCAGCGTTTACCGAATGCTGCCAGGCCGCTGATA

AAGCCGCTTGTCTGCTGCCTAAGCTTGATGAGCTTCGCGA

CGAGGGTAAGGCTTCCAGCGCTAAACAACGCCTGAAGTG

TGCATCTTTGCAAAAATTTGGTGAACGAGCCTTCAAGGCT

TGGGCTGTTGCCAGGCTGAGTCAACGGTTCCCGAAGGCG

GAGTTTGCGGAGGTTTCCAAGTTGGTAACGGACCTGACA

AAGGTACATACCGAATGCTGCCATGGCGACCTGTTGGAG

TGCGCCGATGATCGAGCGGATCTTGCCAAGTATATTTGCG

AAAACCAAGACTCCATTTCCAGTAAACTTAAGGAGTGTT

GTGAGAAACCTCTCCTTGAAAAGAGCCATTGTATAGCGG

AGGTCGAAAACGATGAAATGCCCGCTGATCTGCCGTCAC

TCGCTGCTGACTTCGTTGAATCCAAGGATGTATGTAAAAA

CTATGCCGAAGCTAAGGACGTCTTTCTTGGAATGTTCTTG

TATGAATACGCCCGACGGCATCCTGACTATTCAGTTGTGC

TCCTTCTTCGATTGGCTAAAACTTATGAGACGACACTTGA

AAAGTGTTGTGCCGCCGCCGACCCACATGAGTGCTACGC

TAAGGTTTTCGACGAATTTAAGCCCTTGGTTGAAGAACCG

CAGAATCTCATTAAGCAAAATTGTGAGCTCTTTGAACAAC

TCGGTGAATACAAATTTCAGAACGCGCTTCTGGTTAGATA

TACGAAGAAAGTGCCACAGGTGAGCACCCCTACATTGGT

TGAGGTCAGTAGGAACCTCGGCAAGGTGGGATCTAAGTG

CTGCAAACACCCGGAGGCAAAGAGAATGCCTTGCGCTGA

GGATTATCTCTCAGTGGTTCTGAATCAGCTTTGCGTTCTTC

ACGAAAAGACTCCCGTCAGCGACCGAGTCACGAAGTGCT

GTACCGAGAGCCTTGTTAATAGACGACCTTGCTTCTCCGC

GCTTGAGGTGGATGAGACCTACGTCCCAAAGGAATTCAA

CGCCGAGACGTTCACTTTCCATGCCGATATTTGCACCTTG

TCAGAAAAGGAGCGACAGATAAAAAAGCAAACTGCTTTG

GTGGAGCTGGTTAAGCATAAGCCTAAAGCGACGAAGGAA

CAGCTCAAAGCCGTAATGGATGATTTCGCTGCCTTCGTGG

AGAAATGTTGTAAGGCCGATGACAAGGAAACCTGCTTCG

CTGAAGAGGGTAAAAAGCTCGTCGCCGCTAGTCAGGCGG

CACTTGGTTTGTCAGGTGGGGAGCAGAAACTTATCTCCGA

AGAGGATTTGTAA

132
ProC1164/
METDTLLLWVLLLWVPGSTGQGQSGSRHPCRHDPHIICYKF

ProC_mLm-
GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

16_1490_LIGHT_
SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKAGYYYI

IgG4 WT hinge_HSA-
YSKVQLGGVGCPLGLASTITHGLYKRTPRYPEELELLVSQQS

cMyc
PCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLDERLV

Protein with signal
RLRDGTRSYFGAFMVESKYGPPCPSCPAPEFLGGPSDAHKS

sequence
EVAHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEV

TEFAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEM

ADCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAF

HDNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTEC

CQAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGE

RAFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHG

DLLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCI

AEVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMF

LYEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECY

AKVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRY

TKKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAED

YLSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALE

VDETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVK

HKPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGK

KLVAASQAALGLSGGEQKLISEEDL

133
ProC1164/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcCA

ProC_mLm-
AGGCCAGAGTGGGAGTAGGCATCCATGTCGCCATGATCC

16_1490_LIGHT_
TCACATTATATGCTATAAATTTGGTGGGGGAAGCAGTGGT

IgG4 WT hinge_HSA-
GGGTCCATCAGTAGTGGGCTGTTGTCCGGTCGGAGTGAT

cMyc
AATATTGGAGGCTCCCAGGAACGCAGGAGTCATGAAGTT

DNA with coding
AACCCGGCGGCACATCTTACGGGTGCGAACTCTAGTCTTA

sequence for signal
CCGGGAGTGGGGGGCCCCTGCTTTGGGAGACACAGCTTG

peptide
GGCTCGCTTTCCTCAGGGGACTCTCTTACCATGATGGCGC

ACTGGTAGTAACCAAAGCTGGATACTATTATATTTACTCT

AAAGTTCAATTGGGGGGCGTTGGCTGCCCACTCGGCCTC

GCATCTACTATCACCCATGGGTTGTATAAGCGGACCCCTA

GATACCCTGAGGAACTTGAGCTTTTGGTTTCTCAACAGTC

ACCTTGCGGTAGGGCTACCTCATCAAGCCGCGTTTGGTGG

GACAGTTCATTTCTCGGGGGCGTAGTCCATCTGGAGGCA

GGTGAGGAAGTAGTGGTTCGAGTGCTCGACGAGCGCCTC

GTACGACTCCGGGATGGGACGAGAAGTTATTTCGGCGCC

TTTATGGTAGAGTCAAAATACGGGCCTCCCTGTCCCTCTT

GTCCGGCACCCGAATTTCTTGGCGGGCCCTCTGATGCCCA

CAAGTCTGAAGTTGCGCATAGATTTAAAGACCTCGGAGA

GGAGAATTTTAAAGCACTCGTGCTTATCGCATTTGCGCAG

TACCTGCAGCAGTGCCCTTTCGAGGACCACGTCAAGCTTG

TCAACGAGGTGACAGAATTCGCCAAAACATGTGTCGCCG

ATGAGTCTGCCGAGAACTGTGACAAAAGTTTGCATACCC

TGTTCGGCGACAAACTCTGCACTGTAGCAACTCTTAGGGA

AACATACGGGGAAATGGCAGACTGTTGCGCGAAACAGGA

GCCAGAACGAAACGAATGTTTCTTGCAGCACAAGGATGA

TAACCCTAATCTCCCGAGGTTGGTCAGGCCCGAAGTCGA

CGTAATGTGCACGGCTTTCCATGACAATGAGGAAACCTTC

CTCAAGAAGTACCTCTACGAAATAGCACGAAGACATCCG

TATTTCTATGCTCCTGAGCTGCTCTTTTTCGCTAAACGCTA

TAAGGCCGCATTCACGGAGTGTTGTCAAGCCGCCGATAA

GGCTGCTTGCCTTCTGCCCAAGTTGGACGAACTGCGCGAT

GAGGGGAAAGCATCATCAGCAAAGCAACGCCTGAAATGC

GCTAGTTTGCAAAAATTCGGGGAACGCGCCTTCAAAGCT

TGGGCTGTCGCGCGGCTCTCACAGAGGTTCCCCAAGGCT

GAGTTCGCCGAAGTTTCCAAGCTGGTTACTGATTTGACCA

AAGTGCACACAGAATGTTGCCACGGCGACCTGCTTGAGT

GTGCGGATGACCGCGCAGATCTCGCGAAGTATATATGCG

AAAACCAGGATTCAATTAGCTCTAAATTGAAAGAATGTT

GTGAGAAACCTCTGCTTGAAAAGTCACACTGCATTGCGG

AGGTGGAAAATGATGAAATGCCCGCAGATCTCCCCTCTTT

GGCAGCGGACTTCGTGGAGAGTAAAGACGTCTGTAAGAA

TTACGCCGAGGCGAAGGATGTATTCCTGGGGATGTTTCTC

TATGAATACGCTCGCAGACATCCTGACTACTCTGTGGTGC

TGCTGTTGCGCCTCGCTAAGACCTACGAAACAACCCTGG

AAAAATGTTGTGCCGCAGCTGATCCACACGAATGCTATG

CTAAAGTCTTTGATGAATTTAAGCCTTTGGTTGAGGAGCC

CCAGAACCTGATAAAACAGAACTGTGAATTGTTCGAGCA

ACTTGGAGAGTATAAATTCCAAAACGCGCTTCTCGTGCG

GTACACCAAGAAGGTGCCTCAAGTCAGTACTCCAACCCT

TGTGGAGGTAAGTCGCAATCTCGGTAAAGTTGGCAGTAA

ATGTTGTAAGCATCCTGAAGCGAAGCGCATGCCTTGTGC

AGAGGACTATCTGTCAGTAGTTCTTAACCAGCTGTGTGTG

CTTCATGAGAAAACACCCGTGTCCGACAGGGTGACAAAG

TGTTGCACTGAGAGTCTCGTGAACCGGAGACCTTGTTTCT

CCGCCCTGGAAGTGGACGAAACCTATGTGCCGAAGGAAT

TCAATGCTGAAACGTTTACGTTCCATGCCGACATCTGCAC

GCTTAGCGAGAAAGAGAGACAGATAAAGAAGCAAACCG

CCTTGGTGGAACTCGTTAAGCACAAGCCAAAAGCAACCA

AAGAACAACTCAAAGCGGTCATGGACGATTTCGCTGCAT

TTGTAGAGAAATGCTGCAAAGCGGATGACAAGGAGACGT

GTTTCGCTGAAGAGGGAAAAAAGCTCGTGGCAGCATCCC

AGGCTGCACTTGGTCTGTCTGGTGGTGAGCAAAAACTGA

TTTCAGAGGAGGATTTGTGA

134
ProC2076/
METDTLLLWVLLLWVPGSTGGSGEQKLISEEDLGDAHKSEV

ProC_cMyc-HSA-
AHRFKDLGEENFKALVLIAFAQYLQQCPFEDHVKLVNEVTE

mLm16-1490-
FAKTCVADESAENCDKSLHTLFGDKLCTVATLRETYGEMA

mhLIGHT
DCCAKQEPERNECFLQHKDDNPNLPRLVRPEVDVMCTAFH

Protein with signal
DNEETFLKKYLYEIARRHPYFYAPELLFFAKRYKAAFTECC

sequence
QAADKAACLLPKLDELRDEGKASSAKQRLKCASLQKFGER

AFKAWAVARLSQRFPKAEFAEVSKLVTDLTKVHTECCHGD

LLECADDRADLAKYICENQDSISSKLKECCEKPLLEKSHCIA

EVENDEMPADLPSLAADFVESKDVCKNYAEAKDVFLGMFL

YEYARRHPDYSVVLLLRLAKTYETTLEKCCAAADPHECYA

KVFDEFKPLVEEPQNLIKQNCELFEQLGEYKFQNALLVRYT

KKVPQVSTPTLVEVSRNLGKVGSKCCKHPEAKRMPCAEDY

LSVVLNQLCVLHEKTPVSDRVTKCCTESLVNRRPCFSALEV

DETYVPKEFNAETFTFHADICTLSEKERQIKKQTALVELVKH

KPKATKEQLKAVMDDFAAFVEKCCKADDKETCFAEEGKKL

VAASQAALGLGGGSSGGSGSQGQSGSRHPCRHDPHIICYKF

GGGSSGGSISSGLLSGRSDNIGGSQERRSHEVNPAAHLTGAN

SSLTGSGGPLLWETQLGLAFLRGLSYHDGALVVTKTGYYYI

YSKVQLGGVGCPLGLAGTITHGLYKRTPRYPEELELLVSQQ

SPCGRATSSSRVWWDSSFLGGVVHLEAGEEVVVRVLGKRL

VRLRDGTRSYFGAFMV

135
ProC2076/
atggaaaccgacacactgctgctgtgggtgctgcttttgtgggtgccaggatccacaggcGG

ProC_cMyc-HSA-
CTCTGGCGAACAAAAACTCATTTCCGAGGAAGATCTTGG

mLm16-1490-
CGATGCACATAAAAGTGAGGTGGCCCACCGCTTTAAAGA

mbLIGHT
CCTCGGCGAGGAGAACTTCAAGGCACTCGTACTTATTGCC

DNA with coding
TTTGCACAATACCTGCAGCAATGTCCGTTTGAAGATCATG

sequence for signal
TCAAGCTCGTAAATGAAGTGACAGAGTTCGCTAAGACCT

peptide
GTGTAGCTGACGAAAGTGCCGAAAACTGCGACAAATCAT

TGCATACATTGTTCGGCGACAAGCTTTGTACAGTTGCCAC

GCTCCGCGAGACATACGGCGAAATGGCCGATTGTTGTGC

GAAACAGGAACCCGAAAGAAATGAGTGCTTCTTGCAACA

CAAAGACGATAATCCCAATCTTCCGCGACTGGTGAGACC

CGAAGTAGATGTAATGTGCACAGCTTTTCATGACAATGA

GGAAACCTTTCTTAAAAAATATCTGTACGAAATCGCCCGC

CGACACCCGTATTTCTATGCCCCAGAGCTGTTGTTTTTCG

CAAAGCGCTACAAGGCAGCGTTTACaGAATGCTGtCAGGC

CGCTGATAAAGCCGCTTGTCTGCTGCCTAAGCTTGATGAG

CTTCGCGACGAGGGTAAGGCTTCCAGCGCTAAACAACGC

CTGAAGTGTGCATCTTTGCAAAAATTTGGTGAACGAGCCT

TCAAGGCTTGGGCTGTTGCCAGGCTGAGTCAACGGTTCCC

GAAGGCGGAGTTTGCGGAGGTTTCCAAGTTGGTAACGGA

CCTGACAAAGGTACATACCGAATGCTGCCATGGCGACCT

GTTGGAGTGCGCCGATGATCGAGCGGATCTTGCCAAGTA

TATTTGCGAAAACCAAGACTCCATTTCCAGTAAACTTAAG

GAGTGTTGTGAGAAACCTCTCCTTGAAAAGAGCCATTGT

ATAGCGGAGGTCGAAAACGATGAAATGCCCGCTGATCTG

CCGTCACTCGCTGCTGACTTCGTTGAATCCAAGGATGTAT

GTAAAAACTATGCCGAAGCTAAGGACGTCTTTCTTGGAA

TGTTCTTGTATGAATACGCCCGACGGCATCCTGACTATTC

AGTTGTGCTCCTTCTTCGATTGGCTAAAACTTATGAGACG

ACACTTGAAAAGTGTTGTGCCGCCGCCGACCCACATGAG

TGCTACGCTAAGGTTTTCGACGAATTTAAGCCCTTGGTTG

AAGAACCGCAGAATCTCATTAAGCAAAATTGTGAGCTCT

TTGAACAACTCGGTGAATACAAATTTCAGAACGCGCTTCT

GGTTAGATATACGAAGAAAGTGCCACAGGTGAGCACCCC

TACATTGGTTGAGGTCAGTAGGAACCTCGGCAAGGTGGG

ATCTAAGTGCTGCAAACACCCGGAGGCAAAGAGAATGCC

TTGCGCTGAGGATTATCTCTCAGTGGTTCTGAATCAGCTT

TGCGTTCTTCACGAAAAGACTCCCGTCAGCGACCGAGTC

ACGAAGTGCTGTACCGAGAGCCTTGTTAATAGACGACCT

TGCTTCTCCGCGCTTGAGGTGGATGAGACCTACGTCCCAA

AGGAATTCAACGCCGAGACGTTCACTTTCCATGCCGATAT

TTGCACCTTGTCAGAAAAGGAGCGACAGATAAAAAAGCA

AACTGCTTTGGTGGAGCTGGTTAAGCATAAGCCTAAAGC

GACGAAGGAACAGCTCAAAGCCGTAATGGATGATTTCGC

TGCCTTCGTGGAGAAATGTTGTAAGGCCGATGACAAGGA

AACCTGCTTCGCTGAAGAGGGTAAAAAGCTCGTCGCCGC

TAGTCAGGCGGCACTTGGTTTGGGGGGCGGAAGCAGCGG

CGGCAGCGGCAGCCAAGGCCAGAGCGGCAGCAGGCACC

CTTGTAGACACGATCCTCACATCATCTGTTACAAGTTTGG

AGGAGGCAGTAGCGGTGGCAGTATTAGCAGCGGACTGCT

GAGTGGCAGAAGCGACAACATCGGCGGCAGCCAAGAAC

GCCGATCACACGAAGTGAACCCTGCTGCTCACTTGACTG

GAGCTAACTCCAGCCTTACGGGGAGCGGGGGTCCTTTGC

TCTGGGAAACGCAGCTGGGTCTCGCGTTTCTTAGAGGGCT

GAGTTATCACGATGGCGCCTTGGTCGTCACGAAGACTGG

GTACTACTATATTTATAGTAAGGTACAGTTGGGGGGAGT

GGGGTGCCCTCTCGGCCTGGCTGGGACGATCACGCATGG

GCTCTACAAGCGCACGCCTAGGTATCCGGAGGAGTTGGA

ACTGTTGGTCTCACAGCAGTCCCCGTGCGGGCGAGCGAC

TTCCTCCAGTAGAGTGTGGTGGGACTCTAGCTTTCTCGGG

GGAGTGGTTCATCTTGAGGCAGGAGAGGAAGTGGTGGTA

CGGGTTTTGGGCAAGAGATTGGTGAGACTGCGGGATGGT

ACAAGATCTTATTTTGGTGCTTTCATGGTCtgaaccggttagtaatg

agtttgatatctcgacaatcaacctctggattacaaaatttgtgaaagattgactggta

Other Embodiments

It is to be understood that while the invention has been described in conjunction with the detailed description thereof, the foregoing description is intended to illustrate and not limit the scope of the invention, which is defined by the scope of the appended claims. Other aspects, advantages, and modifications are within the scope of the following claims.

TRIMERIC ACTIVATABLE CYTOKINE CONSTRUCTS AND RELATED COMPOSITIONS AND METHODS

Information

Publication Number

Date Filed

Date Published

Inventors

Original Assignees

CPC

International Classifications

Abstract

Description

Claims

CROSS-REFERENCE TO RELATED APPLICATIONS

PCT Information

Provisional Applications (1)