IMMUNOBINDERS DIRECTED AGAINST TNF

Abstract

Isolated binding proteins, e.g., antibodies or antigen binding portions thereof, which bind to tumor necrosis factor-alpha (TNF-α), e.g., human TNF-α, and related antibody-based compositions and molecules are disclosed. Also disclosed are pharmaceutical compositions comprising the antibodies, as well as therapeutic and diagnostic methods for using the antibodies.

Description

BACKGROUND OF THE INVENTION

1. Field of the Invention

TNF-α binding proteins and their uses in the prevention and/or treatment of acute and chronic immunological diseases are provided.

2. Background of the Invention

There is a need in the art for improved binding proteins capable of binding TNF-α (also referred to as tumor necrosis factor, tumor necrosis factor-alpha, tumor necrosis factor-α, TNF, and cachectin). Provided are a novel family of binding proteins, CDR grafted binding proteins, humanized binding proteins, and fragments thereof, capable of binding TNF-α with high affinity and neutralizing TNF-α.

BRIEF SUMMARY OF THE INVENTION

TNF-α binding proteins, or antigen-binding portions thereof, that bind TNF-α are provided. In an embodiment, the antigen binding domain comprises the VH region chosen from any one of SEQ ID NOs: 22, 24, 26, 28, 30, 32, 34-58, 74-83, 94-266, 478-486, 496-675, 738-762, 778-956, 1053-1062, 1073, 1075, and 1077, or one, two, or three CDRs therefrom. In another embodiment, the antigen binding domain comprises the VL region chosen from any one of SEQ ID NOs: 23, 25, 27, 29, 31, 33, 59-73, 84-93, 267-477, 487-495, 676-737, 763-777, 957-1052, 1063-1072, 1074, 1076, and 1078, or one, two, or three CDRs therefrom. In a particular embodiment, the antigen binding domain comprises a VH region and a VL region, for example, wherein the VH region comprises SEQ ID NOs: 22, 24, 26, 28, 30, 32, 34-58, 74-83, 94-266, 478-486, 496-675, 738-762, 778-956, 1053-1062, 1073, 1075, and 1077, or one, two, or three CDRs therefrom, and the VL region comprises SEQ ID NOs: 23, 25, 27, 29, 31, 33, 59-73, 84-93, 267-477, 487-495, 676-737, 763-777, 957-1052, 1063-1072, 1074, 1076, and 1078, or one, two, or three CDRs therefrom.

In an embodiment, the binding protein binds TNF-α. In another embodiment, the binding protein modulates a biological function of TNF-α. In another embodiment, the binding protein neutralizes TNF-α. In yet another embodiment, the binding protein diminishes the ability of TNF-α to bind to its receptor, for example, the binding protein diminishes the ability of pro-human TNF-α, mature-human TNF-α, or truncated-human TNF-α to bind to its receptor. In yet another embodiment, the binding protein reduces one or more TNF-α biological activities selected from: TNF-dependent cytokine production; TNF-dependent cell killing; TNF-dependent inflammation; TNF-dependent bone erosion; and TNF-dependent cartilage damage.

In an embodiment, the binding protein has an on rate constant (K_on) selected from: at least about 10²M⁻¹ s⁻¹; at least about 10³M⁻¹ s⁻¹; at least about 10⁴M⁻¹ s⁻¹; at least about 10⁵M⁻¹ s⁻¹; and at least about 10⁶M⁻¹ s⁻¹; as measured by surface plasmon resonance. In another embodiment, the binding protein has an off rate constant (K_off) selected from: at most about 10⁻³ s⁻¹; at most about 10⁻⁴ s⁻¹; at most about 10⁻⁵ s⁻¹; and at most about 10⁻⁶ s⁻¹, as measured by surface plasmon resonance. In yet another embodiment, the binding protein has a dissociation constant (K_D) selected from: at most about 10⁻⁷ M; at most about 10⁻⁸ M; at most about 10⁻⁹ M; at most about 10⁻¹⁰ M; m at most about 10⁻¹¹ M; at most about 10⁻¹² M; and at most 10⁻¹³M.

In another aspect, a method for treating a mammal is provided comprising administering to the mammal an effective amount of the pharmaceutical composition disclosed herein. In another embodiment, a method for reducing human TNF-α activity is provided, the method comprising: contacting human TNF-α with the binding protein disclosed herein such that human TNF-α activity is reduced. In another embodiment, provided is a method for reducing human TNF-α activity in a human subject suffering from a disorder in which TNF-α activity is detrimental, the method comprising administering to the human subject the binding protein disclosed herein such that human TNF-α activity in the human subject is reduced. In another embodiment, provided is a method for treating a subject for a disease or a disorder in which TNF-α activity is detrimental, the method comprising administering to the subject the binding protein disclosed herein such that treatment is achieved.

In one embodiment, the method treats diseases involving immune and inflammatory elements, such as autoimmune diseases, particularly those associated with inflammation, including Crohn's disease, psoriasis (including plaque psoriasis), arthritis (including rheumatoid arthritis, psoriatic arthritis, osteoarthritis, or juvenile idiopathic arthritis), multiple sclerosis, and ankylosing spondylitis. Therefore, the binding proteins herein may be used to treat these disorders.

DETAILED DESCRIPTION OF THE INVENTION

Provided are TNF-α binding proteins, or antigen-binding portions thereof, that bind TNF-α, pharmaceutical compositions thereof, as well as nucleic acids, recombinant expression vectors and host cells for making such binding proteins and fragments. Also provided are methods of using the binding proteins disclosed herein to detect human TNF-α, to inhibit human TNF-α either in vitro or in vivo, and to regulate gene expression or TNF-α related functions.

Unless otherwise defined herein, scientific and technical terms used in connection with the present disclosure shall have the meanings that are commonly understood by those of ordinary skill in the art. The meaning and scope of the terms should be clear, however, in the event of any latent ambiguity, definitions provided herein take precedent over any dictionary or extrinsic definition. Further, unless otherwise required by context, singular terms shall include pluralities and plural terms shall include the singular. In this application, the use of “or” means “and/or”, unless stated otherwise. Furthermore, the use of the term “including”, as well as other forms of the term, such as “includes” and “included”, is not limiting. Also, terms such as “element” or “component” encompass both elements and components comprising one unit and elements and components that comprise more than one subunit unless specifically stated otherwise.

Generally, nomenclatures used in connection with, and techniques of, cell and tissue culture, pathology, oncology, molecular biology, immunology, microbiology, genetics and protein and nucleic acid chemistry and hybridization described herein are those well known and commonly used in the art. The methods and techniques of the present disclosure are generally performed according to conventional methods well known in the art and as described in various general and more specific references that are cited and discussed throughout the present specification unless otherwise indicated. See, e.g., Sambrook et al. Molecular Cloning: A Laboratory Manual (2d ed., Cold Spring Harbor Laboratory Press, Cold Spring Harbor, N.Y. (1989)). Enzymatic reactions and purification techniques are performed according to manufacturer's specifications, as commonly accomplished in the art or as described herein. The nomenclatures used in connection with, and the laboratory procedures and techniques of, analytical chemistry, synthetic organic chemistry, and medicinal and pharmaceutical chemistry described herein are those well known and commonly used in the art. Standard techniques are used for chemical syntheses, chemical analyses, pharmaceutical preparation, formulation, and delivery, and treatment of patients.

The term “human TNF-α” (abbreviated herein as hTNF-α) includes a trimeric cytokine protein. The term includes a homotrimeric protein comprising three 17.5 kD TNF-α proteins. The homotrimeric protein is referred to as a “TNF-α protein”. The term human “TNF-α” is intended to include recombinant human TNF-α (rhTNF-α), which can be prepared by standard recombinant expression methods. The sequence of human TNF-α is shown in Table 1.

TABLE 1
Sequence of Human TNF-α
	Sequence
	Identi-	Sequence
Protein	fier	12345678901234567890123456789012
Human	SEQ	VRSSSRTPSDKPVAHVVANPQAEGQLQWLNDR
TNF-α	ID NO.: 1	ANALLANGVELRDNQLVVPSEGLYLIYSQVLF
		KGQGCPSTHVLLTHTISRIAVSYQTKVNLLSA
		IKSPCQRETPEGAEAKPWYEPIYLGGVFQLEK
		GDRLSAEINRPDYLDFAESGQVYFGIIAL

The term “antibody”, broadly refers to any immunoglobulin (Ig) molecule, or antigen binding portion thereof, comprised of four polypeptide chains, two heavy (H) chains and two light (L) chains, or any functional fragment, mutant, variant, or derivation thereof, which retains the essential epitope binding features of an Ig molecule. Such mutant, variant, or derivative antibody formats are known in the art.

In a full-length antibody, each heavy chain is comprised of a heavy chain variable region (abbreviated herein as HCVR or VH) and a heavy chain constant region. The heavy chain constant region is comprised of three domains, CH1, CH2 and CH3. Each light chain is comprised of a light chain variable region (abbreviated herein as LCVR or VL) and a light chain constant region. The light chain constant region is comprised of one domain, CL. The VH and VL regions can be further subdivided into regions of hypervariability, termed complementarity determining regions (CDR), interspersed with regions that are more conserved, termed framework regions (FR). Each VH and VL is composed of three CDRs and four FRs, arranged from amino-terminus to carboxy-terminus in the following order: FR1, CDR1, FR2, CDR2, FR3, CDR3, FR4. Immunoglobulin molecules can be of any type (e.g., IgG, IgE, IgM, IgD, IgA and IgY), class (e.g., IgG 1, IgG2, IgG 3, IgG4, IgA1 and IgA2) or subclass.

The term “antigen-binding portion” or “antigen-binding region” of a binding protein (or simply “binding protein portion”), refers to one or more fragments of a binding protein that retain the ability to specifically bind to an antigen (e.g., hTNF-α). The antigen-binding function of a binding protein can be performed by fragments of a full-length binding protein. Such binding protein embodiments may also have bispecific, dual specific, or multi-specific formats; specifically binding to two or more different antigens. Examples of binding fragments encompassed within the term “antigen-binding portion” of a binding protein include (i) a Fab fragment, a monovalent fragment consisting of the VL, VH, CL and CH1 domains; (ii) a F(ab′)₂ fragment, a bivalent fragment comprising two Fab fragments linked by a disulfide bridge at the hinge region; (iii) a Fd fragment consisting of the VH and CH1 domains; (iv) a Fv fragment consisting of the VL and VH domains of a single arm of an antibody, (v) a dAb fragment (Ward et al. (1989) Nature 341:544-546, Winter et al., PCT publication WO 90/05144 A1), which comprises a single variable domain; and (vi) an isolated complementarity determining region (CDR). Furthermore, although the two domains of the Fv fragment, VL and VH, are coded for by separate genes, they can be joined, using recombinant methods, by a synthetic linker that enables them to be made as a single protein chain in which the VL and VH regions pair to form monovalent molecules (known as single chain Fv (scFv); see, e.g., Bird et al. (1988) Science 242:423-426; and Huston et al. (1988) Proc. Natl. Acad. Sci. USA 85:5879-5883). Such single chain binding proteins are also intended to be encompassed within the term “antigen-binding portion” of a binding protein. Other forms of single chain binding proteins, such as diabodies are also encompassed. Diabodies are bivalent, bispecific binding proteins in which VH and VL domains are expressed on a single polypeptide chain, but using a linker that is too short to allow for pairing between the two domains on the same chain, thereby forcing the domains to pair with complementary domains of another chain and creating two antigen binding sites (see, e.g., Holliger, et al. (1993) Proc. Natl. Acad. Sci. USA 90:6444-6448; Poljak, et al. (1994) Structure 2:1121-1123).

The term “binding protein” refers to a polypeptide comprising one or more antigen-binding portions disclosed herein optionally linked to a linker polypeptide or a constant domain. Linker polypeptides comprise two or more amino acid residues joined by peptide bonds and are used to link one or more antigen binding portions. Such linker polypeptides are well known in the art (see e.g., Holliger, et al. (1993) Proc. Natl. Acad. Sci. USA 90:6444-6448; Poljak, et al. (1994) Structure 2:1121-1123). A constant domain refers to a heavy or light chain constant domain. Human IgG heavy chain and light chain constant domain amino acid sequences are known in the art and represented in Table 2.

TABLE 2
Sequence of Human IgG Heavy Chain Constant Domain and Light
Chain Constant Domain
	Sequence	Sequence
Protein	Identifier	12345678901234567890123456789012
Ig gamma-1	SEQ ID NO.: 2	ASTKGPSVFFLAPSSKSTSGGTAALGCLVKDY
constant region		FPEPVTVSWNSGALTSGVHTFPAVLQSSGLYS
		LSSVVTVPSSSLGTQTYICNVNHKPSNTKVDK
		KVEPKSCDKTHTCPPCPAPELLGGPSVFLFPP
		KPKDTLMISRTPEVTCVVVDVSHEDPEVKFNW
		YVDGVEVHNAKTKPREEQYNSTYRVVSVLTVL
		HQDWLNGKEYKCKVSNKALPAPIEKTISKAKG
		QPREPQVYTLPPSREEMTKNQVSLTCLVKGFY
		PSDIAVEWESNGQPENNYKTTPPVLDSDGSFF
		LYSKLTVDKSRWQQGNVFSCSVMHEALHNHYT
		QKSLSLSPGK
Ig gamma-1	SEQ ID NO.: 3	ASTKGPSVFPLAPSSKSTSGGTAALGCLVKDY
constant region		FPEPVTVSWNSGALTSGVHTFPAVLQSSGLYS
mutant		LSSVVTVPSSSLGTQTYICNVNHKPSNTKVDK
		KVEPKSCDKTHTCPPCPAPEAAGGPSVFLFPP
		KPKDTLMISRTPEVTCVVVDVSHEDPEVKFNW
		YVDGVEVHNAKTKPREEQYNSTYRVVSVLTVL
		HQDWLNGKEYKCKVSNKALPAPIEKTISKAKG
		QPREPQVYTLPPSREEMTKNQVSLTCLVKGFY
		PSDIAVEWESNGQPENNYKTTPPVLDSDGSFF
		LYSKLTVDKSRWQQGNVFSCSVMHEALHNHYT
		QKSLSLSPGK
Ig Kappa constant	SEQ ID NO.: 4	TVAAPSVFIFPPSDEQLKSGTASVVCLLNNFY
region		PREAKVQWKVDNALQSGNSQESVTEQDSKDST
		YSLSSTLTLSKADYEKHKVYACEVTHQGLSSP
		VTKSFNRGEC
Ig Lambda	SEQ ID NO.: 5	QPKAAPSVTLFPPSSEELQANKATLVCLISDF
constant region		YPGAVTVAWKADSSPVKAGVETTTPSKQSNNK
		YAASSYLSLTPEQWKSHRSYSCQVTHEGSTVE
		KTVAPTECS

A binding protein, or antigen-binding portion thereof, may be part of a larger immunoadhesion molecule, formed by covalent or noncovalent association of the binding protein or binding protein portion with one or more other proteins or peptides. Examples of such immunoadhesion molecules include use of the streptavidin core region to make a tetrameric scFv molecule (Kipriyanov, et al. (1995) Hum. Antibod. Hybridomas 6:93-101) and use of a cysteine residue, a marker peptide and a C-terminal polyhistidine tag to make bivalent and biotinylated scFv molecules (Kipriyanov, et al. (1994) Mol. Immunol. 31:1047-1058). Antibody portions, such as Fab and F(ab′)₂ fragments, can be prepared from whole antibodies using conventional techniques, such as papain or pepsin digestion, respectively, of whole antibodies. Moreover, binding proteins, binding protein portions and immunoadhesion molecules can be obtained using standard recombinant DNA techniques, as described herein.

An “isolated binding protein” refers to a binding protein, or antigen-binding portion thereof, that is substantially free of other binding proteins having different antigenic specificities (e.g., an isolated binding protein that specifically binds hTNF-α is substantially free of binding proteins that specifically bind antigens other than hTNF-α). An isolated binding protein that specifically binds hTNF-α may, however, have cross-reactivity to other antigens, such as TNF-α molecules from other species. Moreover, an isolated binding protein may be substantially free of other cellular material and/or chemicals.

The term “human binding protein” includes binding proteins, or antigen-binding portion thereof, that having variable and constant regions derived from human germline immunoglobulin sequences. The human binding proteins disclosed herein may include amino acid residues not encoded by human germline immunoglobulin sequences (e.g., mutations introduced by random or site-specific mutagenesis in vitro or by somatic mutation in vivo), for example in the CDRs and in particular CDR3. However, the term “human binding protein”, is not intended to include binding proteins in which CDR sequences derived from the germline of another mammalian species, such as a mouse, have been grafted onto human framework sequences.

The terms “Kabat numbering”, “Kabat definitions” and “Kabat labeling” are used interchangeably herein. These terms, which are recognized in the art, refer to a system of numbering amino acid residues which are more variable (i.e., hypervariable) than other amino acid residues in the heavy and light chain variable regions of an antibody, or an antigen binding portion thereof (Kabat et al. (1971) Ann. NY Acad. Sci. 190:382-391 and Kabat, et al. (1991) Sequences of Proteins of Immunological Interest, Fifth Edition, U.S. Department of Health and Human Services, NIH Publication No. 91-3242). See also, Martin, “Protein Sequence and Structure Analysis of Antibody Variable Domains,” In Kontermann and Dübel, eds., Antibody Engineering (Springer-Verlag, Berlin, 2001), Chapter 31, especially pages 432-433. For the heavy chain variable region, the hypervariable region ranges from amino acid positions 31 to 35 for CDR1, amino acid positions 50 to 65 for CDR2, and amino acid positions 95 to 106 for CDR3. For the light chain variable region, the hypervariable region ranges from amino acid positions 24 to 34 for CDR1, amino acid positions 50 to 56 for CDR2, and amino acid positions 89 to 97 for CDR3.

The term “CDR” refers to the complementarity determining region within antibody variable sequences. There are three CDRs in each of the variable regions of the heavy chain and the light chain, which are designated CDR1, CDR2 and CDR3, for each of the variable regions. The term “CDR set” refers to a group of three CDRs that occur in a single variable region capable of binding the antigen. The exact boundaries of these CDRs have been defined differently according to different systems. The system described by Kabat (Kabat et al., Sequences of Proteins of Immunological Interest (National Institutes of Health, Bethesda, Md. (1987) and (1991)) not only provides an unambiguous residue numbering system applicable to any variable region of an antibody, but also provides precise residue boundaries defining the three CDRs. These CDRs may be referred to as Kabat CDRs. Chothia and coworkers (Chothia and Lesk (1987) J. Mol. Biol. 196:901-917) and Chothia et al. (1989) Nature 342:877-883) found that certain sub-portions within Kabat CDRs adopt nearly identical peptide backbone conformations, despite having great diversity at the level of amino acid sequence. These sub-portions were designated as L1, L2 and L3 or H1, H2 and H3 where the “L” and the “H” designates the light chain and the heavy chains regions, respectively. These regions may be referred to as Chothia CDRs, which have boundaries that overlap with Kabat CDRs. Other boundaries defining CDRs overlapping with the Kabat CDRs have been described by Padlan (1995) FASEB J. 9:133-139 and MacCallum (1996) J. Mol. Biol. 262(5):732-745. Still other CDR boundary definitions may not strictly follow one of the above systems, but will nonetheless overlap with the Kabat CDRs, although they may be shortened or lengthened in light of prediction or experimental findings that particular residues or groups of residues or even entire CDRs do not significantly impact antigen binding. The methods used herein may utilize CDRs defined according to any of these systems, although particular embodiments use Kabat or Chothia defined CDRs.

Human heavy chain and light chain acceptor sequences are known in the art. In one embodiment of the disclosure the human heavy chain and light chain acceptor sequences are selected from the sequences listed from V-base (hvbase.mrc-cpe.cam.ac.uk/) or from IMGT®, the international ImMunoGeneTics information system® (himgt.cines.fr/textes/IMGTrepertoire/LocusGenes/). In another embodiment of the disclosure the human heavy chain and light chain acceptor sequences are selected from the sequences described in Table 3 and Table 4, respectively.

TABLE 3
Heavy Chain Acceptor Sequences
SEQ ID	Protein	Sequence
No.	region	12345678901234567890123456789012
SEQ ID	VH4-59 FR1	QVQLQESGPGLVKPSETLSLTCTVSGGSISS
NO: 6
SEQ ID	VH4-59 FR2	WIRQPPGKGLEWIG
NO: 7
SEQ ID	VH4-59 FR3	RVTISVDTSKNQFSLKLSSVTAADTAVYYCAR
NO: 8
SEQ ID	VH3-53 FR1	EVQLVESGGGLIQPGGSLRLSCAASGFTVSS
NO: 9
SEQ ID	VH3-53 FR2	WVRQAPGKGLEWVS
NO: 10
SEQ ID	VH3-53 FR3	RFTISRDNSKNTLYLQMNSLRAEDTAVYYCAR
NO: 11
SEQ ID	JH1/JH4/JH5	WGQGTLVTVSS
NO: 12	FR4
SEQ ID	JH2 FR4	WGRGTLVTVSS
NO: 13
SEQ ID	JH6 FR4	WGQGTTVTVSS
NO: 14

TABLE 4
Light Chain Acceptor Sequences
SEQ ID	Protein	Sequence
No.	region	12345678901234567890123456789012
SEQ ID	1-39/O12	DIQMTQSPSSLSASVGDRVTITC
NO: 15	FR1
SEQ ID	1-39/O12	WYQQKPGKAPKLLIY
NO: 16	FR2
SEQ ID	1-39/O12	GVPSRFSGSGSGTDFTLTISSLQPEDFATYYC
NO: 17	FR3
SEQ ID	3-15/L2 FR1	EIVMTQSPATLSVSPGERATLSC
NO: 18
SEQ ID	3-15/L2 FR2	WYQQKPGQAPRLLIY
NO: 19
SEQ ID	3-15/L2 FR3	GIPARFSGSGSGTEFTLTISSLQSEDFAVYYC
NO: 20
SEQ ID	JK2 FR4	FGQGTKLEIKR
NO: 21

The term “multivalent binding protein” is used in this specification to denote a binding protein comprising two or more antigen binding sites. The multivalent binding protein may be engineered to have the three or more antigen binding sites, and is generally not a naturally occurring antibody. The term “multispecific binding protein” refers to a binding protein capable of binding two or more related or unrelated targets. Dual variable domain (DVD) binding proteins or immunoglobulins (DVD-Ig) as used herein, are binding proteins that comprise two or more antigen binding sites and are tetravalent or multivalent binding proteins. Such DVD-binding proteins may be monospecific, i.e., capable of binding one antigen or multispecific, i.e., capable of binding two or more antigens. DVD-binding proteins comprising two heavy chain DVD-Ig polypeptides and two light chain DVD-Ig polypeptides are referred to a DVD-Ig. Each half of a DVD-Ig comprises a heavy chain DVD-Ig polypeptide, and a light chain DVD-Ig polypeptide, and two antigen binding sites. Each binding site comprises a heavy chain variable domain and a light chain variable domain with a total of 6 CDRs involved in antigen binding per antigen binding site. DVD binding proteins and methods of making DVD binding proteins are disclosed in U.S. Pat. No. 7,612,181.

One aspect of the disclosure pertains to a DVD binding protein comprising binding proteins capable of binding TNF-α. In a particular embodiment, the DVD binding protein is capable of binding TNF-α and a second target.

The term “neutralizing” refers to neutralization of a biological activity of a cytokine when a binding protein specifically binds the cytokine. In a particular embodiment, binding of a neutralizing binding protein to hTNF-α results in inhibition of a biological activity of hTNF-α, e.g., the neutralizing binding protein binds hTNF-α and reduces a biologically activity of hTNF-α by at least about 20%, 40%, 60%, 80%, 85% or more Inhibition of a biological activity of hTNF-α by a neutralizing binding protein can be assessed by measuring one or more indicators of hTNF-α biological activity well known in the art. For example neutralization of the cytoxicity of TNF-α on L929 cells.

In another embodiment, the terms “agonist” or “agonizing” refer to an increase of a biological activity of TNF-α when a binding protein specifically binds TNF-α, e.g., hTNF-α. In a particular embodiment, binding of an agonizing binding protein to TNF-α results in the increase of a biological activity of TNF-α. In a particular embodiment, the agonistic binding protein binds TNF-α and increases a biologically activity of TNF-α by at least about 20%, 40%, 60%, 80%, 85%, 90%, 95, 96%, 97%, 98%, 99%, and 100%. An inhibition of a biological activity of TNF-α by an agonistic binding protein can be assessed by measuring one or more indicators of TNF-α biological activity well known in the art.

The term “activity” includes activities such as the binding specificity/affinity of a binding protein for an antigen, for example, a hTNF-α binding protein that binds to a TNF-α antigen and/or the neutralizing potency (or agonizing potency) of a binding protein, for example, a hTNF-α binding protein whose binding to hTNF-α inhibits the biological activity of hTNF-α, e.g., neutralization of the cytoxicity of TNF-α on L929 cells.

The term “surface plasmon resonance” refers to an optical phenomenon that allows for the analysis of real-time biospecific interactions by detection of alterations in protein concentrations within a biosensor matrix, for example using the BIAcore system (Pharmacia Biosensor AB, Uppsala, Sweden and Piscataway, N.J.).

The term “K_on” refers to the on rate constant for association of a binding protein (e.g., an antibody) to the antigen to form, e.g., the antibody/antigen complex as is known in the art. The “K_on” also is known by the terms “association rate constant”, or “ka”, as used interchangeably herein. This value indicating the binding rate of an antibody to its target antigen or the rate of complex formation between an antibody and antigen also is shown by the equation below:

Antibody(“Ab”)+Antigen(“Ag”)→Ab−Ag

The term “K_off” refers to the off rate constant for dissociation, or “dissociation rate constant”, of a binding protein (e.g., an antibody), from the, e.g., antibody/antigen complex as is known in the art. This value indicates the dissociation rate of an antibody from its target antigen or separation of Ab−Ag complex over time into free antibody and antigen as shown by the equation below:

Ab+Ag←Ab−Ag

The term “K_D” refers to the “equilibrium dissociation constant” and refers to the value obtained in a titration measurement at equilibrium, or by dividing the dissociation rate constant (K_off) by the association rate constant (K_on). The association rate constant, the dissociation rate constant and the equilibrium dissociation constant are used to represent the binding affinity of an antibody to an antigen. Methods for determining association and dissociation rate constants are well known in the art. Using fluorescence-based techniques offers high sensitivity and the ability to examine samples in physiological buffers at equilibrium. Other experimental approaches and instruments such as a BIAcore® (biomolecular interaction analysis) assay can be used (e.g., instrument available from BIAcore International AB, a GE Healthcare company, Uppsala, Sweden). Additionally, a KinExA® (Kinetic Exclusion Assay) assay, available from Sapidyne Instruments (Boise, Id.) can also be used.

I. Binding Proteins that Bind Human TNF-α

One aspect of the present disclosure provides isolated fully-human anti-human TNF binding proteins, such as monoclonal antibodies, or antigen-binding portions thereof, that bind to TNF-α with high affinity, a slow off rate and high neutralizing capacity. A second aspect of the disclosure provides affinity-matured fully-human anti-TNF binding proteins, such as monoclonal antibodies, or antigen-binding portions thereof, that bind to TNF-α with high affinity, a slow off rate and high neutralizing capacity.

A. Method of Making TNF-α Binding Proteins

The binding proteins disclosed herein may be made by any of a number of techniques known in the art.

1. Anti-TNF-α Monoclonal Antibodies Using Transgenic Animals

In another embodiment of the disclosure, binding proteins are produced by immunizing a non-human animal comprising some, or all, of the human immunoglobulin locus with a TNF-α antigen. In a particular embodiment, the non-human animal is a XENOMOUSE transgenic mouse, an engineered mouse strain that comprises large fragments of the human immunoglobulin loci and is deficient in mouse antibody production. See, e.g., Green et al. (1994) Nature Genet. 7:13-21 and U.S. Pat. Nos. 5,916,771; 5,939,598; 5,985,615; 5,998,209; 6,075,181; 6,091,001; 6,114,598 and 6,130,364. See also PCT Publications WO 91/10741, published Jul. 25, 1991; WO 94/02602, published Feb. 3, 1994; WO 96/34096 and WO 96/33735, both published Oct. 31, 1996; WO 98/16654, published Apr. 23, 1998; WO 98/24893, published Jun. 11, 1998; WO 98/50433, published Nov. 12, 1998; WO 99/45031, published Sep. 10, 1999; WO 99/53049, published Oct. 21, 1999; WO 00/09560, published Feb. 24, 2000; and WO 00/37504, published Jun. 29, 2000. The XENOMOUSE transgenic mouse produces an adult-like human repertoire of fully human antibodies, and generates antigen-specific human Mabs. The XENOMOUSE transgenic mouse contains approximately 80% of the human antibody repertoire through introduction of megabase sized, germline configuration YAC fragments of the human heavy chain loci and x light chain loci. See, Mendez et al. (1997) Nature Genet. 15:146-156; Green and Jakobovits (1998) J. Exp. Med. 188:483-495.

2. Anti-TNF-α Monoclonal Antibodies Using Recombinant Antibody Libraries

In vitro methods also can be used to make the binding protein disclosed herein, wherein an antibody library is screened to identify an antibody having the desired binding specificity. Methods for such screening of recombinant antibody libraries are well known in the art and include methods described in, for example, U.S. Pat. No. 5,223,409; PCT Publications WO 92/18619; WO 91/17271; WO 92/20791; WO 92/15679; WO 93/01288; WO 92/01047; WO 92/09690; and WO 97/29131; Fuchs et al. (1991) Bio/Technology 9:1369-1372; Hay et al. (1992) Hum. Antibod. Hybridomas 3:81-85; Huse et al. (1989) Science 246:1275-1281; McCafferty et al. (1990) Nature 348:552-554; Griffiths et al. (1993) EMBO J. 12:725-734; Hawkins et al. (1992) J. Mol. Biol. 226:889-896; Clackson et al. (1991) Nature 352:624-628; Gram et al. (1992) Proc. Natl. Acad. Sci. USA 89:3576-3580; Garrard et al. (1991) Bio/Technology 9:1373-1377; Hoogenboom et al. (1991) Nucl. Acid Res. 19:4133-4137; and Barbas et al. (1991) Proc. Natl. Acad. Sci. USA 88:7978-7982; and U.S. Patent Publication No. 2003.0186374.

The recombinant antibody library may be from a subject immunized with TNF-α, or a portion of TNF-α. Alternatively, the recombinant antibody library may be from a naïve subject, i.e., one who has not been immunized with TNF-α, such as a human antibody library from a human subject who has not been immunized with human TNF-α. Antibodies disclosed herein are selected by screening the recombinant antibody library with the peptide comprising human TNF-α to thereby select those antibodies that recognize TNF-α. Methods for conducting such screening and selection are well known in the art, such as described in the references in the preceding paragraph. To select antibodies disclosed herein having particular binding affinities for hTNF-α, such as those that dissociate from human TNF-α with a particular k_off rate constant, the art-known method of surface plasmon resonance can be used to select antibodies having the desired k_off rate constant. To select antibodies disclosed herein having a particular neutralizing activity for hTNF-α, such as those with a particular an IC₅₀, standard methods known in the art for assessing the inhibition of hTNF-α activity may be used.

In one aspect, provided is an isolated binding protein, or an antigen-binding portion thereof, that binds TNF-α, e.g., human TNF-α. In a particular embodiment, the binding protein is a neutralizing binding protein. In various embodiments, the binding protein is a recombinant binding protein or a monoclonal antibody.

For example, the binding proteins disclosed herein can also be generated using various phage display methods known in the art. In phage display methods, functional antibody domains are displayed on the surface of phage particles which carry the polynucleotide sequences encoding them. In a particular, such phage can be utilized to display antigen-binding domains expressed from a repertoire or combinatorial antibody library (e.g., human or murine). Phage expressing an antigen binding domain that binds the antigen of interest can be selected or identified with antigen, e.g., using labeled antigen or antigen bound or captured to a solid surface or bead. Phage used in these methods are typically filamentous phage including fd and M13 binding domains expressed from phage with Fab, Fv or disulfide stabilized Fv antibody domains recombinantly fused to either the phage gene III or gene VIII protein. Examples of phage display methods that can be used to make the binding proteins disclosed herein can be found in the art.

As described in the above references, after phage selection, the binding protein coding regions from the phage can be isolated and used to generate whole binding proteins including human binding protein or any other desired antigen binding fragment, and expressed in any desired host, including mammalian cells, insect cells, plant cells, yeast, and bacteria, e.g., as described in detail below. For example, techniques to recombinantly produce Fab, Fab′ and F(ab′)₂ fragments can also be employed using methods known in the art such as those disclosed in PCT Publication WO 92/22324; Mullinax et al. (1992) BioTechniques 12(6):864-869; and Sawai et al. (1995) Am. J. Reprod. Immunol. 34:26-34; and Better et al. (1998) Science 240:1041-1043. Examples of techniques which can be used to produce single-chain Fvs and antibodies include those described in U.S. Pat. Nos. 4,946,778 and 5,258,498; Huston et al. (1991) Methods Enzymol. 203:46-88; Shu et al. (1993) Proc. Natl. Acad. Sci. USA 90:7995-7999; and Skerra et al. (1998) Science 240:1038-1041.

Alternative to screening of recombinant antibody libraries by phage display, other methodologies known in the art for screening large combinatorial libraries can be applied to the identification of dual specificity binding protein disclosed herein. One type of alternative expression system is one in which the recombinant antibody library is expressed as RNA-protein fusions, as described in PCT Publication No. WO 98/31700 and in Roberts and Szostak (1997) Proc. Natl. Acad. Sci. USA 94:12297-12302. In this system, a covalent fusion is created between an mRNA and the peptide or protein that it encodes by in vitro translation of synthetic mRNAs that carry puromycin, a peptidyl acceptor antibiotic, at their 3′ end. Thus, a specific mRNA can be enriched from a complex mixture of mRNAs (e.g., a combinatorial library) based on the properties of the encoded peptide or protein, e.g., antibody, or portion thereof, such as binding of the antibody, or portion thereof, to the dual specificity antigen. Nucleic acid sequences encoding antibodies, or portions thereof, recovered from screening of such libraries can be expressed by recombinant means as described above (e.g., in mammalian host cells) and, moreover, can be subjected to further affinity maturation by either additional rounds of screening of mRNA-peptide fusions in which mutations have been introduced into the originally selected sequence(s), or by other methods for affinity maturation in vitro of recombinant antibodies, as described above.

In another approach the binding proteins disclosed herein can also be generated using yeast display methods known in the art. In yeast display methods, genetic methods are used to tether antibody domains to the yeast cell wall and display them on the surface of yeast. In particular, such yeast can be utilized to display antigen-binding domains expressed from a repertoire or combinatorial antibody library (e.g., human or murine). Examples of yeast display methods that can be used to make the binding proteins disclosed herein include those disclosed Wittrup et al. U.S. Pat. No. 6,699,658 and Frenken et al., U.S. Pat. No. 6,114,147.

B. Production of Recombinant TNF-α Binding Proteins

Binding proteins disclosed herein may be produced by any of a number of techniques known in the art. For example, expression from host cells, wherein expression vector(s) encoding the heavy and light chains is (are) transfected into a host cell by standard techniques. The various forms of the term “transfection” are intended to encompass a wide variety of techniques commonly used for the introduction of exogenous DNA into a prokaryotic or eukaryotic host cell, e.g., electroporation, calcium-phosphate precipitation, DEAE-dextran transfection and the like. Although it is possible to express the binding proteins disclosed herein in either prokaryotic or eukaryotic host cells, expression of binding protein in eukaryotic cells is contemplated, for example, in mammalian host cells, because such eukaryotic cells (and in particular mammalian cells) are more likely than prokaryotic cells to assemble and secrete a properly folded and immunologically active binding protein.

Mammalian host cells for expressing the recombinant binding proteins disclosed herein include Chinese Hamster Ovary (CHO cells) (including dhfr-CHO cells, described in Urlaub and Chasin (1980) Proc. Natl. Acad. Sci. USA 77:4216-4220, used with a DHFR selectable marker, e.g., as described in Kaufman and Sharp (1982) J. Mol. Biol. 159:601-621), NS0 myeloma cells, COS cells and SP2 cells. When recombinant expression vectors encoding binding protein genes are introduced into mammalian host cells, the binding proteins are produced by culturing the host cells for a period of time sufficient to allow for expression of the binding protein in the host cells or, in particular, secretion of the antibody into the culture medium in which the host cells are grown. Antibodies can be recovered from the culture medium using standard protein purification methods.

Host cells can also be used to produce functional binding protein fragments, such as Fab fragments or scFv molecules. It will be understood that variations on the above procedure are within the scope of the present disclosure. For example, it may be desirable to transfect a host cell with DNA encoding functional fragments of either the light chain and/or the heavy chain of a binding protein disclosed herein. Recombinant DNA technology may also be used to remove some, or all, of the DNA encoding either or both of the light and heavy chains that is not necessary for binding to the antigens of interest. The molecules expressed from such truncated DNA molecules are also encompassed by the binding proteins disclosed herein. In addition, bifunctional binding proteins may be produced in which one heavy and one light chain are a binding protein disclosed herein and the other heavy and light chain are specific for an antigen other than the antigens of interest by crosslinking a binding protein disclosed herein to a second binding protein by standard chemical crosslinking methods.

In an exemplary system for recombinant expression of a binding protein, or antigen-binding portion thereof, disclosed herein, a recombinant expression vector encoding both the heavy chain and the light chain is introduced into dhfr⁻ CHO cells by calcium phosphate-mediated transfection. Within the recombinant expression vector, the heavy and light chain genes are each operatively linked to CMV enhancer/AdMLP promoter regulatory elements to drive high levels of transcription of the genes. The recombinant expression vector also carries a DHFR gene, which allows for selection of CHO cells that have been transfected with the vector using methotrexate selection/amplification. The selected transformant host cells are cultured to allow for expression of the heavy and light chains and intact binding protein is recovered from the culture medium. Standard molecular biology techniques are used to prepare the recombinant expression vector, transfect the host cells, select for transformants, culture the host cells and recover the binding protein from the culture medium. Still further a method of synthesizing a recombinant binding protein disclosed herein is provided by culturing a host cell disclosed herein in a suitable culture medium until a recombinant binding protein disclosed herein is synthesized. The method can further comprise isolating the recombinant binding protein from the culture medium.

II. hTNF-α Binding Proteins

A. Individual Clone Sequences

Table 5 provides the VH and VL sequences of fully human anti-human TNF binding proteins, including CDRs from each VH and VL sequence.

TABLE 5
Individual Fully Human Anti-TNF-α VH Sequences
		Sequence
Protein region		123456789012345678901234567890
AE11-1 VH		SEQ ID NO.: 22	EVQLVQSGAEVKKPGASVKVSCKASGYTFT
			SYDVNWVRQATGQGLEWMGWMNPNSGNTGY
			AQKFQGRVTITADESTSTAYMELSSLRSED
			TAVYYCAIFDSDYMDVWGKGTLVTVSS
AE11-1 VH	CDR-	Residues 31-35	SYDVN
	H1	of SEQ ID
		NO.: 22
AE11-1 VH	CDR-	Residues 50-66	WMNPNSGNTGYAQKFQG
	H2	of SEQ ID
		NO.: 22
AE11-1 VH	CDR-	Residues 99-106	FDSDYMDV
	H3	of SEQ ID
		NO.: 22
AE11-1 VL		SEQ ID NO.: 23	SYELTQPPSVSLSPGQTARITCSGDALPKQ
			YAYWYQQKPGQAPVLVIYKDTERPSGIPER
			FSGSSSGTTVTLTISGAQAEDEADYYCQSA
			DSSGTSWVFGGGTKLTVL
AE11-1 VL	CDR-	Residues 23-33	SGDALPKQYAY
	L1	of SEQ ID
		NO.: 23
AE11-1 VL	CDR-	Residues 49-55	KDTERPS
	L2	of SEQ ID
		NO.: 23
AE11-1 VL	CDR-	Residues 89-98	SADSSGTSWV
	L3	of SEQ ID
		NO.: 23
AE11-5 VH		SEQ ID NO.: 24	EVQLVQSGAEVKKPGSSAKVSCKASGGTFS
			SYAISWVRQAPGQGLEWMGGIIPILGTANY
			AQKFLGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGLYYDPTRADYWGQGTLVTVSS
AE11-5 VH	CDR-	Residues 31-35	SYAIS
	H1	of SEQ ID
		NO.: 24
AE11-5 VH	CDR-	Residues 50-66	GIIPILGTANYAQKFLG
	H2	of SEQ ID
		NO.: 24
AE11-5 VH	CDR-	Residues 99-109	GLYYDPTRADY
	H3	of SEQ ID
		NO.: 24
AE11-5 VL		SEQ ID NO.: 25	DIVMTQSPDFHSVTPKEKVTITCRASQSIG
			SSLHWYQQKPDQSPKLLIRHASQSISGVPS
			RFSGSGSGTDFTLTIHSLEAEDAATYYCHQ
			SSSSPPPTFGQGTQVEIK
AE11-5 VL	CDR-	Residues 24-34	RASQSIGSSLH
	L1	of SEQ ID
		NO.: 25
AE11-5 VL	CDR-	Residues 50-56	HASQSIS
	L2	of SEQ ID
		NO.: 25
AE11-5 VL	CDR-	Residues 89-98	HQSSSSPPPT
	L3	of SEQ ID
		NO.: 25
TNF-JK1 VH		SEQ ID NO.: 26	EVQLVESGGGLVQPGGSLRLSCATSGFTFN
			NYWMSWVRQAPGKGLEWVANINHDESEKYY
			VDSAKGRFTISRDNAEKSLFLQMNSLRAED
			TAVYYCARIIRGRVGFDYYNYAMDVWGQGT
			LVTVSS
TNF-JK1 VH	CDR-	Residues 31-35	NYWMS
	H1	of SEQ ID
		NO.: 26
TNF-JK1 VH	CDR-	Residues 50-66	NINHDESEKYYVDSAKG
	H2	of SEQ ID
		NO.: 26
TNF-JK1 VH	CDR-	Residues 99-115	IIRGRVGFDYYNYAMDV
	H3	of SEQ ID
		NO.: 26
TNF-JK1 VL		SEQ ID NO.: 27	DIRLTQSPSPLSASVGDRVTITCRASQSIG
			NYLNWYQHKPGKAPKLLIYAASSLQSGVPS
			RFSGTGSGTDFTLTISSLQPEDFATYYCQE
			SYSLIFAGGTKVEIK
TNF-JK1 VL	CDR-	Residues 24-34	RASQSIGNYLN
	L1	of SEQ ID
		NO.: 27
TNF-JK1 VL	CDR-	Residues 50-56	AASSLQS
	L2	of SEQ ID
		NO.: 27
TNF-JK1 VL	CDR-	Residues 89-95	QESYSLI
	L3	of SEQ ID
		NO.: 27
TNF-Y7C VH		SEQ ID NO.: 28	EVQLVQSGAEVKKPGASVKVSCKTSGYTFS
			NYDINWVRQPTGQGLEWMGWMDPNNGNTGY
			AQKFVGRVTMTRDTSKTTAYLELSGLKSED
			TAVYYCARSSGSGGTWYKEYFQSWGQGTMV
			TVSS
TNF-Y7C VH	CDR-	Residues 31-35	NYDIN
	H1	of SEQ ID
		NO.: 28
TNF-Y7C VH	CDR-	Residues 50-66	WMDPNNGNTGYAQKFVG
	H2	of SEQ ID
		NO.: 28
TNF-Y7C VH	CDR-	Residues 99-112	KSSGSGGTWYKEYFQS
	H3	of SEQ ID
		NO.: 28
TNF-Y7C VL		SEQ ID NO.: 29	DIVMTQSPLSLPVTPGEPASISCRSSQSLL
			HSNGYNYLDWYLQKPGQFPQLLIYLGSYRA
			SGVPDRFSGSGSGTDFTLKISRVEAEDVGV
			YYCMQRIEFPPGTFGQGTKLGIK
TNF-Y7C VL	CDR-	Residues 24-39	RSSQSLLHSNGYNYLD
	L1	of SEQ ID
		NO.: 29
TNF-Y7C VL	CDR-	Residues 55-61	LGSYRAS
	L2	of SEQ ID
		NO.: 29
TNF-Y7C VL	CDR-	Residues 94-103	MQRIEFPPGT
	L3	of SEQ ID
		NO.: 29
AE11-7 VH		SEQ ID NO.: 30	EVQLVQSGAEVKKPGASVKVSCKTSGYSLT
			QYPIHWVRQAPGQRPEWMGWISPGNGNTKL
			SPKFQGRVTLSRDASAGTVFMDLSGLTSDD
			TAVYFCTSVDLGDHWGQGTLVTVSS
AE11-7 VH	CDR-	Residues 31-35	QYPIH
	H1	of SEQ ID
		NO.: 30
AE11-7 VH	CDR-	Residues 50-66	WISPGNGNTKLSPKFQG
	H2	of SEQ ID
		NO.: 30
AE11-7 VH	CDR-	Residues 99-104	VDLGDH
	H3	of SEQ ID
		NO.: 30
AE11-7 VL		SEQ ID NO.: 31	DIVMTQSPEFQSVTPKEKVTITCRASQSIG
			SSLHWYQQKPDQSPKLLINYASQSFSGVPS
			RFSGGGSGTDFTLTINSLEAEDAATYYCHQ
			SSNLPITFGQGTRLEIK
AE11-7 VL	CDR-	Residues 24-34	RASQSIGSSLH
	L1	of SEQ ID
		NO.: 31
AE11-7 VL	CDR-	Residues 50-56	YASQSFS
	L2	of SEQ ID
		NO.: 31
AE11-7 VL	CDR-	Residues 89-97	HQSSNLPIT
	L3	of SEQ ID
		NO.: 31
AE11-13 VH		SEQ ID NO.: 32	EVQLVESGGGLVQPGRSLRLSCAASGFTFD
			DYPMHWVRQAPGEGLEWVSGISSNSASIGY
			ADSVKGRFTISRDNAQNTLYLQMNSLGDED
			TAVYYCVSLTLGIGQGTLVTVSS
AE11-13 VH	CDR-	Residues 31-35	DYPMH
	H1	of SEQ ID
		NO.: 32
AE11-13 VH	CDR-	Residues 50-66	GISSNSASIGYADSVKG
	H2	of SEQ ID
		NO.: 332
AE11-13 VH	CDR-	Residues 99-102	LTLG
	H3	of SEQ ID
		NO.: 32
AE11-13 VL		SEQ ID NO.: 33	DIRLTQSPSSLSASVGDRVTITCRASQSIG
			NYLHWYQQKPGKAPKLLIYAASSLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			SYSTLYSFGQGTKLEIK
AE11-13 VL	CDR-	Residues 24-34	RASQSIGNYLH
	L1	of SEQ ID
		NO.: 33
AE11-13 VL	CDR-	Residues 50-56	AASSLQS
	L2	of SEQ ID
		NO.: 33
AE11-13 VL	CDR-	Residues 89-97	QQSYSTLYS
	L3	of SEQ ID
		NO.: 33

B. IgG Converted Clones

Table 6 provides the VH sequence of humanized anti-TNF MAK-195 antibodies that were converted into IgG clones as discussed in detail in Example 2.

TABLE 6
Humanized anti-TNF MAK-195 Ab VH sequences of IgG
converted clones
Protein		Sequence
region		123456789012345678901234567890
A8		SEQ ID NO.: 34	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVNWVRQAPGKGLEWVSMIAADGFTDYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWHHGPVAYWGQGTLVTVSS
A8	CDR-H1	Residues 31-35	NYGVN
VH		of SEQ ID
		NO.: 34
A8	CDR-H2	Residues 50-65	MIAADGFTDYASSVKG
VH		of SEQ ID
		NO.: 34
A8	CDR-H3	Residues 98-106	EWHHGPVAY
VH		of SEQ ID
		NO.: 34
B5		SEQ ID NO.: 35	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSLIRGDGSTDYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWHHGPVAYWGQGTLVTVSS
B5	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 35
B5	CDR-H2	Residues 50-65	LIRGDGSTDYASSLKG
VH		of SEQ ID
		NO.: 35
B5	CDR-H3	Residues 98-106	EWHHGPVAY
VH		of SEQ ID
		NO.: 35
rHC44		SEQ ID NO.: 36	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSMIWADGSTHYA
			DTLKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC44	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 36
rHC44	CDR-H2	Residues 50-65	MIWADGSTHYADTLKS
VH		of SEQ ID
		NO.: 36
rHC44	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 36
rHC22		SEQ ID NO.: 37	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTDYA
			DTVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC22	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 37
rHC22	CDR-H2	Residues 50-65	MIWADGSTDYADTVKG
VH		of SEQ ID
		NO.: 37
rHC22	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 37
rHC81		SEQ ID NO.: 38	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			DSVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
rHC81	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 38
rHC81	CDR-H2	Residues 50-65	MIWADGSTHYADSVKS
VH		of SEQ ID
		NO.: 38
rHC81	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 38
rHC18		SEQ ID NO.: 39	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWSDGSTDYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC18	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 39
rHC18	CDR-H2	Residues 50-65	MIWSDGSTDYASSVKG
VH		of SEQ ID
		NO.: 39
rHC18	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 39
rHC14		SEQ ID NO.: 40	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPAAYWGQGTLVTVSS
rHC14	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 40
rHC14	CDR-H2	Residues 50-65	MIWADGSTHYASSLKG
VH		of SEQ ID
		NO.: 40
rHC14	CDR-H3	Residues 98-106	EWQHGPAAY
VH		of SEQ ID
		NO.: 40
rHC3		SEQ ID NO.: 41	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSMIWADGSTHYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC3	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 41
rHC3	CDR-H2	Residues 50-65	MIWADGSTHYASSLKG
VH		of SEQ ID
		NO.: 41
rHC3	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 41
rHC19		SEQ ID NO.: 42	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPAAYWGQGTLVTVSS
rHC19	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 42
rHC19	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 42
rHC19	CDR-H3	Residues 98-106	EWQHGPAAY
VH		of SEQ ID
		NO.: 42
rHC34		SEQ ID NO.: 43	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPSAYWGQGTLVTVSS
rHC34	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 43
rHC34	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 43
rHC34	CDR-H3	Residues 98-106	EWQHGPSAY
VH		of SEQ ID
		NO.: 43
rHC83		SEQ ID NO.: 44	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC83	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 44
rHC83	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 44
rHC83	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 44
S4-19		SEQ ID NO.: 45	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVEWVRQAPGKGLEWVSGIWADGSTHYA
			DTVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-19	CDR-H1	Residues 31-35	NYGVE
VH		of SEQ ID
		NO.: 45
S4-19	CDR-H2	Residues 50-65	GIWADGSTHYADTVKS
VH		of SEQ ID
		NO.: 45
S4-19	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 45
S4-50		SEQ ID NO.: 46	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVEWVRQAPGKGLEWVSGIWADGSTHYA
			DTVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVGYWGQGTLVTVSS
S4-50	CDR-H1	Residues 31-35	NYGVE
VH		of SEQ ID
		NO.: 46
S4-50	CDR-H2	Residues 50-65	GIWADGSTHYADTVKS
VH		of SEQ ID
		NO.: 46
S4-50	CDR-H3	Residues 98-106	EWQHGPVGY
VH		of SEQ ID
		NO.: 46
S4-63		SEQ ID NO.: 47	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVEWVRQAPGKGLEWVSGIWADGSTHYA
			DTVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVGYWGQGTLVTVSS
S4-63	CDR-H1	Residues 31-35	NYGVE
VH		of SEQ ID
		NO.: 47
S4-63	CDR-H2	Residues 50-65	GIWADGSTHYADTVKS
VH		of SEQ ID
		NO.: 47
S4-63	CDR-H3	Residues 98-106	EWQHGPVGY
VH		of SEQ ID
		NO.: 47
S4-55		SEQ ID NO.: 48	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTDYA
			STVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVGYWGQGTLVTVSS
S4-55	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 48
S4-55	CDR-H2	Residues 50-65	MIWADGSTDYASTVKG
VH		of SEQ ID
		NO.: 48
S4-55	CDR-H3	Residues 98-106	EWQHGPVGY
VH		of SEQ ID
		NO.: 48
S4-6		SEQ ID NO.: 49	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-6	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 49
S4-6	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 49
S4-6	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 49
S4-18		SEQ ID NO.: 50	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			DSVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
S4-18	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 50
S4-18	CDR-H2	Residues 50-65	MIWADGSTHYADSVKS
VH		of SEQ ID
		NO.: 50
S4-18	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 50
S4-31		SEQ ID NO.: 51	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVQWVRQAPGKGLEWVSGIGADGSTAYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHSGLAYWGQGTLVTVSS
S4-31	CDR-H1	Residues 31-35	NYGVQ
VH		of SEQ ID
		NO.: 51
S4-31	CDR-H2	Residues 50-65	GIGADGSTAYASSLKG
VH		of SEQ ID
		NO.: 51
S4-31	CDR-H3	Residues 98-106	EWQHSGLAY
VH		of SEQ ID
		NO.: 51
S4-34		SEQ ID NO.: 52	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSMIWADGSTHYA
			DTVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
S4-34	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 52
S4-34	CDR-H2	Residues 50-65	MIWADGSTHYADTVKG
VH		of SEQ ID
		NO.: 52
S4-34	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 52
S4-74		SEQ ID NO.: 53	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			DTVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
S4-74	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 53
S4-74	CDR-H2	Residues 50-65	MIWADGSTHYADTVKG
VH		of SEQ ID
		NO.: 53
S4-74	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 53
S4-12		SEQ ID NO.: 54	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-12	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 54
S4-12	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 54
S4-12	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 54
S4-54		SEQ ID NO.: 55	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-54	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 55
S4-54	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 55
S4-54	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 55
S4-17		SEQ ID NO.: 56	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-17	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 56
S4-17	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 56
S4-17	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 56
S4-40		SEQ ID NO.: 57	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-40	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 57
S4-40	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 57
S4-40	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 57
S4-24		SEQ ID NO.: 58	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-24	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 58
S4-24	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 58
S4-24	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 58

Table 7 provides VL sequences of IgG converted clones for Humanized anti-TNF MAK-195 antibodies as discussed in detail in Example 2.

TABLE 7
Humanized anti-TNF MAK-195 Ab VL sequences of IgG
converted clones
		Sequence
Protein region		123456789012345678901234567890
hMAK195		SEQ ID NO.: 59	DIQMTQSPSSLSASVGDRVTITCKASQAVS
VL.1			SAVAWYQQKPGKAPKLLIYWASTRHTGVPS
VL			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSTPFTFGQGTKLEIKR
hMAK195	CDR-L1	Residues 24-34	KASQAVSSAVA
VL.1		of SEQ ID
VL		NO.: 59
hMAK195	CDR-L2	Residues 50-56	WASTRHT
VL.1		of SEQ ID
VL		NO.: 59
hMAK195	CDR-L3	Residues 89-97	QQHYSTPFT
VL.1		of SEQ ID
VL		NO.: 59
S4-24		SEQ ID NO.: 60	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-24	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 60
S4-24	CDR-L2	Residues 50-56	WASTLHT
VL		of SEQ ID
		NO.: 60
S4-24	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 60
S4-40		SEQ ID NO.: 61	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFSFGQGTKLEIKR
S4-40	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 61
S4-40	CDR-L2	Residues 50-56	WASTRHS
VL		of SEQ ID
		NO.: 61
S4-40	CDR-L3	Residues 89-97	QQHYRTPFS
VL		of SEQ ID
		NO.: 61
S4-17		SEQ ID NO.: 62	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-17	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 62
S4-17	CDR-L2	Residues 50-56	WASTRHS
VL		of SEQ ID
		NO.: 62
S4-17	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 62
S4-54		SEQ ID NO.: 63	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASARHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYKTPFSFGQGTKLEIKR
S4-54	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 63
S4-54	CDR-L2	Residues 50-56	WASARHT
VL		of SEQ ID
		NO.: 63
S4-54	CDR-L3	Residues 89-97	QQHYKTPFS
VL		of SEQ ID
		NO.: 63
S4-12		SEQ ID NO.: 64	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASARHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYKTPFTFGQGTKLEIKR
S4-12	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 64
S4-12	CDR-L2	Residues 50-56	WASARHT
VL		of SEQ ID
		NO.: 64
S4-12	CDR-L3	Residues 89-97	QQHYKTPFT
VL		of SEQ ID
		NO.: 64
S4-74		SEQ ID NO.: 65	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASARHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-74	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 65
S4-74	CDR-L2	Residues 50-56	WASARHT
VL		of SEQ ID
		NO.: 65
S4-74	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 65
S4-34		SEQ ID NO.: 66	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-34	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 66
S4-34	CDR-L2	Residues 50-56	WASTRHT
VL		of SEQ ID
		NO.: 66
S4-34	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 66
S4-31		SEQ ID NO.: 67	DIQMTQSPSSLSASVGDRVTITCRASQGVS
VL			SALAWYQQKPGKAPKLLIYWASALHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSAPFTFGQGTKLEIKR
S4-31	CDR-L1	Residues 24-34	RASQGVSSALA
VL		of SEQ ID
		NO.: 67
S4-31	CDR-L2	Residues 50-56	WASALHS
VL		of SEQ ID
		NO.: 67
S4-31	CDR-L3	Residues 89-97	QQHYSAPFT
VL		of SEQ ID
		NO.: 67
S4-18		SEQ ID NO.: 68	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSTPFTFGQGTKLEIKR
S4-18	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 68
S4-18	CDR-L2	Residues 50-56	WASTLHS
VL		of SEQ ID
		NO.: 68
S4-18	CDR-L3	Residues 89-97	QQHYSTPFT
VL		of SEQ ID
		NO.: 68
S4-6		SEQ ID NO.: 69	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSTPFTFGQGTKLEIKR
S4-6	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 69
S4-6	CDR-L2	Residues 50-56	WASTRHT
VL		of SEQ ID
		NO.: 69
S4-6	CDR-L3	Residues 89-97	QQHYSTPFT
VL		of SEQ ID
		NO.: 69
S4-55		SEQ ID NO.: 70	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-55	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 70
S4-55	CDR-L2	Residues 50-56	WASTLHT
VL		of SEQ ID
		NO.: 70
S4-55	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 70
S4-63		SEQ ID NO.: 71	DIQMTQSPSSLSASVGDRVTITCKASQKVS
VL			SALAWYQQKPGKAPKLLIYWASALHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRPPFTFGQGTKLEIKR
S4-63	CDR-L1	Residues 24-34	KASQKVSSALA
VL		of SEQ ID
		NO.: 71
S4-63	CDR-L2	Residues 50-56	WASALHS
VL		of SEQ ID
		NO.: 71
S4-63	CDR-L3	Residues 89-97	QQHYRPPFT
VL		of SEQ ID
		NO.: 71
S4-50		SEQ ID NO.: 72	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASALHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSSPYTFGQGTKLEIKR
S4-50	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 72
S4-50	CDR-L2	Residues 50-56	WASALHT
VL		of SEQ ID
		NO.: 72
S4-50	CDR-L3	Residues 89-97	QQHYSSPYT
VL		of SEQ ID
		NO.: 72
S4-19		SEQ ID NO.: 73	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-19	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 73
S4-19	CDR-L2	Residues 50-56	WASTLHT
VL		of SEQ ID
		NO.: 73
S4-19	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 73

C. Individual hMAK-199 Sequences from Converted Clones

Table 8 provides VH sequences of humanized anti-TNF MAK-199 converted clones as discussed in detail in Example 3.

TABLE 8
Humanized Anti-TNF MAK-199 Ab VH sequences of IgG
converted clones
		Sequence
Protein region		123456789012345678901234567890
J662M2S3		SEQ ID NO.: 74	EVQLVQSGAEVKKPGASVKVSCKASGYTFA
#10 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
10 VH		of SEQ ID
		NO.: 74
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
10 VH		of SEQ ID
		NO.: 74
J662M2S3#	CDR-H3	Residues 99-112	RASQDISQYLN
10 VH		of SEQ ID
		NO.: 74
J662M2S3#		SEQ ID NO.: 75	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
13 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKLQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFNTVDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
13 VH		of SEQ ID
		NO.: 75
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKLQG
13 VH		of SEQ ID
		NO.: 75
J662M2S3#	CDR-H3	Residues 99-112	KLFNTVDVTDNAMD
13 VH		of SEQ ID
		NO.: 75
J662M2S3#		SEQ ID NO.: 76	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
15 VH			NYGIIWVRQAPGQGLEWMGWINTYTGVPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFNTVDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
15 VH		of SEQ ID
		NO.: 76
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGVPTYAQKFQG
15 VH		of SEQ ID
		NO.: 76
J662M2S3#	CDR-H3	Residues 99-112	KLFNTVDVTDNAMD
15 VH		of SEQ ID
		NO.: 76
J662M2S3#		SEQ ID NO.: 77	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
16 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFNTVAVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
16 VH		of SEQ ID
		NO.: 77
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
16 VH		of SEQ ID
		NO.: 77
J662M2S3#	CDR-H3	Residues 99-112	KLFNTVAVTDNAMD
16 VH		of SEQ ID
		NO.: 77
J662M2S3#		SEQ ID NO.: 78	EVQLVQSGAEVKKPGASVKVSCKASGYTFR
21 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFTTVDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
21 VH		of SEQ ID
		NO.: 78
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
21 VH		of SEQ ID
		NO.: 78
J662M2S3#	CDR-H3	Residues 99-112	KLFTTVDVTDNAMD
21 VH		of SEQ ID
		NO.: 78
J662M2S3#		SEQ ID NO.: 79	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
34 VH			NYGINWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKFRNTVAVTDYAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGIN
34 VH		of SEQ ID
		NO.: 79
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
34 VH		of SEQ ID
		NO.: 79
J662M2S3#	CDR-H3	Residues 99-112	KFRNTVAVTDYAMD
34 VH		of SEQ ID
		NO.: 79
J662M2S3#		SEQ ID NO.: 80	EVQLVQSGAEVKKPGASVKVSCKASGYTFR
36 VH			NYGITWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGIT
36 VH		of SEQ ID
		NO.: 80
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
36 VH		of SEQ ID
		NO.: 80
J662M2S3#	CDR-H3	Residues 99-112	KLFTTMDVTDNAMD
36 VH		of SEQ ID
		NO.: 80
J662M2S3#		SEQ ID NO.: 81	EVQLVQSGAEVKKPGASVKVSCKASGYTFA
45 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
45 VH		of SEQ ID
		NO.: 81
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
45 VH		of SEQ ID
		NO.: 81
J662M2S3#	CDR-H3	Residues 99-112	KLFTTMDVTDNAMD
45 VH		of SEQ ID
		NO.: 81
J662M2S3#		SEQ ID NO.: 82	EVQLVQSGAEVKKPGASVKVSCKASGYTFS
58 VH			NYGINWVRQAPGQGLEWMGWINTYTGQPSY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFKTEAVTDYAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGIN
58 VH		of SEQ ID
		NO.: 82
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGQPSYAQKFQG
58 VH		of SEQ ID
		NO.: 82
J662M2S3#	CDR-H3	Residues 99-112	KLFKTEAVTDYAMD
58 VH		of SEQ ID
		NO.: 82
J662M2S3#		SEQ ID NO.: 83	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
72 VH			NYGIIWVRQAPGQGLEWMGWINTYSGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
72 VH		of SEQ ID
		NO.: 83
J662M2S3#	CDR-H2	Residues 50-66	WINTYSGKPTYAQKFQG
72 VH		of SEQ ID
		NO.: 83
J662M2S3#	CDR-H3	Residues 99-112	KLFTTMDVTDNAMD
72 VH		of SEQ ID
		NO.: 83

Table 9 provides VL sequences of humanized anti-TNF MAK-199 converted clones as discussed in detail in Example 3.

TABLE 9
Humanized Anti-TNF MAK-199 Ab VL sequences of IgG
converted clones
		Sequence
Protein region		123456789012345678901234567890
J662M2S3#		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIS
10 VL		NO.: 84	QYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#10	CDR-L1	Residues 24-34	RASQDISQYLN
VL		of SEQ ID
		NO.: 84
J662M2S3#10	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 84
J662M2S3#10	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 84
J662M2S3#13		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIS
VL		NO.: 85	NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNSWPPTFGQGTKLEIK
J662M2S3#13	CDR-L1	Residues 24-34	RASQDISNYLN
VL		of SEQ ID
		NO.: 85
J662M2S3#13	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 85
J662M2S3#13	CDR-L3	Residues 89-97	QQGNSWPPT
VL		of SEQ
		ID NO.: 85
J662M2S3#15		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIY
VL		NO.: 86	NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTQPPTFGQGTKLEIK
J662M2S3#15	CDR-L1	Residues 24-34	RASQDIYNYLN
VL		of SEQ ID
		NO.: 86
J662M2S3#15	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 86
J662M2S3#15	CDR-L3	Residues 89-97	QQGNTQPPT
VL		of SEQ
		ID NO.: 86
J662M2S3#16		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIE
VL		NO.: 87	NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTQPPTFGQGTKLEIK
J662M2S3#16	CDR-L1	Residues 24-34	RASQDIENYLN
VL		of SEQ ID
		NO.: 87
J662M2S3#16	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 87
J662M2S3#16	CDR-L3	Residues 89-97	QQGNTQPPT
VL		of SEQ
		ID NO.: 87
J662M2S3#21		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIS
VL		NO.: 88	NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#21	CDR-L1	Residues 24-34	RASQDISNYLN
VL		of SEQ ID
		NO.: 88
J662M2S3#21	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 88
J662M2S3#21	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 88
J662M2S3#34		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIY
VL		NO.: 89	DVLNWYQQKPGKAPKLLIYYASRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			GITLPPTFGQGTKLEIK
J662M2S3#34	CDR-L1	Residues 24-34	RASQDIYDVLN
VL		of SEQ ID
		NO.: 89
J662M2S3#34	CDR-L2	Residues 50-56	YASRLQS
VL		of SEQ ID
		NO.: 89
J662M2S3#34	CDR-L3	Residues 89-97	QQGITLPPT
VL		of SEQ
		ID NO.: 89
J662M2S3#36		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIS
VL		NO.: 90	NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#36	CDR-L1	Residues 24-34	RASQDISNYLN
VL		of SEQ ID
		NO.: 90
J662M2S3#36	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 90
J662M2S3#36	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 90
J662M2S3#45		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIS
VL		NO.: 91	QYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#45	CDR-L1	Residues 24-34	RASQDISQYLN
VL		of SEQ ID
		NO.: 91
J662M2S3#45	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 91
J662M2S3#45	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 91
J662M2S3#58		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQNIY
VL		NO.: 92	NVLNWYQQKPGKAPKLLIYYASRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTMPPTFGQGTKLEIK
J662M2S3#58	CDR-L1	Residues 24-34	RASQNIYNVLN
VL		of SEQ ID
		NO.: 92
J662M2S3#58	CDR-L2	Residues 50-56	YASRLQS
VL		of SEQ ID
		NO.: 92
J662M2S3#58	CDR-L3	Residues 89-97	QQGNTMPPT
VL		of SEQ
		ID NO.: 92
J662M2S3#72		SEQ ID	DIQMTQSPSSLSASVGDRVTITCRASQDIS
VL		NO.: 93	NFLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTQPPTFGQGTKLEIK
J662M2S3#72	CDR-L1	Residues 24-34	RASQDISNFLN
VL		of SEQ ID
		NO.: 93
J662M2S3#72	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 93
J662M2S3#72	CDR-L3	Residues 89-97	QQGNTQPPT
VL		of SEQ
		ID NO.: 93

In an embodiment, the antigen binding domain comprises the VH region chosen from any one of SEQ ID NOs: 22, 24, 26, 28, 30, 32, 34-58, 74-83, 94-266, 478-486, 496-675, 738-762, 778-956, 1053-1062, 1073, 1075, and 1077, or one, two, or three CDRs therefrom. In another embodiment, the antigen binding domain comprises the VL region chosen from any one of SEQ ID NOs: 23, 25, 27, 29, 31, 33, 59-73, 84-93, 267-477, 487-495, 676-737, 763-777, 957-1052, 1063-1072, 1074, 1076, and 1078, or one, two, or three CDRs therefrom. In a particular embodiment, the antigen binding domain comprises a VH region and a VL region, for example, wherein the VH region comprises SEQ ID NOs: 22, 24, 26, 28, 30, 32, 34-58, 74-83, 94-266, 478-486, 496-675, 738-762, 778-956, 1053-1062, 1073, 1075, and 1077, or one, two, or three CDRs therefrom, and the VL region comprises SEQ ID NOs: 23, 25, 27, 29, 31, 33, 59-73, 84-93, 267-477, 487-495, 676-737, 763-777, 957-1052, 1063-1072, 1074, 1076, and 1078, or one, two, or three CDRs therefrom.

In an embodiment where the VH and/or the VL CDR sequences are provided above, the human acceptor framework comprises at least one amino acid sequence selected from: SEQ ID NOs: 6-21. In a particular embodiment, the human acceptor framework comprises an amino acid sequence selected from: SEQ 1N NOs: 9, 10, 11, 12, 15, 16, 17, and 21. In another embodiment, the human acceptor framework comprises at least one framework region amino acid substitution, wherein the amino acid sequence of the framework is at least 65% identical to the sequence of the human acceptor framework and comprises at least 70 amino acid residues identical to the human acceptor framework. In another embodiment, the human acceptor framework comprises at least one framework region amino acid substitution at a key residue. The key residue selected from: a residue adjacent to a CDR; a glycosylation site residue; a rare residue; a residue capable of interacting with human TNF-α; a residue capable of interacting with a CDR; a canonical residue; a contact residue between heavy chain variable region and light chain variable region; a residue within a Vernier zone; and a residue in a region that overlaps between a Chothia-defined variable heavy chain CDR1 and a Kabat-defined first heavy chain framework. In an embodiment, the key residue is selected from: H1, H12, H24, H27, H29, H37, H48, H49, H67, H71, H73, H76, H78, L13, L43, L58, L70, and L80. In an embodiment, the VH mutation is selected from: Q1E, I12V, A24V, G27F, I29L, V29F F29L 137V, I48L, V48L, S49G, V67L, F67L, V71K, R71K, T73N, N76S, L78I, and F78I. In another embodiment, the VL mutation is selected from: V13L, A435, I58V, E70D, and S80P. In an embodiment, the binding protein comprises two variable domains, wherein the two variable domains have amino acid sequences selected from: SEQ ID NOS: 22 and 23; 23 and 24; 24 and 25; 26 and 27; 28 and 29; 30 and 31; or 32 and 33.

III. Production of Binding Proteins and Binding Protein-Producing Cell Lines

In an embodiment, TNF-α binding proteins disclosed herein exhibit a high capacity to reduce or to neutralize TNF-α activity, e.g., as assessed by any one of several in vitro and in vivo assays known in the art. Alternatively, TNF-α binding proteins disclosed herein, also exhibit a high capacity to increase or agonize TNF-α activity.

In particular embodiments, the isolated binding protein, or antigen-binding portion thereof, binds human TNF-α, wherein the binding protein, or antigen-binding portion thereof, dissociates from human TNF-α with a k_off rate constant of about 0.1 s⁻¹ or less, as determined by surface plasmon resonance, such as 1×10⁻² s⁻¹ or less, 1×10⁻³ s⁻¹ or less, 1×10⁻⁴ s⁻¹ or less, 1×10⁻⁵ s⁻¹ or less and 1×10⁻⁶ s⁻¹ or less; or which inhibits human TNF-α activity with an IC₅₀ of about 1×10⁻⁶ M or less, such as 1×10⁻⁷M or less, 1×10⁻⁸M or less, 1×10⁻⁹M or less, 1×10−10 M or less and 1×10¹¹ M or less. In certain embodiments, the binding protein comprises a heavy chain constant region, such as an IgG1, IgG2, IgG3, IgG4, IgA, IgE, IgM or IgD constant region. In an embodiment, the heavy chain constant region is an IgG1 heavy chain constant region or an IgG4 heavy chain constant region. Furthermore, the binding protein can comprise a light chain constant region, either a kappa light chain constant region or a lambda light chain constant region. In another embodiment, the binding protein comprises a kappa light chain constant region. Alternatively, the binding protein portion can be, for example, a Fab fragment or a single chain Fv fragment.

Replacements of amino acid residues in the Fc portion to alter binding protein effector function are known in the art (See U.S. Pat. Nos. 5,648,260 and 5,624,821). The Fc portion of a binding protein mediates several important effector functions, e.g., cytokine induction, ADCC, phagocytosis, complement dependent cytotoxicity (CDC) and half-life/clearance rate of antibody and antigen-antibody complexes. In some cases these effector functions are desirable for therapeutic antibody but in other cases might be unnecessary or even deleterious, depending on the therapeutic objectives. Certain human IgG isotypes, particularly IgG1 and IgG3, mediate ADCC and CDC via binding to FcγRs and complement C1q, respectively. Neonatal Fc receptors (FcRn) are the critical components determining the circulating half-life of antibodies. In still another embodiment at least one amino acid residue is replaced in the constant region of the binding protein, for example the Fc region of the binding protein, such that effector functions of the binding protein are altered.

One embodiment provides a labeled binding protein wherein an antibody or antibody portion disclosed herein is derivatized or linked to another functional molecule (e.g., another peptide or protein). For example, a labeled binding protein disclosed herein can be derived by functionally linking an antibody or antibody portion disclosed herein (by chemical coupling, genetic fusion, noncovalent association or otherwise) to one or more other molecular entities, such as another antibody (e.g., a bispecific antibody or a diabody), a detectable agent, a cytotoxic agent, a pharmaceutical agent, and/or a protein or peptide that can mediate associate of the antibody or antibody portion with another molecule (such as a streptavidin core region or a polyhistidine tag).

Useful detectable agents with which an antibody or antibody portion disclosed herein may be derivatized include fluorescent compounds. Exemplary fluorescent detectable agents include fluorescein, fluorescein isothiocyanate, rhodamine, 5-dimethylamine-1-napthalenesulfonyl chloride, phycoerythrin and the like. An antibody may also be derivatized with detectable enzymes, such as alkaline phosphatase, horseradish peroxidase, glucose oxidase and the like. When an antibody is derivatized with a detectable enzyme, it is detected by adding additional reagents that the enzyme uses to produce a detectable reaction product. For example, when the detectable agent horseradish peroxidase is present, the addition of hydrogen peroxide and diaminobenzidine leads to a colored reaction product, which is detectable. An antibody may also be derivatized with biotin, and detected through indirect measurement of avidin or streptavidin binding.

Another embodiment of the disclosure provides a crystallized binding protein. In an embodiment, provided are crystals of whole TNF-α binding proteins and fragments thereof as disclosed herein, and formulations and compositions comprising such crystals. In one embodiment the crystallized binding protein has a greater half-life in vivo than the soluble counterpart of the binding protein. In another embodiment the binding protein retains biological activity after crystallization.

Crystallized binding protein disclosed herein may be produced according methods known in the art and as disclosed in PCT Publication WO 02/72636.

Another embodiment of the disclosure provides a glycosylated binding protein wherein the binding protein or antigen-binding portion thereof comprises one or more carbohydrate residues. Nascent in vivo protein production may undergo further processing, known as post-translational modification. In particular, sugar (glycosyl) residues may be added enzymatically, a process known as glycosylation. The resulting proteins bearing covalently linked oligosaccharide side chains are known as glycosylated proteins or glycoproteins. Protein glycosylation depends on the amino acid sequence of the protein of interest, as well as the host cell in which the protein is expressed. Different organisms may produce different glycosylation enzymes (e.g., glycosyltransferases and glycosidases), and have different substrates (nucleotide sugars) available. Due to such factors, protein glycosylation pattern, and composition of glycosyl residues, may differ depending on the host system in which the particular protein is expressed. Glycosyl residues useful in the disclosure may include, but are not limited to, glucose, galactose, mannose, fucose, n-acetylglucosamine and sialic acid. In an embodiment, the glycosylated binding protein comprises glycosyl residues such that the glycosylation pattern is human.

It is known to those skilled in the art that differing protein glycosylation may result in differing protein characteristics. For instance, the efficacy of a therapeutic protein produced in a microorganism host, such as yeast, and glycosylated utilizing the yeast endogenous pathway may be reduced compared to that of the same protein expressed in a mammalian cell, such as a CHO cell line. Such glycoproteins may also be immunogenic in humans and show reduced half-life in vivo after administration. Specific receptors in humans and other animals may recognize specific glycosyl residues and promote the rapid clearance of the protein from the bloodstream. Other adverse effects may include changes in protein folding, solubility, susceptibility to proteases, trafficking, transport, compartmentalization, secretion, recognition by other proteins or factors, antigenicity, or allergenicity. Accordingly, a practitioner may prefer a therapeutic protein with a specific composition and pattern of glycosylation, for example glycosylation composition and pattern identical, or at least similar, to that produced in human cells or in the species-specific cells of the intended subject animal.

Expressing glycosylated proteins different from that of a host cell may be achieved by genetically modifying the host cell to express heterologous glycosylation enzymes. Using techniques known in the art a practitioner may generate antibodies or antigen-binding portions thereof exhibiting human protein glycosylation. For example, yeast strains have been genetically modified to express non-naturally occurring glycosylation enzymes such that glycosylated proteins (glycoproteins) produced in these yeast strains exhibit protein glycosylation identical to that of animal cells, especially human cells (U.S. Pat. Nos. 7,449,308 and 7,029,872).

Further, it will be appreciated by one skilled in the art that a protein of interest may be expressed using a library of host cells genetically engineered to express various glycosylation enzymes, such that member host cells of the library produce the protein of interest with variant glycosylation patterns. A practitioner may then select and isolate the protein of interest with particular novel glycosylation patterns. In an embodiment, the protein having a particularly selected novel glycosylation pattern exhibits improved or altered biological properties.

IV. Uses of TNF-α Binding Proteins

Given their ability to bind to human TNF-α, e.g., the human TNF-α binding proteins, or portions thereof, disclosed herein can be used to detect TNF-α (e.g., in a biological sample, such as serum or plasma), using a conventional immunoassay, such as an enzyme linked immunosorbent assays (ELISA), an radioimmunoassay (RIA) or tissue immunohistochemistry. A method for detecting TNF-α in a biological sample is provided comprising contacting a biological sample with a binding protein, or binding protein portion, disclosed herein and detecting either the binding protein (or binding protein portion) bound to TNF-α or unbound binding protein (or binding protein portion), to thereby detect TNF-α in the biological sample. The binding protein is directly or indirectly labeled with a detectable substance to facilitate detection of the bound or unbound antibody. Suitable detectable substances include various enzymes, prosthetic groups, fluorescent materials, luminescent materials and radioactive materials. Examples of suitable enzymes include horseradish peroxidase, alkaline phosphatase, β-galactosidase, or acetylcholinesterase; examples of suitable prosthetic group complexes include streptavidin/biotin and avidin/biotin; examples of suitable fluorescent materials include umbelliferone, fluorescein, fluorescein isothiocyanate, rhodamine, dichlorotriazinylamine fluorescein, dansyl chloride or phycoerythrin; an example of a luminescent material includes luminol; and examples of suitable radioactive material include ³H, ¹⁴C, ³⁵S, ⁹⁰Y, ⁹⁹Tc, ¹¹¹In, ¹²⁵I, ¹³¹I, ¹⁷⁷Lu, ¹⁶⁶Ho, or ¹⁵³Sm.

Alternative to labeling the binding protein, human TNF-α can be assayed in biological fluids by a competition immunoassay utilizing rhTNF-α standards labeled with a detectable substance and an unlabeled human TNF-α binding protein. In this assay, the biological sample, the labeled rhTNF-α standards and the human TNF-α binding protein are combined and the amount of labeled rhTNF-α standard bound to the unlabeled binding protein is determined. The amount of human TNF-α in the biological sample is inversely proportional to the amount of labeled rhTNF-α standard bound to the TNF-α binding protein. Similarly, human TNF-α can also be assayed in biological fluids by a competition immunoassay utilizing rhTNF-α standards labeled with a detectable substance and an unlabeled human TNF-α binding protein.

In an embodiment, the binding proteins and binding protein portions disclosed herein are capable of neutralizing TNF-α activity, e.g., human TNF-α activity, both in vitro and in vivo. In another embodiment, the binding proteins and binding protein portions disclosed herein are capable of increasing or agonizing human TNF-α activity, e.g., human TNF-α activity. Accordingly, such binding proteins and binding protein portions disclosed herein can be used to inhibit or increase hTNF-α activity, e.g., in a cell culture containing hTNF-α, in human subjects or in other mammalian subjects having TNF-α with which a binding protein disclosed herein cross-reacts. In one embodiment, a method for inhibiting or increasing hTNF-α activity is provided comprising contacting hTNF-α with a binding protein or binding protein portion disclosed herein such that hTNF-α activity is inhibited or increased. For example, in a cell culture containing, or suspected of containing hTNF-α, a binding protein or binding protein portion disclosed herein can be added to the culture medium to inhibit or increase hTNF-α activity in the culture.

In another embodiment, a method is provided for reducing or increasing hTNF-α activity in a subject, advantageously from a subject suffering from a disease or disorder in which TNF-α activity is detrimental or, alternatively, beneficial. Methods for reducing or increasing TNF-α activity in a subject suffering from such a disease or disorder is provided, which method comprises administering to the subject a binding protein or binding protein portion disclosed herein such that TNF-α activity in the subject is reduced or increased. In a particular embodiment, the TNF-α is human TNF-α, and the subject is a human subject. Alternatively, the subject can be a mammal expressing a TNF-α to which a binding protein provided is capable of binding. Still further the subject can be a mammal into which TNF-α has been introduced (e.g., by administration of TNF-α or by expression of a TNF-α transgene). A binding protein disclosed herein can be administered to a human subject for therapeutic purposes. Moreover, a binding protein disclosed herein can be administered to a non-human mammal expressing a TNF-α with which the binding protein is capable of binding for veterinary purposes or as an animal model of human disease. Regarding the latter, such animal models may be useful for evaluating the therapeutic efficacy of binding proteins disclosed herein (e.g., testing of dosages and time courses of administration).

The term “a disorder in which TNF-α activity is detrimental” includes diseases and other disorders in which the presence of TNF-α activity in a subject suffering from the disorder has been shown to be or is suspected of being either responsible for the pathophysiology of the disorder or a factor that contributes to a worsening of the disorder. Accordingly, a disorder in which TNF-α activity is detrimental is a disorder in which reduction of TNF-α activity is expected to alleviate the symptoms and/or progression of the disorder. Such disorders may be evidenced, for example, by an increase in the concentration of TNF-α in a biological fluid of a subject suffering from the disorder (e.g., an increase in the concentration of TNF-α in serum, plasma, synovial fluid, etc. of the subject), which can be detected, for example, using an anti-TNF-α antibody as described above. Non-limiting examples of disorders that can be treated with the binding proteins disclosed herein include those disorders discussed in the section below pertaining to pharmaceutical compositions of the antibodies disclosed herein.

Alternatively, the term “a disorder in which TNF-α activity is beneficial” include diseases and other disorders in which the presence of TNF-α activity in a subject suffering from the disorder has been shown to be or is suspected of being either beneficial for treating the pathophysiology of the disorder or a factor that contributes to a treatment of the disorder. Accordingly, a disorder in which TNF-α activity is beneficial is a disorder in which an increase of TNF-α activity is expected to alleviate the symptoms and/or progression of the disorder. Non-limiting examples of disorders that can be treated with the antibodies disclosed herein include those disorders discussed in the section below pertaining to pharmaceutical compositions of the antibodies disclosed herein.

V. Pharmaceutical Compositions

Pharmaceutical compositions are also provided comprising a binding protein, or antigen-binding portion thereof, disclosed herein and a pharmaceutically acceptable carrier. The pharmaceutical compositions comprising binding protein disclosed herein are for use in, but not limited to, diagnosing, detecting, or monitoring a disorder, in preventing, treating, managing, or ameliorating of a disorder or one or more symptoms thereof, and/or in research. In a specific embodiment, a composition comprises one or more binding proteins disclosed herein. In another embodiment, the pharmaceutical composition comprises one or more binding proteins disclosed herein and one or more prophylactic or therapeutic agents other than binding proteins disclosed herein for treating a disorder in which TNF-α activity is detrimental. In a particular embodiment, the prophylactic or therapeutic agents known to be useful for or having been or currently being used in the prevention, treatment, management, or amelioration of a disorder or one or more symptoms thereof. In accordance with these embodiments, the composition may further comprise of a carrier, diluent or excipient.

The binding proteins and binding protein-portions disclosed herein can be incorporated into pharmaceutical compositions suitable for administration to a subject. Typically, the pharmaceutical composition comprises a binding protein or binding protein portion disclosed herein and a pharmaceutically acceptable carrier. The term “pharmaceutically acceptable carrier” includes any and all solvents, dispersion media, coatings, antibacterial and antifungal agents, isotonic and absorption delaying agents, and the like that are physiologically compatible. Examples of pharmaceutically acceptable carriers include one or more of water, saline, phosphate buffered saline, dextrose, glycerol, ethanol and the like, as well as combinations thereof. In many cases, isotonic agents, for example, sugars, polyalcohols such as mannitol, sorbitol, or sodium chloride in the composition, may be included. Pharmaceutically acceptable carriers may further comprise minor amounts of auxiliary substances such as wetting or emulsifying agents, preservatives or buffers, which enhance the shelf life or effectiveness of the binding protein or binding protein portion.

Various delivery systems are known and can be used to administer one or more binding proteins disclosed herein or the combination of one or more binding proteins disclosed herein and a prophylactic agent or therapeutic agent useful for preventing, managing, treating, or ameliorating a disorder or one or more symptoms thereof, e.g., encapsulation in liposomes, microparticles, microcapsules, recombinant cells capable of expressing the binding protein or binding protein fragment, receptor-mediated endocytosis (see, e.g., Wu and Wu (1987) J. Biol. Chem. 262:4429-4432), construction of a nucleic acid as part of a retroviral or other vector, etc. Methods of administering a prophylactic or therapeutic agent disclosed herein include, but are not limited to, parenteral administration (e.g., intradermal, intramuscular, intraperitoneal, intravenous and subcutaneous), epidural administration, intratumoral administration, and mucosal administration (e.g., intranasal and oral routes). In addition, pulmonary administration can be employed, e.g., by use of an inhaler or nebulizer, and formulation with an aerosolizing agent. In one embodiment, a binding protein disclosed herein, combination therapy, or a composition disclosed herein is administered using Alkermes AIR® pulmonary drug delivery technology (Alkermes, Inc., Cambridge, Mass.). In a specific embodiment, prophylactic or therapeutic agents disclosed herein are administered intramuscularly, intravenously, intratumorally, orally, intranasally, pulmonary, or subcutaneously. The prophylactic or therapeutic agents may be administered by any convenient route, for example by infusion or bolus injection, by absorption through epithelial or mucocutaneous linings (e.g., oral mucosa, rectal and intestinal mucosa, etc.) and may be administered together with other biologically active agents Administration can be systemic or local.

In a specific embodiment, it may be desirable to administer the prophylactic or therapeutic agents disclosed herein locally to the area in need of treatment; this may be achieved by, for example, and not by way of limitation, local infusion, by injection, or by means of an implant, said implant being of a porous or non-porous material, including membranes and matrices, such as sialastic membranes, polymers, fibrous matrices (e.g., Tissuel®), or collagen matrices. In one embodiment, an effective amount of one or more binding proteins disclosed herein antagonists is administered locally to the affected area to a subject to prevent, treat, manage, and/or ameliorate a disorder or a symptom thereof. In another embodiment, an effective amount of one or more binding proteins disclosed herein is administered locally to the affected area in combination with an effective amount of one or more therapies (e.g., one or more prophylactic or therapeutic agents) other than an antibody disclosed herein of a subject to prevent, treat, manage, and/or ameliorate a disorder or one or more symptoms thereof.

In a specific embodiment, where the composition disclosed herein is a nucleic acid encoding a prophylactic or therapeutic agent, the nucleic acid can be administered in vivo to promote expression of its encoded prophylactic or therapeutic agent, by constructing it as part of an appropriate nucleic acid expression vector and administering it so that it becomes intracellular, e.g., by use of a retroviral vector (see U.S. Pat. No. 4,980,286), or by direct injection, or by use of microparticle bombardment (e.g., a gene gun; Biolistic, DuPont), or coating with lipids or cell-surface receptors or transfecting agents, or by administering it in linkage to a homeobox-like peptide which is known to enter the nucleus (see, e.g., Joliot et al. (1991) Proc. Natl. Acad. Sci. USA 88:1864-1868). Alternatively, a nucleic acid can be introduced intracellularly and incorporated within host cell DNA for expression by homologous recombination.

The method disclosed herein may comprise administration of a composition formulated for parenteral administration by injection (e.g., by bolus injection or continuous infusion). Formulations for injection may be presented in unit dosage form (e.g., in ampoules or in multi-dose containers) with an added preservative. The compositions may take such forms as suspensions, solutions or emulsions in oily or aqueous vehicles, and may contain formulatory agents such as suspending, stabilizing and/or dispersing agents. Alternatively, the active ingredient may be in powder form for constitution with a suitable vehicle (e.g., sterile pyrogen-free water) before use.

The methods disclosed herein may additionally comprise of administration of compositions formulated as depot preparations. Such long acting formulations may be administered by implantation (e.g., subcutaneously or intramuscularly) or by intramuscular injection. Thus, for example, the compositions may be formulated with suitable polymeric or hydrophobic materials (e.g., as an emulsion in an acceptable oil) or ion exchange resins, or as sparingly soluble derivatives (e.g., as a sparingly soluble salt).

The methods disclosed herein encompass administration of compositions formulated as neutral or salt forms. Pharmaceutically acceptable salts include those formed with anions such as those derived from hydrochloric, phosphoric, acetic, oxalic, tartaric acids, etc., and those formed with cations such as those derived from sodium, potassium, ammonium, calcium, ferric hydroxides, isopropylamine, triethylamine, 2-ethylamino ethanol, histidine, procaine, etc.

Generally, the ingredients of compositions are supplied either separately or mixed together in unit dosage form, for example, as a dry lyophilized powder or water free concentrate in a hermetically sealed container such as an ampoule or sachette indicating the quantity of active agent. Where the mode of administration is infusion, composition can be dispensed with an infusion bottle containing sterile pharmaceutical grade water or saline. Where the mode of administration is by injection, an ampoule of sterile water for injection or saline can be provided so that the ingredients may be mixed prior to administration.

In particular, it is also provided that one or more of the prophylactic or therapeutic agents, or pharmaceutical compositions disclosed herein is packaged in a hermetically sealed container such as an ampoule or sachette indicating the quantity of the agent. In one embodiment, one or more of the prophylactic or therapeutic agents, or pharmaceutical compositions disclosed herein is supplied as a dry sterilized lyophilized powder or water free concentrate in a hermetically sealed container and can be reconstituted (e.g., with water or saline) to the appropriate concentration for administration to a subject. In an embodiment, one or more of the prophylactic or therapeutic agents or pharmaceutical compositions disclosed herein is supplied as a dry sterile lyophilized powder in a hermetically sealed container at a unit dosage of at least 5 mg, at least 10 mg, at least 15 mg, at least 25 mg, at least 35 mg, at least 45 mg, at least 50 mg, at least 75 mg, or at least 100 mg. The lyophilized prophylactic or therapeutic agents or pharmaceutical compositions disclosed herein should be stored at between 2° C. and 8° C. in its original container and the prophylactic or therapeutic agents, or pharmaceutical compositions disclosed herein should be administered within 1 week, within 5 days, within 72 hours, within 48 hours, within 24 hours, within 12 hours, within 6 hours, within 5 hours, within 3 hours, or within 1 hour after being reconstituted. In an alternative embodiment, one or more of the prophylactic or therapeutic agents or pharmaceutical compositions disclosed herein is supplied in liquid form in a hermetically sealed container indicating the quantity and concentration of the agent. In an embodiment, the liquid form of the administered composition is supplied in a hermetically sealed container at least 0.25 mg/ml, at least 0.5 mg/ml, at least 1 mg/ml, at least 2.5 mg/ml, at least 5 mg/ml, at least 8 mg/ml, at least 10 mg/ml, at least 15 mg/kg, at least 25 mg/ml, at least 50 mg/ml, at least 75 mg/ml or at least 100 mg/ml. The liquid form should be stored at between 2° C. and 8° C. in its original container.

The binding proteins and binding protein-portions disclosed herein can be incorporated into a pharmaceutical composition suitable for parenteral administration. In an embodiment, the binding protein or binding protein-portions will be prepared as an injectable solution containing 0.1-250 mg/ml binding protein. The injectable solution can be composed of either a liquid or lyophilized dosage form in a flint or amber vial, ampoule or pre-filled syringe. The buffer can be L-histidine (1-50 mM), optimally 5-10 mM, at pH 5.0 to 7.0 (optimally pH 6.0). Other suitable buffers include but are not limited to, sodium succinate, sodium citrate, sodium phosphate or potassium phosphate. Sodium chloride can be used to modify the toxicity of the solution at a concentration of 0-300 mM (optimally 150 mM for a liquid dosage form). Cryoprotectants can be included for a lyophilized dosage form, principally 0-10% sucrose (optimally 0.5-1.0%). Other suitable cryoprotectants include trehalose and lactose. Bulking agents can be included for a lyophilized dosage form, principally 1-10% mannitol (optimally 2-4%). Stabilizers can be used in both liquid and lyophilized dosage forms, principally 1-50 mM L-Methionine (optimally 5-10 mM). Other suitable bulking agents include glycine, arginine, can be included as 0-0.05% polysorbate-80 (optimally 0.005-0.01%). Additional surfactants include but are not limited to polysorbate 20 and BRIJ surfactants.

Typical compositions are in the form of injectable or infusible solutions, such as compositions similar to those used for passive immunization of humans with other antibodies. Therapeutic compositions typically must be sterile and stable under the conditions of manufacture and storage. The composition can be formulated as a solution, microemulsion, dispersion, liposome, or other ordered structure suitable to high drug concentration. Sterile injectable solutions can be prepared by incorporating the active compound (i.e., binding protein or binding protein portion) in the required amount in an appropriate solvent with one or a combination of ingredients enumerated above, as required, followed by filtered sterilization. Generally, dispersions are prepared by incorporating the active compound into a sterile vehicle that contains a basic dispersion medium and the required other ingredients from those enumerated above. In the case of sterile, lyophilized powders for the preparation of sterile injectable solutions, the methods of preparation include vacuum drying and spray-drying that yields a powder of the active ingredient plus any additional desired ingredient from a previously sterile-filtered solution thereof. The proper fluidity of a solution can be maintained, for example, by the use of a coating such as lecithin, by the maintenance of the required particle size in the case of dispersion and by the use of surfactants. Prolonged absorption of injectable compositions can be brought about by including, in the composition, an agent that delays absorption, for example, monostearate salts and gelatin.

As will be appreciated by the skilled artisan, the route and/or mode of administration will vary depending upon the desired results. In certain embodiments, the active compound may be prepared with a carrier that will protect the compound against rapid release, such as a controlled release formulation, including implants, transdermal patches, and microencapsulated delivery systems. Biodegradable, biocompatible polymers can be used, such as ethylene vinyl acetate, polyanhydrides, polyglycolic acid, collagen, polyorthoesters, and polylactic acid. Many methods for the preparation of such formulations are patented or generally known to those skilled in the art. See, e.g., Sustained and Controlled Release Drug Delivery Systems, J. R. Robinson, ed., Marcel Dekker, Inc., New York, 1978.

Supplementary active compounds can also be incorporated into the compositions. In certain embodiments, a binding protein or binding protein portion disclosed herein is coformulated with and/or coadministered with one or more additional therapeutic agents that are useful for treating disorders in which TNF-α activity is detrimental. For example, an anti-hTNF-α antibody or antibody portion disclosed herein may be coformulated and/or coadministered with one or more additional antibodies that bind other targets (e.g., antibodies that bind other cytokines or that bind cell surface molecules). Furthermore, one or more binding proteins disclosed herein may be used in combination with two or more of the foregoing therapeutic agents. Such combination therapies may advantageously utilize lower dosages of the administered therapeutic agents, thus avoiding possible toxicities or complications associated with the various monotherapies.

In certain embodiments, a binding protein to TNF-α or fragment thereof is linked to a half-life extending vehicle known in the art. Such vehicles include, but are not limited to, the Fc domain, polyethylene glycol, and dextran. Such vehicles are described, e.g., in U.S. Pat. No. 6,660,843.

In a specific embodiment, nucleic acid sequences comprising nucleotide sequences encoding a binding protein disclosed herein or another prophylactic or therapeutic agent disclosed herein are administered to treat, prevent, manage, or ameliorate a disorder or one or more symptoms thereof by way of gene therapy. Gene therapy refers to therapy performed by the administration to a subject of an expressed or expressible nucleic acid. In this embodiment of the disclosure, the nucleic acids produce their encoded binding protein or prophylactic or therapeutic agent disclosed herein that mediates a prophylactic or therapeutic effect.

Any of the methods for gene therapy available in the art can be used according to the present disclosure.

TNF-α plays a critical role in the pathology associated with a variety of diseases involving immune and inflammatory elements, such as autoimmune diseases, particularly those associated with inflammation, including Crohn's disease, psoriasis (including plaque psoriasis), arthritis (including rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis), multiple sclerosis, systemic lupus erythematosus, and ankylosing spondylitis. Therefore, the binding proteins herein may be used to treat these disorders. In another embodiment, the disorder is a respiratory disorder; asthma; allergic and nonallergic asthma; asthma due to infection; asthma due to infection with respiratory syncytial virus (RSV); chronic obstructive pulmonary disease (COPD); a condition involving airway inflammation; eosinophilia; fibrosis and excess mucus production; cystic fibrosis; pulmonary fibrosis; an atopic disorder; atopic dermatitis; urticaria; eczema; allergic rhinitis; allergic enterogastritis; an inflammatory and/or autoimmune condition of the skin; an inflammatory and/or autoimmune condition of gastrointestinal organs; inflammatory bowel diseases (IBD); ulcerative colitis; an inflammatory and/or autoimmune condition of the liver; liver cirrhosis; liver fibrosis; liver fibrosis caused by hepatitis B and/or C virus; scleroderma; tumors or cancers; hepatocellular carcinoma; glioblastoma; lymphoma; Hodgkin's lymphoma; a viral infection; a bacterial infection; a parasitic infection; HTLV-1 infection; suppression of expression of protective type 1 immune responses, suppression of expression of a protective type 1 immune response during vaccination, neurodegenerative diseases, neuronal regeneration, and spinal cord injury.

It will be readily apparent to those skilled in the art that other suitable modifications and adaptations of the methods disclosed herein may be made using suitable equivalents without departing from the scope of the invention or the embodiments disclosed herein. Having now described the present disclosure in detail, the same will be more clearly understood by reference to the following examples, which are included for purposes of illustration only and are not intended to be limiting of the invention.

EXAMPLES

Example 1

Identification of Fully Human Antibodies to TNF by In Vitro Display Systems

1.1: Antibody Selections

Fully human anti-human TNF monoclonal antibodies were isolated by in vitro display technologies from human antibody libraries by their ability to bind recombinant human TNF proteins. The amino acid sequences of the variable heavy (VH) and variable light (VL) chains were determined from DNA sequencing and listed in Table 10.

TABLE 10
Individual clones sequences
		Sequence
Protein region	SEQ ID NO:	123456789012345678901234567890
AE11-1 VH		22	EVQLVQSGAEVKKPGASVKVSCKASGYTFT
			SYDVN WVRQATGQGLEWMGWMNPNSGNTGY
			AQKFQG RVTITADESTSTAYMELSSLRSED
			TAVYYCAIFDSDYMDVWGKGTLVTVSS
AE11-1 VH	CDR-	Residues 31-35	SYDVN
	H1	of SEQ ID
		NO.: 22
AE11-1 VH	CDR-	Residues 50-66	WMNPNSGNTGYAQKFQG
	H2	of SEQ ID
		NO.: 22
AE11-1 VH	CDR-	Residues 99-106	FDSDYMDV
	H3	of SEQ ID
		NO.: 22
AE11-1 VL		23	SYELTQPPSVSLSPGQTARITCSGDALPKQ
			YAY WYQQKPGQAPVLVIYKDTERPSGIPER
			FSGSSSGTTVTLTISGAQAEDEADYYCQSA
			DSSGTSWV FGGGTKLTVL
AE11-1 VL	CDR-	Residues 23-33	SGDALPKQYAY
	L1	of SEQ ID
		NO.: 23
AE11-1 VL	CDR-	Residues 49-55	KDTERPS
	L2	of SEQ ID
		NO.: 23
AE11-1 VL	CDR-	Residues 89-98	SADSSGTSWV
	L3	of SEQ ID
		NO.: 23
AE11-5 VH		24	EVQLVQSGAEVKKPGSSAKVSCKASGGTFS
			SYAIS WVRQAPGQGLEWMGGIIPILGTANY
			AQKFLG RVTITADESTSTVYMELSSLRSED
			TAVYYCARGLYYDPTRADYWGQGTLVTVSS
AE11-5 VH	CDR-	Residues 31-35	SYAIS
	H1	of SEQ ID
		NO.: 24
AE11-5 VH	CDR-	Residues 50-66	GIIPILGTANYAQKFLG
	H2	of SEQ ID
		NO.: 24
AE11-5 VH	CDR-	Residues 99-109	GLYYDPTRADY
	H3	of SEQ ID
		NO.: 24
AE11-5 VL		25	DIVMTQSPDFHSVTPKEKVTITCRASQSIG
			SSLH WYQQKPDQSPKLLIRHASQSISGVPS
			RFSGSGSGTDFTLTIHSLEAEDAATYYCHQ
			SSSSPPPT FGQGTQVEIK
AE11-5 VL	CDR-	Residues 24-34	RASQSIGSSLH
	L1	of SEQ ID
		NO.: 25
AE11-5 VL	CDR-	Residues 50-56	HASQSIS
	L2	of SEQ ID
		NO.: 25
AE11-5 VL	CDR-	Residues 89-98	HQSSSSPPPT
	L3	of SEQ ID
		NO.: 25
TNF-JK1 VH		26	EVQLVESGGGLVQPGGSLRLSCATSGFTFN
			NYWMS WVRQAPGKGLEWVANINHDESEKYY
			VDSAKG RFTISRDNAEKSLFLQMNSLRAED
			TAVYYCARIIRGRVGFDYYNYAMDVWGQGT
			LVTVSS
TNF-JK1 VH	CDR-	Residues 31-35	NYWMS
	H1	of SEQ ID
		NO.: 26
TNF-JK1 VH	CDR-	Residues 50-66	NINHDESEKYYVDSAKG
	H2	of SEQ ID
		NO.: 26
TNF-JK1 VH	CDR-	Residues 99-115	IIRGRVGFDYYNYAMDV
	H3	of SEQ ID
		NO.: 26
TNF-JK1 VL		27	DIRLTQSPSPLSASVGDRVTITCRASQSIG
			NYLN WYQHKPGKAPKLLIYAASSLQSGVPS
			RFSGTGSGTDFTLTISSLQPEDFATYYCQE
			SYSLI FAGGTKVEIK
TNF-JK1 VL	CDR-	Residues 24-34	RASQSIGNYLN
	L1	of SEQ ID
		NO.: 27
TNF-JK1 VL	CDR-	Residues 50-56	AASSLQS
	L2	of SEQ ID
		NO.: 27
TNF-JK1 VL	CDR-	Residues 89-95	QESYSLI
	L3	of SEQ ID
		NO.: 27
TNF-Y7C VH		28	EVQLVQSGAEVKKPGASVKVSCKTSGYTFS
			NYDIN WVRQPTGQGLEWMGWMDPNNGNTGY
			AQKFVG RVTMTRDTSKTTAYLELSGLKSED
			TAVYYCARSSGSGGTWYKEYFQSWGQGTMV
			TVSS
TNF-Y7C VH	CDR-	Residues 31-35	NYDIN
	H1	of SEQ ID
		NO.: 28
TNF-Y7C VH	CDR-	Residues 50-66	WMDPNNGNTGYAQKFVG
	H2	of SEQ ID
		NO.: 28
TNF-Y7C VH	CDR-	Residues 99-112	KSSGSGGTWYKEYFQS
	H3	of SEQ ID
		NO.: 28
TNF-Y7C VL		29	DIVMTQSPLSLPVTPGEPASISCRSSQSLL
			HSNGYNYLD WYLQKPGQFPQLLIYLGSYRA
			S GVPDRFSGSGSGTDFTLKISRVEAEDVGV
			YYCMQRIEFPPGTFGQGTKLGIK
TNF-Y7C VL	CDR-	Residues 24-39	RSSQSLLHSNGYNYLD
	L1	of SEQ ID
		NO.: 29
TNF-Y7C VL	CDR-	Residues 55-61	LGSYRAS
	L2	of SEQ ID
		NO.: 29
TNF-Y7C VL	CDR-	Residues 94-103	MQRIEFPPGT
	L3	of SEQ ID
		NO.: 29
AE11-7 VH		30	EVQLVQSGAEVKKPGASVKVSCKTSGYSLT
			QYPIH WVRQAPGQRPEWMGWISPGNGNTKL
			SPKFQG RVTLSRDASAGTVFMDLSGLTSDD
			TAVYFCTSVDLGDHWGQGTLVTVSS
AE11-7 VH	CDR-	Residues 31-35	QYPIH
	H1	of SEQ ID
		NO.: 30
AE11-7 VH	CDR-	Residues 50-66	WISPGNGNTKLSPKFQG
	H2	of SEQ ID
		NO.: 30
AE11-7 VH	CDR-	Residues 99-104	VDLGDH
	H3	of SEQ ID
		NO.: 30
AE11-7 VL		31	DIVMTQSPEFQSVTPKEKVTITCRASQSIG
			SSLH WYQQKPDQSPKLLINYASQSFSGVPS
			RFSGGGSGTDFTLTINSLEAEDAATYYCHQ
			SSNLPIT FGQGTRLEIK
AE11-7 VL	CDR-	Residues 24-34	RASQSIGSSLH
	L1	of SEQ ID
		NO.: 31
AE11-7 VL	CDR-	Residues 50-56	YASQSFS
	L2	of SEQ ID
		NO.: 31
AE11-7 VL	CDR-	Residues 89-97	HQSSNLPIT
	L3	of SEQ ID
		NO.: 31
AE11-13 VH		32	EVQLVESGGGLVQPGRSLRLSCAASGFTFD
			DYPMH WVRQAPGEGLEWVSGISSNSASIGY
			ADSVKG RFTISRDNAQNTLYLQMNSLGDED
			TAVYYCVSLTLGIGQGTLVTVSS
AE11-13 VH	CDR-	Residues 31-35	DYPMH
	H1	of SEQ ID
		NO.: 32
AE11-13 VH	CDR-	Residues 50-66	GISSNSASIGYADSVKG
	H2	of SEQ ID
		NO.: 32
AE11-13 VH	CDR-	Residues 99-102	LTLG
	H3	of SEQ ID
		NO.: 32
AE11-13 VL		33	DIRLTQSPSSLSASVGDRVTITCRASQSIG
			NYLH WYQQKPGKAPKLLIYAASSLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			SYSTLYS FGQGTKLEIK
AE11-13 VL	CDR-	Residues 24-34	RASQSIGNYLH
	L1	of SEQ ID
		NO.: 33
AE11-13 VL	CDR-	Residues 50-56	AASSLQS
	L2	of SEQ ID
		NO.: 33
AE11-13 VL	CDR-	Residues 89-97	QQSYSTLYS
	L3	of SEQ ID
		NO.: 33

1.2: Affinity Maturation of the Fully Human Anti-Human TNF Antibody AE11-5

The AE11-5 human antibody to human TNF was affinity matured by in vitro display technology. One light chain library was constructed to contain limited mutagenesis at the following residues: 28, 31, 32, 51, 55, 91, 92, 93, 95a and 96 (Kabat numbering). This library also contained framework germline back-mutations D1E, M4L, H11Q, R49K, H76N and Q103K as well as toggled residues at position 50(R/K) and 94(S/L) to allow for framework germlining during library selections. Two heavy chain libraries were made to contain limited mutagenesis in CDRH1 and CDRH2 at residues 30, 31, 33, 50, 52, and 55 to 58 (Kabat numbering) or in CDRH3 at residues 95 to 100b. The library containing CDRH1 and CDRH2 diversities also had framework germline back-mutations A18V and L64Q and toggled residue at 54(L/F) and 78(V/A). The CDRH3 library has an additional toggled residue at 100c(A/F).

All three libraries were selected separately for the ability to bind human or cynomolgus monkey TNF in the presence of decreasing concentrations of biotinylated human or cynomolgus monkey TNF antigens. All mutated CDR sequences recovered from library selections were recombined into additional libraries and the recombined libraries were subjected to more stringent selection conditions before individual antibodies are identified.

Table 11 provides a list of amino acid sequences of VH regions of affinity matured fully human TNF antibodies derived from AE11-5 Amino acid residues of individual CDRs of each VH sequence are indicated in bold.

TABLE 11
List of amino acid sequences of affinity matured
AE11-5 VH variants
	SEQ
	ID
Clone	NO:	VH
J685M2S2-	94	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
10VH		ISWVRQAPGQGLEWMGGITPILGSANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	95	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSYYS
12VH		ISWVRQAPGQGLEWMGGIMPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	96	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
13VH		ISWVRQAPGQGLEWMGGIIPILGSPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	97	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
14VH		ISWVRQAPGQGLEWMGGIIPILGSPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	98	EVQLVQSGAEVKKPGSSVKVSCKASGGTFAWYS
16VH		ISWVRQAPGQGLEWMGGITPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	99	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSFYA
18VH		ISWVRQAPGQGLEWMGGITPILGAATYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	100	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYA
1VH		ISWVRQAPGQGLEWMGGITPILGAAVYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	101	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
21VH		ISWVRQAPGQGLEWMGGIMPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	102	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
23VH		ISWVRQAPGQGLEWMGGITPILGVAVYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	103	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
25VH		ISWVRQAPGQGLEWMGGITPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	104	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
27VH		ISWVRQAPGQGLEWMGGITPILGSAHYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	105	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
28VH		ISWVRQAPGQGLEWMGGITPILGSAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	106	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
29VH		ISWVRQAPGQGLEWMGGITPILGTAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	107	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYT
31VH		ISWVRQAPGQGLEWMGGIIPILRNPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	108	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSYYA
32VH		ISWVRQAPGQGLEWMGGIMPILGTPTYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	109	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYT
35VH		ISWVRQAPGQGLEWMGGIIPILGAPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	110	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
37VH		ISWVRQAPGQGLEWMGGITPILGSATYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	111	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYS
38VH		ISWVRQAPGQGLEWMGGIMPILGSASYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	112	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
43VH		ISWVRQAPGQGLEWMGGIMPILGTASYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	113	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYS
44VH		ISWVRQAPGQGLEWMGGITPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	114	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
45VH		ISWVRQAPGQGLEWMGGIMPILGTATYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	115	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSFYT
46VH		ISWVRQAPGQGLEWMGGIMPILGSPHYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	116	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
47VH		ISWVRQAPGQGLEWMGGITPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	117	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
48VH		ISWVRQAPGQGLEWMGGIMPILGSATYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	118	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
4VH		ISWVRQAPGQGLEWMGGIIPILGTPTYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	119	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
50VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J685M2S2-	120	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSLYT
51VH		ISWVRQAPGQGLEWMGGIMPILGAPRYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	121	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSYYA
52VH		ISWVRQAPGQGLEWMGGIMPILGSPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	122	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYA
53VH		ISWVRQAPGQGLEWMGGILPILGSPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	123	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYA
55VH		ISWVRQAPGQGLEWMGGIIPILGSPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	124	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
56VH		ISWVRQAPGQGLEWMGGIVPILGAPLYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	125	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYA
58VH		ISWVRQAPGQGLEWMGGIMPILGAPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	126	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSYYT
5VH		ISWVRQAPGQGLEWMGGIMPILGTPAYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	127	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYS
61VH		ISWVRQAPGQGLEWMGGITPILGAATYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	128	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
62VH		ISWVRQAPGQGLEWMGGIIPILGTPTYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	129	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
63VH		ISWVRQAPGQGLEWMGGIIPILGTPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	130	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
64VH		ISWVRQAPGQGLEWMGGITPILGIGNYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	131	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYA
66VH		ISWVRQAPGQGLEWMGGIVPILGAATYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	132	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
67VH		ISWVRQAPGQGLEWMGGITPILGSSTYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	133	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
68VH		ISWVRQAPGQGLEWMGGIMPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	134	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
6VH		ISWVRQAPGQGLEWMGGITPILGNSIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	135	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
70VH		ISWVRQAPGQGLEWMGGITPILGSPIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	136	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
71VH		ISWVRQAPGQGLEWMGGIMPILGTPTYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	137	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSYYA
72VH		ISWVRQAPGQGLEWMGGITPILGAANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	138	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
73VH		ISWVRQAPGQGLEWMGGITPILGAAIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	139	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
75VH		ISWVRQAPGQGLEWMGGITPILGTATYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	140	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYS
76VH		ISWVRQAPGQGLEWMGGITPILGSAHYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	141	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
77VH		ISWVRQAPGQGLEWMGGITPILGNAIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	142	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
78VH		ISWVRQAPGQGLEWMGGITPILRSAVYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	143	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYS
7VH		ISWVRQAPGQGLEWMGGIMPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	144	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
80VH		ISWVRQAPGQGLEWMGGITPILGTASYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	145	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
81VH		ISWVRQAPGQGLEWMGGITPILGTAIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	146	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
82VH		ISWVRQAPGQGLEWMGGITPILGSPAYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	147	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSRYA
83VH		ISWVRQAPGQGLEWMGGIIPILGPASYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	148	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
84VH		ISWVRQAPGQGLEWMGGITPILDAAIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	149	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
86VH		ISWVRQAPGQGLEWMGGIMPILGIPNYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	150	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYA
87VH		ISWVRQAPGQGLEWMGGITPILGSAIYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	151	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSYYA
88VH		ISWVRQAPGQGLEWMGGIMPILGTATYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	152	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
89VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYFDPKRADYWGQGTLVTVSS
J685M2S2-	153	EVQLVQSGAEVKKPGSSVKVSCKASGGTFNWYT
8VH		ISWVRQAPGQGLEWMGGIMPILGTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	154	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
90VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYFDFTRADYWGQGTLVTVSS
J685M2S2-	155	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
91VH		ISWVRQAPGQGLEWMGGIIPILRFPTYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	156	EVQLVQSGAEVKKPGSSVKVSCKVSGGTFSWYS
92VH		ISWVRQAPGQGLEWMGGILPILDTANYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	157	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
93VH		ISWVRQAPGQGLEWMGGIMPILGTAVYAQKFQG
		RVTITADESTSTAYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J685M2S2-	158	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSIYS
94VH		ISWVRQAPGQGLEWMGGILPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J688M2-11VH	159	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPTRADYWGQGTLVTVSS
J688M2-13VH	160	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPSRADYWGQGTLVTVSS
J688M2-14VH	161	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYFNPTRADYWGQGTLVTVSS
J688M2-16VH	162	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPARFDYWGQGTLVTVSS
J688M2-20VH	163	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYNPSRADYWGQGTLVTVSS
J688M2-21VH	164	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPKRADYWGQGTLVTVSS
J688M2-22VH	165	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPRRADYWGQGTLVTVSS
J688M2-28VH	166	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		FYYDPTRADYWGQGTLVTVSS
J688M2-29VH	167	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDFTRADYWGQGTLVTVSS
J688M2-2VH	168	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYFDPKRADYWGQGTLVTVSS
J688M2-37VH	169	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYFDPTRADYWGQGTLVTVSS
J688M2-3VH	170	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPSRADYWGQGTLVTVSS
J688M2-46VH	171	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARS
		LYYERTRADYWGQGTLVTVSS
J688M2-48VH	172	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARW
		RFYIPIRFDYWGQGTLVTVSS
J688M2-4VH	173	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDFTRADYWGQGTLVTVSS
J688M2-50VH	174	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LFYDPSRADYWGQGTLVTVSS
J688M2-52VH	175	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPVRADYWGQGTLVTVSS
J688M2-56VH	176	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPIRADYWGQGTLVTVSS
J688M2-57VH	177	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J688M2-58VH	178	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYNPIRFDYWGQGTLVTVSS
J688M2-64VH	179	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYFDPARADYWGQGTLVTVSS
J688M2-65VH	180	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VFFDPTRADYWGQGTLVTVSS
J688M2-68VH	181	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VFYNPTRADYWGQGTLVTVSS
J688M2-69VH	182	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYEGPSADYWGQGTLVTVSS
J688M2-6VH	183	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYAPNRADYWGQGTLVTVSS
J688M2-73VH	184	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LFYDPTRADYWGQGTLVTVSS
J688M2-74VH	185	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYNPTRADYWGQGTLVTVSS
J688M2-75VH	186	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPARADYWGQGTLVTVSS
J688M2-7VH	187	EVQLVQSGAEVKKSGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPGRADYWGQGTLVTVSS
J688M2-81VH	188	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYFDPSRADYWGQGTLVTVSS
J688M2-82VH	189	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYFDPSRFDYWGQGTLVTVSS
J688M2-83VH	190	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYFDFTRADYWGQGTLVTVSS
J688M2-84VH	191	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPTRADYWGQGTLVTVSS
J688M2-88VH	192	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYFDPSRADYWGQGTLVTVSS
J688M2-89VH	193	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPSRFDYWGQGTLVTVSS
J688M2-8VH	194	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		QYYDTSRADYWGQGTLVTVSS
J688M2-90VH	195	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARS
		LYYDTTRFDYWGQGTLVTVSS
J688M2-92VH	196	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VFYDPTRADYWGQGTLVTVSS
J688M2-94VH	197	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPARADYWGQGTLVTVSS
J688M2-95VH	198	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LFYDPRRADYWGQGTLVTVSS
J688M2-96VH	199	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDTTRADYWGQGTLVTVSS
J693FRM2S-	200	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
2L-32VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPARADYWGQGTLVTVSS
J693FRM2S-	201	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
2L-40VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCSRG
		LYYDPTRADYWGQGTLVTVSS
J693FRM2S-	202	EVQLVQSGAEVMKPGSSVKVSCKASGGTFSSYA
2L-70VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCTRG
		LYYDPTRADYWGQGTLVTVSS
J693FRM2-S	203	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYA
2R-29VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693FRM2S-	204	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
2R-46VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCTRG
		LYYDPTRADYWGQGTLVTVSS
J693FRM2S-	205	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
2R-65VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCTRG
		IYYDPTRADYWGQGTLVTVSS
J693M2S2L-	206	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
17VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQEFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2L-	207	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
32VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCVRG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2L-	208	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
67VH		ISWVRQAPGQGLEWMGGIIPILGTASYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2L-	209	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
75VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCAKG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2L-	210	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
78VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCERG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2L-	211	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSNYA
79VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2L-	212	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
94VH		ISWVRQAPGQGLEWMGGIIPILGTANYAHKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2R-	213	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
22VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADCWGQGTLVTVSS
J693M2S2R-	214	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
24VH		ISWVQQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2R-	215	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
2VH		ISWVRQAPGQGLEWMGGITPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2R-	216	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
31VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2R-	217	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
71VH		TSWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2R-	218	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSSYA
84VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFLG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J693M2S2R-	219	EVQLVQSGAEVKKPGSSVKVSCKASGGTSSSYA
89VH		ISWVRQAPGQGLEWMGGIIPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPTRADYWGQGTLVTVSS
J703M1S3-	220	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
10VH		ISWVRQAPGQGLEWMGGITPILGSATYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPKRADYWGQGTLVTVSS
J703M1S3-	221	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
11VH		ISWVRQAPGQGLEWMGGITPILGAASYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPTRADYWGQGTLVTVSS
J703M1S3-	222	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
12VH		ISWVRQAPGQGLEWMGGITPILGAASYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPARADYWGQGTLVTVSS
J703M1S3-	223	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
13VH		ISWVRQAPGQGLEWMGGITPILGAANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	224	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
14VH		ISWVRQAPGQGLEWMGGIMPILGSPTYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPRRADYWGQGTLVTVSS
J703M1S3-	225	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
16VH		ISWVRQAPGQGLEWMGGITPILGSATYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	226	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
17VH		ISWVRQAPGQGLEWMGGIVPILGTPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	227	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
18VH		ISWVRQAPGQGLEWMGGITPILGSANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPARADYWGQGTLVTVSS
J703M1S3-	228	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
19VH		ISWVRQAPGQGLEWMGGITPILGSPTYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	229	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
1VH		ISWVRQAPGQGLEWMGGIMPILGTPVYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDFRRANYWGQGTLVTVSS
J703M1S3-	230	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
20VH		ISWVRQAPGQGLEWMGGITPILGAATYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	231	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
21VH		ISWVRQAPGQGLEWMGGITPILGDPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	232	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
22VH		ISWVRQAPGQGLEWMGGITPILGNPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDYKRADYWGQGTLVTVSS
J703M1S3-	233	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
25VH		ISWVRQAPGQGLEWMGGITPILGSANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LFYDFRRADYWGQGTLVTVSS
J703M1S3-	234	EVQLVQSGAEVKKPGSSVKVSCKASGGTFAWYA
28VH		ISWVRQAPGQGLEWMGGITPILGNAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	235	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
29VH		ISWVRQAPGQGLEWMGGITPILGNPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	236	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
2VH		TSWVRQAPGQGLEWMGGITPILGSPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDHRRADYWGQGTLVTVSS
J703M1S3-	237	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
34VH		ISWVRQAPGQGLEWMGGITPILGSPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDYKRADYWGQGTLVTVSS
J703M1S3-	238	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
37VH		ISWVRQAPGQGLEWMGGITPILGSAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	239	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
38VH		ISWVRQAPGQGLEWMGGITPILGTPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDFKRADYWGQGTLVTVSS
J703M1S3-	240	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
3VH		ISWVRQAPGQGLEWMGGIMPILGTPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPRRADYWGQGTLVTVSS
J703M1S3-	241	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
41VH		ISWVRQAPGQGLEWMGGITPILGSANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	242	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
42VH		ISWVRQAPGQGLEWMGGITPILGAPVYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	243	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
45VH		ISWVRQAPGQGLEWMGGITPILGSAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	244	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
46VH		ISWVRQAPGQGLEWMGGITPILGSPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	245	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
47VH		ISWVRQAPGQGLEWMGGIMPILGSANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	246	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
4VH		ISWVRQAPGQGLEWMGGITPILGNAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	247	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
50VH		ISWVRQAPGQGLEWMGGITPILGAATYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	248	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
51VH		ISWVRQAPGQGLEWMGGITPILGSPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDYRRADYWGQGTLVTVSS
J703M1S3-	249	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
53VH		ISWVRQAPGQGLEWMGGIMPILGIPTYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPARADYWGQGTLVTVSS
J703M1S3-	250	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
54VH		ISWVRQAPGQGLEWMGGITPILGSPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	251	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
57VH		ISWVRQAPGQGLEWMGGITPILGSAVYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	252	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
5VH		ISWVRQAPGQGLEWMGGITPILGSAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDYKRADYWGQGTLVTVSS
J703M1S3-	253	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
62VH		ISWVRQAPGQGLEWMGGITPILGYPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	254	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
6VH		ISWVRQAPGQGLEWMGGITPILGAATYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDFRRADYWGQGTLVTVSS
J703M1S3-	255	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYP
72VH		ISWVRQAPGQGLEWMGGITPILGSAIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDFRRADYWGQGTLVTVSS
J703M1S3-	256	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
78VH		ISWVRQAPGQGLEWMGGITPILGTANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	257	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
79VH		ISWVRQAPGQGLEWMGGITPILGSAVYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	258	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
7VH		ISWVRQAPGQGLEWMGGITPILGNPIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPARADYWGQGTLVTVSS
J703M1S3-	259	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
81VH		ISWVRQAPGQGLEWMGGIMPILGAPNYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDYTRADYWGQGTLVTVSS
J703M1S3-	260	EVQLVQSGAEVKKPGSSVKVSCKASGGTFAWYA
83VH		ISWVRQAPGQGLEWMGGITPILGSPTYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	261	EVQLVQSGAEVKKPGSSVKVSCKASGGTFGWYA
86VH		TSWVRQAPGQGLEWMGGIIPILGTPNYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	262	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
87VH		ISWVRQAPGQGLEWMGGIMPILGTPTYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDPKRADYWGQGTLVTVSS
J703M1S3-	263	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYT
88VH		ISWVRQAPGQGLEWMGGIMPILGSPNYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		IYYDPKRADYWGQGTLVTVSS
J703M1S3-	264	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
91VH		ISWVRQAPGQGLEWMGGIMPILGSATYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYFDPKRADYWGQGTLVTVSS
J703M1S3-	265	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYA
93VH		ISWVRQAPGQGLEWMGGITPILGAANYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		LYYDPKRADYWGQGTLVTVSS
J703M1S3-	266	EVQLVQSGAEVKKPGSSVKVSCKASGGTFSWYP
9VH		ISWVRQAPGQGLEWMGGITPILGAGIYAQKFQG
		RVTITADESTSTVYMELSSLRSEDTAVYYCARG
		VYYDFKRADYWGQGTLVTVSS

Table 12 provides a list of amino acid sequences of VL regions of affinity matured fully human TNF antibodies derived from AE11-5 Amino acid residues of individual CDRs of each VH sequence are indicated in bold.

TABLE 12
List of amino acid sequences of affinity
matured AE11-5 VL variants
	SEQ
	ID
Clone	NO:	VL
J685M2S2-17Vk	267	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPPPTF
		GQGTKVEIK
J685M2S2-94Vk	268	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPPPTF
		GQWTKVEIK
J688M2-37Vk	269	EIVLTQSPDFQSVTPKEKVTITCRARQSIGSSL
		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTNFTLTINSLEAEDAATYYCHQSSSSPPPTF
		GQGTKVEIK
J688M2-90Vk	270	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPPPTF
		GQGTKVEIK
J693FRM2S2L-	271	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
26Vk		HWYQQKPDQSPKLLIKHASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNRSSPPSTF
		GQGTKVEIK
J693FRM2S2L-	272	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
27Vk		HWYQQKPDQSPKLLIKYASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPPVTF
		GQGTKVEIK
J693FRM2S2L-	273	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
29Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSNLPAPTF
		GQGTKVEIK
J693FRM2S2L-	274	EIVLTQSPDFQSVTPKEKVTITCRASQIIGGSL
39Vk		HWYQQKPDQSPKLLIKYASQSFSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQPICSPPRTF
		GQGTKVEIK
J693FRM2S2L-	275	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSNL
3Vk		HWYQQKPDQSPKLLIKYASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSISPPATF
		GQGTKVEIK
J693FRM2S2L-	276	EIVLTQSPDFQSVTPKEKVTITCRASQCIGTSL
40Vk		HWYQQKPDQSPKLLIKYDSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSSPPPTF
		GQGTKVEIK
J693FRM2S2L-	277	EIVLTQSPDFQSVTPKEKVTITCRASQNIGNSL
42Vk		HWYQQKPDQSPKLLIKYTSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTSSLPLPTF
		GQGTKVEIK
J693FRM2S2L-	278	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
43Vk		HWYQQKPDQSPKLLIKYVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQISDLPTSTF
		GQGTKVEIK
J693FRM2S2L-	279	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSNL
45Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSSLPPPTF
		GQGTKVEIK
J693FRM2S2L-	280	EIVLTQSPDFQSVTPKEKVTITCRASQCIGSSL
46Vk		HWYQQKPDQSPKLLIKHTSQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSNSSPLSTF
		GQGTKVEIK
J693FRM2S2L-	281	EIVLTQSPDFQSVTPKEKVTITCRASQNIGGSL
47Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSLPLPTF
		GQGTKVEIK
J693FRM2S2L-	282	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
48Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSKSPPPTF
		GQGTKVEIK
J693FRM2S2L-	283	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSCL
52Vk		HWYQQKPDQSPKLLIKYASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSSLPTPTF
		GQGTKVEIK
J693FRM2S2L-	284	EIVLTQSPDFQSVTPKEKVTITCRASQSIGGRL
53Vk		HWYQQKPDQSPKLLIKYASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQASSSPSTTF
		GQGTKVEIK
J693FRM2S2L-	285	EIVLTQSPDFQSVTPKEKVTITCRASQRIGPSL
54Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSCLPSTTF
		GQGTKVEIK
J693FRM2S2L-	286	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
58Vk		HWYQQKPDQSPKLLIKYASQSRSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGISPPTTF
		GQGTKVEIK
J693FRM2S2L-	287	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTSL
59Vk		HWYQQKPDQSPKLLIKYVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGMSSPAPTF
		GQGTKVEIK
J693FRM2S2L-	288	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
5Vk		HWYQQKPDQSPKLLIKYASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRRNSPPPTF
		GQGTKVEIK
J693FRM2S2L-	289	EIVLTQSPDFQSVTPKEKVTITCRASQKIGSGL
88Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNNSSPHKTF
		GQGTKVEIK
J693FRM2S2L-	290	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSNL
89Vk		HWYQQKPDQSPKLLIKHSSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSSPLPTF
		GQGTKVEIK
J693FRM2S2L-	291	EIVLTQSPDFQSVTPKEKVTITCRASQNIGRSL
8Vk		HWYQQKPDQSPKLLIKYASQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRSSPPPTF
		GQGTKVEIK
J693FRM2S2L-	292	EIVLTQSPDFQSVTPKEKVTITCRASQCIGKSL
90Vk		HWYQQKPDQSPKLLIKHPSQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSIGLPPTTF
		GQGTKVEIK
J693FRM2S2L-	293	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSSL
91Vk		HWYQQKPDQSPKLLIKHASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSISPPATF
		GQGTKVEIK
J693FRM2S2L-	294	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSTL
92Vk		HWYQQKPDQSPKLLIKYESQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRCCSPTQTF
		GQGTKVEIK
J693FRM2S2L-	295	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRKL
94Vk		HWYQQKPDQSPKLLIKYSSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSRSPPTTF
		GQGTKVEIK
J693FRM2S2R-	296	EIVLTQSPDFQSVTPKEKVTITCRASQTIGTSL
10Vk		HWYQQKPDQSPKLLIKHASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPSPTF
		GQGTKVEIK
J693FRM2S2R-	297	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
11Vk		HWYQQKPDQSPKLLIKHVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRGSSPPRTF
		GQGTKVEIK
J693FRM2S2R-	298	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSTL
12Vk		HWYQQKPDQSPKLLIKHTSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSSSPPPTF
		GQGTKVEIK
J693FRM2S2R-	299	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSNL
14Vk		HWYQQKPDQSPKLLIKHGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRHSSPRATF
		GQGTKVEIK
J693FRM2S2R-	300	EIVLTQSPDFQSVTPKEKVTITCRASQKIGSNL
15Vk		HWYQQKPDQSPKLLIKYASQSFSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSSPPATF
		GQGTKVEIK
J693FRM2S2R-	301	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
16Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSRSPFRTF
		GQGTKVEIK
J693FRM2S2R-	302	EIVLTQSPDFQSVTPKEKVTITCRASQCIGRRL
34Vk		HWYQQKPDQSPKLLIKHASQSRSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCTSSPPPTF
		GQGTKVEIK
J693FRM2S2R-	303	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSNL
36Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSLRLPPQTF
		GQGTKVEIK
J693FRM2S2R-	304	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
39Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNRSLPRLTF
		GQGTKVEIK
J693FRM2S2R-	305	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSCL
3Vk		HWYQQKPDQSPKLLIKYASQSISGVPSSSVASG
		SGTDFTLTINSLEAEDAATYYCHQRSSLPQPTF
		GQGTKVEIK
J693FRM2S2R-	306	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRRL
42Vk		HWYQQKPDQSPKLLIKHPSQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSIDSPPPTF
		GQGTKVEIK
J693FRM2S2R-	307	EIVLTQSPDFQSVTPKEKVTITCRASQTIGRSL
45Vk		HWYQQKPDQSPKLLIKYKSQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRWGLPMPTF
		GQGTKVEIK
J693FRM2S2R-	308	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSML
48Vk		HWYQQKPDQSPKLLIKHSSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTNSLPPRTF
		GQGTKVEIK
J693FRM2S2R-	309	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
50Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSRSPLDTF
		GQGTKVEIK
J693FRM2S2R-	310	EIVLTQSPDFQSVTPKEKVTITCRASQSIGCSL
51Vk		HWYQQKPDQSPKLLIKYASQSVSVVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSTLPPPTF
		GQGTKVEIK
J693FRM2S2R-	311	EIVLTQSPDFQSVTPKEKVTITCRASQGIGTSL
52Vk		HWYQQKPDQSPKLLIKHDSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTSSLPPPTF
		GQGTKVEIK
J693FRM2S2R-	312	EIVLTQSPDFQSVTPKEKVTITCRASQIIGSSL
56Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPLPTF
		GQGTKVEIK
J693FRM2S2R-	313	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
58Vk		HWYQQKPDQSPKLLIKYTSQSKSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGNRSPSTTF
		GQGTKVEIK
J693FRM2S2R-	314	EIVLTQSPDFQSVTPKEKVTITCRASKRIGSSL
59Vk		HWYQQKPDQSPKLLIKHKSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSASPPPTF
		GQGTKVEIK
J693FRM2S2R-	315	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSSL
5Vk		HWYQQKPDQSPKLLIKHPSQSMSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSTSPPATF
		GQGTKVEIK
J693FRM2S2R-	316	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
60Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSSLPTPTF
		GQGTKVEIK
J693FRM2S2R-	317	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSTL
61Vk		HWYQQKPDQSPKLLIKHASQSFSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSNCSPAHTF
		GQGTKVEIK
J693FRM2S2R-	318	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSRL
62Vk		HWYQQKPDQSPKLLIKYVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSRLPPPTF
		GQGTKVEIK
J693FRM2S2R-	319	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSTL
63Vk		HWYQQKPDQSPKLLIKHASQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSCSPQATF
		GQGTKVEIK
J693FRM2S2R-	320	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTSL
64Vk		HWYQQKPDQSPKLLIKYPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGRSPPHTF
		GQGTKVEIK
J693FRM2S2R-	321	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
65Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSILPPPTF
		GQGTKVEIK
J693FRM2S2R-	322	EIVLTQSPDFQSVTPKEKVTITCRASQCIGSYL
92Vk		HWYQQKPDQSPKLLIKHVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPTLTF
		GQGTKVEIK
J693FRM2S2R-	323	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
93Vk		HWYQQKPDQSPKLLIKHASQSMSGVPSGFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTNRSPPPTF
		GQGTKVEIK
J693FRM2S2R-	324	EIVLTQSPDFQSVTPKEKVTITCRASQNIGTSL
9Vk		HWYQQKPDQSPKLLIKYVSQSISGVPSRFSGSG
		SGTDFTLNINSLEAEDAATYYCHQSSCLPRPTF
		GQGTKVEIK
J693M2S2L-	325	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSPL
10Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSSSPPPTF
		GQGTKVEIK
J693M2S2L-	326	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSTL
11Vk		HWYQQKPDQSPKLLIKHDSQSKSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSDSPAPTF
		GQGTKVEIK
J693M2S2L-	327	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSCL
12Vk		HWYQQKPDQSPKLLIKHASQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRISPLPTF
		GQGTKVEIK
J693M2S2L-	328	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRRL
13Vk		HWYQQKPDQSPKLLIKHSSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSSLPHPTF
		GQGTKVEIK
J693M2S2L-	329	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSRL
14Vk		HWYQQKPDQSPKLLIKHASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSCSSPLVTF
		GQGTKVEIK
J693M2S2L-	330	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
16Vk		HWYQQKPDQSPKLLIKHASQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGSSPQATF
		GQGTKVEIK
J693M2S2L-	331	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
17Vk		HWYQQKPDQSPKLLIKHASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNRGSPPQTF
		GQGTKVEIK
J693M2S2L-	332	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSIL
18Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNTSLPPPTF
		GQGTKVEIK
J693M2S2L-	333	EIVLTQSPDFQSVTPKEKVTITCRASQSIGNSL
19Vk		HWYQQKPDQSPKLLIKYPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSRLPVPTF
		GQGTKVEIK
J693M2S2L-1Vk	334	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
		HWYQQKPDQSPKLLIKHTSQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPAPTF
		GQGTKVEIK
J693M2S2L-	335	EIVLTQSPDFQSVTPKEKVTITCRASQNIGSSL
20Vk		HWYQQKPDQSPKLLIKHVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSNSLPAPTF
		GQGTKVEIK
J693M2S2L-	336	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
21Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSMSLPSATF
		GQGTKVEIK
J693M2S2L-	337	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
22Vk		HWYQQKPDQSPKLLIKHLSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQPCRLPPSTF
		GQGTKVEIK
J693M2S2L-	338	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSLL
23Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSCSSPRHTF
		GQGTKVEIK
J693M2S2L-	339	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
24Vk		HWYQQKPDQSPKLLIKHPSQSKSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSRSPAPTF
		GQGTKVEIK
J693M2S2L-	340	EIVLTQSPDFQSVTPKEKVTITCRASQSIGGSL
25Vk		HWYQQKPDQSPKLLIKYSSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSILPSLTF
		GQGTKVEIK
J693M2S2L-	341	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
26Vk		HWYQQKPDQSPKLLIKHPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRNLPPRTF
		GQGTKVEIK
J693M2S2L-	342	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSIL
27Vk		HWYQQKPDQSPKLLIKYGSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNGSSPPRTF
		GQGTKVEIK
J693M2S2L-	343	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
28Vk		HWYQQKPDQSPKLLIKYFSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSCLPMQTF
		GQGTKVEIK
J693M2S2L-	344	EIVLTQSPDFQSVTPKEKVTITCRASQNIGSSL
29Vk		HWYQQKPDQSPKLLIKYSSQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSISPPATF
		GQGTKVEIK
J693M2S2L-2Vk	345	EIVLTQSPDFQSVTPKEKVTITCRASQCIGSSL
		HWYQQKPDQSPKLLIKHASQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSTCLPPRTF
		GQGTKVEIK
J693M2S2L-	346	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
30Vk		HWYQQKPDQSPKLLIKYVSQSMSGVLSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQPSTSPRPTF
		GQGTKVEIK
J693M2S2L-	347	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
31Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSLPPSTF
		GQGTKVEIK
J693M2S2L-	348	EIVLTQSPDFQSVTPKEKVTITCRASQSIGCSL
32Vk		HWYQQKPDQSPKLLIKYASQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPSSTF
		GQGTKVEIK
J693M2S2L-	349	EIVLTQSPDFQSVTPKEKVTITCRASQIIGTSL
33Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSRSPPRTF
		GQGTKVEIK
J693M2S2L-	350	EIVLTQSPDFQSVTPKEKVTITCRASQKIGTSL
34Vk		HWYQQKPDQSPKLLIKHESQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSGSPPPTF
		GQGTKVEIK
J693M2S2L-	351	EIVLTQSPDFQSVTPKEKVTITCRASQTIGGSL
35Vk		HWYQQKPDQSPKLLIKHVSQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSISPPPTF
		GQGTKVEIK
J693M2S2L-	352	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSDL
36Vk		HWYQQKPDQSPKLLIKHVSQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSCMSPSLTF
		GQGTKVEIK
J693M2S2L-	353	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSNL
37Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPNTTF
		GQGTKVEIK
J693M2S2L-	354	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSIL
38Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGRISPSSTF
		GQGTKVEIK
J693M2S2L-	355	EIVLTQSPDFQSVTPKEKVTITCRASQSIGNRL
39Vk		HWYQQKPDQSPKLLIKHASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGSLPTLTF
		GQGTKVEIK
J693M2S2L-3Vk	356	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSSL
		HWYQQKPDQSPKLLIKHDSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSLPTHTF
		GQGTKVEIK
J693M2S2L-	357	EIVLTQSPDFQSVTPKEKVTITCRASQTIGRSL
40Vk		HWYQQKPDQSPKLLIKHGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRSSPPSTF
		GQGTKVEIK
J693M2S2L-	358	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
41Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNCSSPPPTF
		GQGTKVEIK
J693M2S2L-	359	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
44Vk		HWYQQKPDQSPKLLIKYESQSDSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRRNSPPSTF
		GQGTKVEIK
J693M2S2L-	360	EIVLTQSPDFQSVTPKEKVTITCRASQGIGSRL
45Vk		HWYQQKPDQSPKLLIKHGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNRGLPAPTF
		GQGTKVEIK
J693M2S2L-	361	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
46Vk		HWYQQKPDQSPKLLIKYASQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNHTSPPPTF
		GQGTKVEIK
J693M2S2L-	362	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
47Vk		HWYQQKPDQSPKLLIKHASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGRLPPPTF
		GQGTKVEIK
J693M2S2L-4Vk	363	EIVLTQSPDFQSVTPKEKVTITCRASQYIGKRL
		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSNISPPPTF
		GQGTKVEIK
J693M2S2L-	364	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
51Vk		HWYQQKPDQSPKLLIKHESQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPPPTF
		GQGTKVEIK
J693M2S2L-	365	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSSL
52Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSSLPPSTF
		GQGTKVEIK
J693M2S2L-	366	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
54Vk		HWYQQKPDQSPKLLIKHPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSSSPAQTF
		GQGTKVEIK
J693M2S2L-	367	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
55Vk		HWYQQKPDQSPKLLIKHTSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSSLPLPTF
		GQGTKVEIK
J693M2S2L-	368	EIVLTQSPDFQSVTPKEKVTITCRASQWIGSSL
56Vk		HWYQQKPDQSPKLLIKHTSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPPQTF
		GQGTKVEIK
J693M2S2L-	369	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
58Vk		HWYQQKPDQSPKLLIKYSSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSSSPPPTF
		GQGTKVEIK
J693M2S2L-	370	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
59Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSRLPPSTF
		GQGTKVEIK
J693M2S2L-5Vk	371	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKYGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNWSLPLPTF
		GQGTKVEIK
J693M2S2L-	372	EIVLTQSPDFQSVTPKEKVTITCRASQRIGTSL
62Vk		HWYQQKPDQSPKLLIKYASQSKSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSCSPTPTF
		GQGTKVEIK
J693M2S2L-	373	EIVLTQSPDFQSVTPKEKVTITCRASQSIGGSL
64Vk		HWYQQKPDQSPKLLIKYGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRCVSPSPTF
		GQGTKVEIK
J693M2S2L-	374	EIVLTQSPDFQSVTPKEKVTITCRASQSIGGTL
65Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPARTF
		GQGTKVEIK
J693M2S2L-	375	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
66Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCGSSPLHTF
		GQGTKVEIK
J693M2S2L-	376	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTSL
67Vk		HWYQQKPDQSPKLLIKHPSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSTSSPPPTF
		GQGTKVEIK
J693M2S2L-	377	EIVLTQSPDFQSVTPKEKVTITCRASQNIGSSL
68Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSGLPLPTF
		GQGTKVEIK
J693M2S2L-	378	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRRL
69Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSSSPSPTF
		GQGTKVEIK
J693M2S2L-6Vk	379	EIVLTQSPDFQSVTPKEKVTITCRASQRIGGNL
		HWYQQKPDQSPKLLIKHESQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPSHTF
		GQGTKVEIK
J693M2S2L-	380	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
70Vk		HWYQQKPDQSPKLLIKYASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSSSPSHTF
		GQGTKVEIK
J693M2S2L-	381	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
71Vk		HWYQQKPDQSPKLLIKHASQSMSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRNSPPTTF
		GQGTKVEIK
J693M2S2L-	382	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSRL
72Vk		HWYQQKPDQSPKLLIKHGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSSPPPTF
		GQGTKVEIK
J693M2S2L-	383	EIVLTQSPDFQSVTPKEKVTITCRASQNIGSSL
74Vk		HWYQQKPDQSPKLLIKYASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSLLPAPTF
		GQGTKVEIK
J693M2S2L-	384	EIVLTQSPDFQSVTPKEKVTITCRASQIIGTTL
75Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSNLPPSTF
		GQGTKVEIK
J693M2S2L-	385	EIVLTQSPDFQSVTPKEKVTITCRASQNIGGNL
76Vk		HWYQQKPDQSPKLLIKHASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSNLPPPTF
		GQGTKVEIK
J693M2S2L-	386	EIVLTQSPDFQSVTPKEKVTITCRASQGIGGSL
77Vk		HWYQQKPDQSPKLLIKYASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSACLPTRTF
		GQGTKVEIK
J693M2S2L-	387	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTSL
78Vk		HWYQQKPDQSPKLLIKYASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQIGSLPPPTF
		GQGTKVEIK
J693M2S2R-	388	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
13Vk		HWYQQKPDQSPKLLIKHASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSRLPPPTF
		GQGTKVEIK
J693M2S2R-	389	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
14Vk		HWYQQKPDQSPKLLIKHNSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSSSPPLTF
		GQGTKVEIK
J693M2S2R-	390	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRNL
15Vk		HWYQQKPDQSPKLLIKHVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSRSPPSTF
		GQGTKVEIK
J693M2S2R-	391	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
16Vk		HWYQQKPDQSPKLLIKHASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSSLPAPTF
		GQGTKVEIK
J693M2S2R-	392	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
17Vk		HWYQQKPDQSPKLLIKHASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSRLPPQTF
		GQGTKVEIK
J693M2S2R-	393	EIVLTQSPDFQSVTPKEKVTITCRASQCIGSRL
18Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRGRLPPRTF
		GQGTKVEIK
J693M2S2R-	394	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
19Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSTSLPRLTF
		GQGTKVEIK
J693M2S2R-	395	EIVLTQSPDFQSVTPKEKVTITCRASQIIGSSL
20Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRSSPQQTF
		GQGTKVEIK
J693M2S2R-	396	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSTL
21Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPPPTF
		GQGTKVEIK
J693M2S2R-	397	EIVLTQSPDFQSVTPKEKVTITCRASQSIGNSL
22Vk		HWYQQKPDQSPKLLIKHGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRRSSPRHTF
		GQGTKVEIK
J693M2S2R-	398	EIVLTQSPDFQSVTPKEKVTITCRASQRIGRRL
27Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSIGSPPLTF
		GQGTKVEIK
J693M2S2R-	399	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRGL
29Vk		HWYQQKPDQSPKLLIKYGSQSMSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPPPTF
		GQGTKVEIK
J693M2S2R-2Vk	400	EIVLTQSPDFQSVTPKEKVTITCRASQSIGCSL
		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCTSLPLPTF
		GQGTKVEIK
J693M2S2R-	401	EIVLTQSPDFQSVTPKEKVTITCRASQGIGSSL
30Vk		HWYQQKPDQSPKLLIKYVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSSLPTPTF
		GQGTKVEIK
J693M2S2R-	402	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTSL
31Vk		HWYQQKPDQSPKLLIKHASQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSRLPPLTF
		GQGTKVEIK
J693M2S2R-	403	EIVLTQSPDFQSVTPKEKVTITCRASQVIGGVL
32Vk		HWYQQKPDQSPKLLIKYTSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPRPTF
		GQGTKVEIK
J693M2S2R-	404	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
33Vk		HWYQQKPDQSPKLLIKHSSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSNSPHRTF
		GQGTKVEIK
J693M2S2R-	405	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRTL
36Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSISPQPTF
		GQGTKVEIK
J693M2S2R-	406	EIVLTQSPDFQSVTPKEKVTITCRASQRIGNTL
37Vk		HWYQQKPDQSPKLLIKYPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGSSPPPTF
		GQGTKVEIK
J693M2S2R-	407	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
39Vk		HWYQQKPDQSPKLLIKYISQSMSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSCGLPPPTF
		GQGTKVEIK
J693M2S2R-3Vk	408	EIVLTQSPDFQSVTPKEKVTITCRASQNIGTRL
		HWYQQKPDQSPKLLIKYGSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRISPPPTF
		GQGTKVEIK
J693M2S2R-	409	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSTL
40Vk		HWYQQKPDQSPKLLIKYVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSRLPPPTF
		GQGTKVEIK
J693M2S2R-	410	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
44Vk		HWYQQKPDQSPKLLIKYASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSNLPSPTF
		GQGTKVEIK
J693M2S2R-	411	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSNL
45Vk		HWYQQKPDQSPKLLIKHASQSMSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPRPTF
		GQGTKVEIK
J693M2S2R-	412	EIVLTQSPDFQSVTPKEKVTITCRASQIIGSSL
46Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSISSPSPTF
		GQGTKVEIK
J693M2S2R-	413	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
47Vk		HWYQQKPDQSPKLLIKYASQSFSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSNCLPPPTF
		GQGTKVEIK
J693M2S2R-	414	EIVLTQSPDFQSVTPKEKVTITCRASQSIGKSL
48Vk		HWYQQKPDQSPKLLIKHESQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQANSLPPPTF
		GQGTKVEIK
J693M2S2R-4Vk	415	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRRL
		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSSSPPSTF
		GQGTKVEIK
J693M2S2R-	416	EIVLTQSPDFQSVTPKEKVTITCRASQIIGHSL
52Vk		HWYQQKPDQSPKLLIKHASQSILGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSIKSPPATF
		GQGTKVEIK
J693M2S2R-	417	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTSL
54Vk		HWYQQKPDQSPKLLIKHTSQSKSGVPSRFSGSG
		SGTDFALTINSLEAEDAATYYCHQSSNSPRYTF
		GQGTKVEIK
J693M2S2R-	418	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
55Vk		HWYQQKPDQSPKLLIKHASQSHSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGGSPPWTF
		GQGTKVEIK
J693M2S2R-	419	EIVLTQSPDFQSVTPKEKVTITCRASQGIGRSL
56Vk		HWYQQKPDQSPKLLIKYASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSNRSPPPTF
		GQGTKVEIK
J693M2S2R-5Vk	420	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTTL
		HWYQQKPDQSPKLLIKHVSQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPHPTF
		GQGTKVEIK
J693M2S2R-	421	EIVLTQSPDFQSVTPKEKVTITCRASQIIGSSL
60Vk		HWYQQKPDQSPKLLIKYPSQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSWSSPLMTF
		GQGTKVEIK
J693M2S2R-	422	EIVLTQSPDFQSVTPKEKVTITCRASQSIGNTL
61Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPPPTF
		GQGTKVEIK
J693M2S2R-	423	EIVLTQSPDFQSVTPKEKVTITCRASQRIGICL
62Vk		HWYQQKPDQSPKLLIKYASQSMSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGFSLPPATF
		GQGTKVEIK
J693M2S2R-	424	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSCL
63Vk		HWYQQKPDQSPKLLIKYPSQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSCSPTTTF
		GQGTKVEIK
J693M2S2R-	425	EIVLTQSPDFQSVTPKEKVTITCRASQRIGNTL
64Vk		HWYQQKPDQSPKLLIKYPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGSSPPPTF
		GQGTKVEIK
J693M2S2R-	426	EIVLTQSPDFQSVTPKEKVTITCRASQTIGTSL
65Vk		HWYQQKPDQSPKLLIKYASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRCSLPPPTF
		GQGTKVEIK
J693M2S2R-	427	EIVLTQSPDFQSVTPKEKVTITCRASQSIGGSL
68Vk		HWYQQKPDQSPKLLIKYASQSHSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCRISPRPTF
		GQGTKVEIK
J693M2S2R-	428	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
69Vk		HWYQQKPDQSPKLLIKHPSQSKSGVPSRFSGSG
		SGTDFTLSINSLEAEDAATYYCHQTSRSPLHTF
		GQGTKVEIK
J693M2S2R-6Vk	429	EIVLTQSPDFQSVTPKEKVTITCRASQNIGKNL
		HWYQQKPDQSPKLLIKYPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRSSPLSTF
		GQGTKVEIK
J693M2S2R-	430	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
70Vk		HWYQQKPDQSPKLLIKYMSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRVLPPPTF
		GQGTKVEIK
J693M2S2R-	431	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
71Vk		HWYQQKPDQSPKLLIKYGSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSISPRRTF
		GQGTKVEIK
J693M2S2R-	432	EIVLTQSPDFQSVTPKEKVTITCRASQTIGRSL
72Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRKSSPTPTF
		GQGTKVEIK
J693M2S2R-	433	EIVLTQSPDFQSVTPKEKVTITCRASQRIGRQL
75Vk		HWYQQKPDQSPKLLIKHPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPPQTF
		GQGTKVEIK
J693M2S2R-	434	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
77Vk		HWYQQKPDQSPKLLIKHTSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQICRSPSPTF
		GQGTKVEIK
J693M2S2R-	435	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
78Vk		HWYQQKPDQSPKLLIKYASQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSGSPAPTF
		GQGTKVEIK
J693M2S2R-	436	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
79Vk		HWYQQKPDQSPKLLIKYSSQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQISSSPPPTF
		GQGTKVEIK
J693M2S2R-7Vk	437	EIVLTQSPDFQSVTPKEKVTITCRASQTIGNSL
		HWYQQKPDQSPKLLIKHASQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTMTSPPPTF
		GQGTKVEIK
J693M2S2R-	438	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
80Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRSSPSPTF
		GQGTKVEIK
J693M2S2R-	439	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
81Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRRWSPPPTF
		GQGTKVEIK
J693M2S2R-	440	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
82Vk		HWYQQKPDQSPKLLIKYASQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQISCLPLPTF
		GQGTKVEIK
J693M2S2R-	441	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
83Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSISLPPPTF
		GQGTKVEIK
J693M2S2R-	442	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRNL
84Vk		HWYQQKPDQSPKLLIKHTSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTSTLPPQTF
		GQGTKVEIK
J693M2S2R-	443	EIVLTQSPDFQSVTPKEKVTITCRASQSIGRSL
85Vk		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRNSPQPTF
		GQGTKVEIK
J693M2S2R-	444	EIVLTQSPDFQSVTPKEKVTITCRASQSIGTRL
86Vk		HWYQQKPDQSPKLLIKYVSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSHSPPPTF
		GQGTKVEIK
J693M2S2R-	445	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSCL
87Vk		HWYQQKPDQSPKLLIKHRSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQWSSSPPPTF
		GQGTKVEIK
J693M2S2R-	446	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
89Vk		HWYQQKPDQSPKLLIKHPSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTSGSPSHTF
		GQGTKVEIK
J693M2S2R-8Vk	447	EIVLTQSPDFQSVTPKEKVTITCRASQGIGSSL
		HWYQQKPDQSPKLLIKYESQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPPPTF
		GQGTKVEIK
J693M2S2R-	448	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
90Vk		HWYQQKPDQSPKLLIKHDSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSSSPPTTF
		GQGTKVEIK
J693M2S2R-	449	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSNL
91Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRISSPPSTF
		GQGTKVEIK
J693M2S2R-	450	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSSL
92Vk		HWYQQKPDQSPKLLIKHASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSCSSPPSTF
		GQGTKVEIK
J693M2S2R-	451	EIVLTQSPDFQSVTPKEKVTITCRASQTIGSSL
93Vk		HWYQQKPDQSPKLLIKYVSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTISSPLPTF
		GQGTKVEIK
J693M2S2R-	452	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
95Vk		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSCSPAHTF
		GQGTKVEIK
J703M1S3-11Vk	453	EIVLTQSPDFQSVTPKEKVTITCRDSRCIGSNL
		HWYQQKPDQSPKLLIKHASQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCSSSPPPTF
		GQGTKVEIK
J703M1S3-13Vk	454	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSTL
		HWYQQKPDQSPKLLIKHASQSNSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPPPTF
		GQGTKVEIK
J703M1S3-16Vk	455	EIVLTQSPDFQSVTPKEKVTITCRASQSIGDSL
		HWYQQKPDQSPKLLIKHASQSKSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGSTSPPRTF
		GQGTKVEIK
J703M1S3-19Vk	456	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHGSQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSWSSPIPTF
		GQGTKVEIK
J703M1S3-22Vk	457	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
		HWYQQKPDQSPKLLIKYASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSNLPSPTF
		GQGTKVEIK
J703M1S3-26Vk	458	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
		HWYQQKPDQSPKLLIKHASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSGSSPPRTF
		GQGTKVEIK
J703M1S3-29Vk	459	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRTSSPVRTF
		GQGTKVEIK
J703M1S3-2Vk	460	EIVLTQSPDFQSVTPKEKVTITCRASQSIGNTL
		HWYQQKPDQSPKLLIKHVSQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQKVSSPSPTF
		GQGTKVEIK
J703M1S3-30Vk	461	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
		HWYQQKPDQSPKLLIKHASQSVSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSRSSPPPTF
		GQGTKVEIK
J703M1S3-33Vk	462	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPPSTF
		GQGTKVEIK
J703M1S3-34Vk	463	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSSPSTTF
		GQGTKVEIK
J703M1S3-57Vk	464	EIVLTQSPDFQSVTPKEKVTITCRASQCIGSSL
		HWYQQKPDQSPKLLIKHESQSSSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRCTSPSPTF
		GQGTKVEIK
J703M1S3-5Vk	465	EIVLTQSPDFQSVTPKEKVTITCRASQRIGSSL
		HWYQQKPDQSPKLLIKHPSQSDSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNCSLPLPTF
		GQGTKVEIK
J703M1S3-62Vk	466	EIVLTQSPDFQSVTPKEKVTITCRASQCIGSSL
		HWYQQKPDQSPKLLIKHASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQGISSPPQTF
		GQGTKVEIK
J703M1S3-69Vk	467	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHVSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQRSSSPSPTF
		GQGTKVEIK
J703M1S3-71Vk	468	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHPSQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSIRLPPSTF
		GQGTKVEIK
J703M1S3-78Vk	469	EIVLTQSPDFQSVTPKEKVTITCRANQSIGGSL
		HWYQQKPDQSPKLLIKHASQSKSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQDSRSPTRTF
		GQGTKVEIK
J703M1S3-79Vk	470	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSGL
		HWYQQKPDQSPKLLIKHTSQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSLPHPTF
		GQGTKVEIK
J703M1S3-7Vk	471	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHASQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSSSPTPTF
		GQGTKVEIK
J703M1S3-81Vk	472	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSRL
		HWYQQKPDQSPKLLIKYPSQSRSGVPSRFSGSG
		SGTDLTLTINSLEAEDAATYYCHQNGSLPPPTF
		GQGTKVEIK
J703M1S3-82Vk	473	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSSL
		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSSPPPTF
		GQGTKVEIK
J703M1S3-86Vk	474	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSAL
		HWYQQKPDQSPKLLIKHASQSLSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQSSILPRPTF
		GQGTKVEIK
J703M1S3-90Vk	475	EIVLTQSPDFQSVTPKEKVTITCRASQSIGSNL
		HWYQQKPDQSPKLLIKHASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQTRTSPPLTF
		GQGTKVEIK
J703M1S3-93Vk	476	EIVLTQSPDFQSVTPKEKVTITCRASQKIGSSL
		HWYQQKPDQSPKLLIKYGSQSTSGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQCISLPTPTF
		GQGTKVEIK
J703M1S3-94Vk	477	EIVLTQSPDFQSVTPKEKVAITCRASQRIGSSL
		HWYQQKPDQSPKLLIKYASQSISGVPSRFSGSG
		SGTDFTLTINSLEAEDAATYYCHQNSSLPPPTF
		GQGTKVEIK

TABLE 13
Amino acid residues observed in affinity matured AE11-5 antibodies
AE11-5 Heavy chain variable region (SEQ ID NO: 1073)
AE11-5VH 1234567890123456789012345678901234567890123456789012a345678901
         EVQLVQSGAEVKKPGSSAKVSCKASGGTFSSYAISWVRQAPGQGLEWMGGIIPILGTANYAQ
         V           NW TTT              WT   FRSPI
         TY SV                M   TDAST
         GI P                 L   I NGS
         AN G                 V     P V
         F                   N     I H
         R                         V A
         L                         K R
         F M
         L
         234567890123456789012abc345678901234567890abc1234567890123
         KFLG              RVTITADESTSTVYMELSSLRSEDTAVYYCARGLYYDPTRADYWGQGTLVTVSS
         Q             A                   SVFFNTSWF
         WIVVEFASM
         TFP TRKP
         ARH IGRA
         Q  ADI
         Y
         V
         P
         N
         G
AE11-5 Light chain variable region (SEQ ID NO: 1074)
AE11-5VL 1234567890123456789012345678901234567890123456789012345678901
         DIVMTQSPDFHSVTPKEKVTITCRASQSIGSSLHWYQQKPDQSPKLLIRHASQSISGVPSR
         E  L      Q                R  RR                KYV   L
         T  TT                  P   V
         N  GN                  T   T
         I  NC                  G   S
         C  KG                  S   M
         G  CI                  E   N
         K  HK                  D   K
         Y  VM                      F
         W  PL                      R
         LY
         P
         V
         2345678901234567890123456789012345a67890123456a
         FSGSGSGTDFTLTIHSLEAEDAATYYCHQSSSSPPPTFGQGTQVEIK
         N              RRRL LS      K
         NGI  AR
         GIC  SL
         TCG  RT
         CNN  TA
         ITT  QQ
         MK  HH
         V
         M

TABLE 14
Individual VH sequences from converted clones
Protein		Sequence
region	SEQ ID NO:	123456789012345678901234567890
J703M1S3		478	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#2			WYATSWVRQAPGQGLEWMGGITPILGSPIY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGVYYDHRRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYATS
#2		of SEQ ID
VH		NO.: 478
J703M1S3	CDR-H2	Residues 50-66	GITPILGSPIYAQKFQG
#2		of SEQ ID
VH		NO.: 478
J703M1S3	CDR-H3	Residues 99-109	GVYYDHRRADY
#2		of SEQ ID
VH		NO.: 478
J703M1S3		479	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#13			WYAISWVRQAPGQGLEWMGGITPILGAANY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGVYYDPKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYAIS
#13		of SEQ ID
		NO.: 479
J703M1S3	CDR-H2	Residues 50-66	GITPILGAANYAQKFQG
#13		of SEQ ID
VH		NO.: 479
J703M1S3	CDR-H3	Residues 99-109	GVYYDPKRADY
#13		of SEQ ID
VH		NO.: 479
J703M1S3		480	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#26			WYAISWVRQAPGQGLEWMGGITPILGTANY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGVYYDPKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYAIS
#26		of SEQ ID
VH		NO.: 480
J703M1S3	CDR-H2	Residues 50-66	GITPILGTANYAQKFQG
#26		of SEQ ID
VH		NO.: 480
J703M1S3	CDR-H3	Residues 99-109	GVYYDPKRADY
#26		of SEQ ID
VH		NO.: 480
J703M1S3		481	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#30			WYAISWVRQAPGQGLEWMGGITPILGSPIY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGVYYDPKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYAIS
#30		of SEQ ID
VH		NO.: 481
J703M1S3	CDR-H2	Residues 50-66	GITPILGSPIYAQKFQG
#30		of SEQ ID
VH		NO.: 481
J703M1S3	CDR-H3	Residues 99-109	GVYYDPKRADY
#30		of SEQ ID
VH		NO.: 481
J703M1S3		482	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#33			WYPISWVRQAPGQGLEWMGGITPILGAGIY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGVYYDFKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYPIS
#33		of SEQ ID
VH		NO.: 482
J703M1S3	CDR-H2	Residues 50-66	GITPILGAGIYAQKFQG
#33		of SEQ ID
VH		NO.: 482
J703M1S3	CDR-H3	Residues 99-109	GVYYDFKRADY
#33		of SEQ ID
VH		NO.: 482
J703M1S3		483	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#35			WYAISWVRQAPGQGLEWMGGITPILGSATY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGIYYDPKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYAIS
#35		of SEQ ID
VH		NO.: 483
J703M1S3	CDR-H2	Residues 50-66	GITPILGSATYAQKFQG
#35		of SEQ ID
VH		NO.: 483
J703M1S3	CDR-H3	Residues 99-109	GIYYDPKRADY
#35		of SEQ ID
VH		NO.: 483
J703M1S3		484	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#38			WYAISWVRQAPGQGLEWMGGITPILGTPIY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGVYYDFKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYAIS
#38		of SEQ ID
VH		NO.: 484
J703M1S3	CDR-H2	Residues 50-66	GITPILGTPIYAQKFQG
#38		of SEQ ID
VH		NO.: 484
J703M1S3	CDR-H3	Residues 99-109	GVYYDFKRADY
#38		of SEQ ID
VH		NO.: 484
J703M1S3		485	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#69			WYAISWVRQAPGQGLEWMGGITPILGSPIY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGIYYDPKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYAIS
#69		of SEQ ID
VH		NO.: 485
J703M1S3	CDR-H2	Residues 50-66	GITPILGSPIYAQKFQG
#69		of SEQ ID
VH		NO.: 485
J703M1S3	CDR-H3	Residues 99-109	GIYYDPKRADY
#69		of SEQ ID
VH		NO.: 485
J703M1S3		486	EVQLVQSGAEVKKPGSSVKVSCKASGGTFS
#90			WYAISWVRQAPGQGLEWMGGITPILGSPIY
VH			AQKFQGRVTITADESTSTVYMELSSLRSED
			TAVYYCARGVYYDYKRADYWGQGTLVTVSS
J703M1S3	CDR-H1	Residues 31-35	WYAIS
#90		of SEQ ID
VH		NO.: 486
J703M1S3	CDR-H2	Residues 50-66	GITPILGSPIYAQKFQG
#90		of SEQ ID
VH		NO.: 486
J703M1S3	CDR-H3	Residues 99-109	GVYYDYKRADY
#90		of SEQ ID
VH		NO.: 486

TABLE 15
Individual clones VL sequences
Protein		Sequence
region		123456789012345678901234567890
J703M1S3		487	EIVLTQSPDFQSVTPKEKVTITCRASQSIG
#2			NTLHWYQQKPDQSPKLLIKHVSQSVSGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			KVSSPSPTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQSIGNTLH
#2		of SEQ ID
VL		NO.: 487
J703M1S3	CDR-L2	Residues 50-56	HVSQSVS
#2		of SEQ ID
VL		NO.: 487
J703M1S3	CDR-L3	Residues 89-98	HQKVSSPSPT
#2		of SEQ
VL		ID NO.: 487
J703M1S3		488	EIVLTQSPDFQSVTPKEKVTITCRASQSIG
#13			STLHWYQQKPDQSPKLLIKHASQSNSGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			SSSLPPPTFGQGTKVEI
J703M1S3	CDR-L1	Residues 24-34	RASQSIGSTLH
#13		of SEQ ID
VL		NO.: 488
J703M1S3	CDR-L2	Residues 50-56	HASQSNS
#13		of SEQ ID
VL		NO.: 488
J703M1S3	CDR-L3	Residues 89-98	HQSSSLPPPT
#13		of SEQ
VL		ID NO.: 488
J703M1S3		489	EIVLTQSPDFQSVTPKEKVTITCRASQSIG
#26			SRLHWYQQKPDQSPKLLIKHASQSTSGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			SGSSPPRTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQSIGSRLH
#26		of SEQ ID
VL		NO.: 489
J703M1S3	CDR-L2	Residues 50-56	HASQSTS
#26		of SEQ ID
VL		NO.: 489
J703M1S3	CDR-L3	Residues 89-98	HQSGSSPPRT
#26		of SEQ
VL		ID NO.: 489
J703M1S3		490	EIVLTQSPDFQSVTPKEKVTITCRASQRIG
#30			SSLHWYQQKPDQSPKLLIKHASQSVSGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			SRSSPPPTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQRIGSSLH
#30		of SEQ ID
VL		NO.: 490
J703M1S3	CDR-L2	Residues 50-56	HASQSVS
#30		of SEQ ID
VL		NO.: 490
J703M1S3	CDR-L3	Residues 89-98	HQSRSSPPPT
#30		of SEQ
VL		ID NO.: 490
J703M1S3		491	EIVLTQSPDFQSVTPKEKVTITCRASQSIG
#33			SSLHWYQQKPDQSPKLLIKHASQSTSGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			SSSSPPSTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQSIGSSLH
#33		of SEQ ID
VL		NO.: 491
J703M1S3	CDR-L2	Residues 50-56	HASQSTS
#33		of SEQ ID
VL		NO.: 491
J703M1S3	CDR-L3	Residues 89-98	HQSSSSPPST
#33		of SEQ
VL		ID NO.: 491
J703M1S3		492	EIVLTQSPDFQSVTPKEKVTITCRASQTIG
#35			SSLHWYQQKPDQSPKLLIKHASQSISGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			TSSLPTPTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQTIGSSLH
#35		of SEQ ID
VL		NO.: 492
J703M1S3	CDR-L2	Residues 50-56	HASQSIS
#35		of SEQ ID
VL		NO.: 492
J703M1S3	CDR-L3	Residues 89-98	HQTSSLPTPT
#35		of SEQ
VL		ID NO.: 492
J703M1S3		493	EIVLTQSPDFQSVTPKEKVTITCRASQTIG
#38			SSLHWYQQKPDQSPKLLIKHASQSISGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			SSSSPPPTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQTIGSSLH
#38		of SEQ ID
VL		NO.: 493
J703M1S3	CDR-L2	Residues 50-56	HASQSIS
#38		of SEQ ID
VL		NO.: 493
J703M1S3	CDR-L3	Residues 89-98	HQSSSSPPPT
#38		of SEQ
VL		ID NO.: 493
J703M1S3		494	EIVLTQSPDFQSVTPKEKVTITCRASQSIG
#69			SSLHWYQQKPDQSPKLLIKHVSQSLSGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			RSSSPSPTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQSIGSSLH
#69		of SEQ ID
VL		NO.: 494
J703M1S3	CDR-L2	Residues 50-56	HVSQSLS
#69		of SEQ ID
VL		NO.: 494
J703M1S3	CDR-L3	Residues 89-98	HQRSSSPSPT
#69		of SEQ
VL		ID NO.: 494
J703M1S3		495	EIVLTQSPDFQSVTPKEKVTITCRASQSIG
#90			SNLHWYQQKPDQSPKLLIKHASQSISGVPS
VL			RFSGSGSGTDFTLTINSLEAEDAATYYCHQ
			TRTSPPLTFGQGTKVEIK
J703M1S3	CDR-L1	Residues 24-34	RASQSIGSNLH
#90		of SEQ ID
VL		NO.: 495
J703M1S3	CDR-L2	Residues 50-56	HASQSIS
#90		of SEQ ID
VL		NO.: 495
J703M1S3	CDR-L3	Residues 89-98	HQTRTSPPLT
#90		of SEQ
VL		ID NO.: 495

TABLE 16
AE11-5 affinity matured scFv clones converted to full length IgG
			Full length
ScFv			IgG (protein)
clone name	HC plasmid	LC plasmid	name
J703M1S3#2	pJP368; pHybE-hCg1,z,non-	pJP369; pHybE-hCk V3-	AE11-5 AM1
	a,mut(234,235)-J703M1S3#2	J703M1S31#2
J703M1S3#13	pJP370; pHybE-hCg1,z,non-	pJP371; pHybE-hCk V3-	AE11-5 AM2
	a,mut(234,235)-J703M1S3#13	J703M1S3#13
J703M1S3#26	pJP372; pHybE-hCg1,z,non-	pJP373; pHybE-hCk V3-	AE11-5 AM3
	a,mut(234,235)-J703M1S3#26	J703M1S3#26
J703M1S3#30	pJP374; pHybE-hCg1,z,non-	pJP375; pHybE-hCk V3-	AE11-5 AM4
	a,mut(234,235)-J703M1S3#30	J703M1S3#30
J703M1S3#33	pJP376; pHybE-hCg1,z,non-	pJP377; pHybE-hCk V3-	AE11-5 AM5
	a,mut(234,235)-J703M1S3#33	J703M1S3#33
J703M1S3#35	pJP378; pHybE-hCg1,z,non-	pJP379; pHybE-hCk V3-	AE11-5 AM6
	a,mut(234,235)-J703M1S3#35	J703M1S3#35
J703M1S3#38	pJP382; pHybE-hCg1,z,non-	pJP383; pHybE-hCk V3-	AE11-5 AM8
	a,mut(234,235)-J703M1S3#38	J703M1S3#38
J703M1S3#69	pJP384; pHybE-hCg1,z,non-	pJP385; pHybE-hCk V3-	AE11-5 AM9
	a,mut(234,235)-J703M1S3#69	J703M1S3#69
J703M1S3#90	pJP386; pHybE-hCg1,z,non-	pJP387; pHybE-hCk V3-	AE11-5 AM10
	a,mut(234,235)-J703M1S3#90	J703M1S3#90

1.3 TNF Enzyme-Linked Immunosorbent Assay Protocol (ELISA) and Assay Result

The following protocol is used to characterize the binding of TNF antibodies to biotinylated human or cyno TNF by enzyme-linked immunosorbent assay (ELISA). An ELISA plate was coated with 50 μl per well of goat anti human IgG-Fc at 2 μg/ml, overnight at 4° C. The plate was washed 3 times with PBS/Tween. 50 μl Mab diluted to 1 μg/ml in PBS/0.1% BSA was added to appropriate wells and incubated for 1 hour at room temperature (RT). The plate was washed 3 times with PBS/Tween. 50 μl of serial diluted biotin-human TNF was added to appropriate wells and incubated for 1 hour at RT. The plate was washed 3 times with PBS/Tween. 50 μl of streptavidin-HRP diluted 1:10,000 in PBS/0.1% BSA was added to appropriate wells and incubated for 1 hour at RT. The plate was washed 3 times with PBS/Tween. 50 μl of TMB was added to appropriate wells and the reaction was allowed to proceed for 1 minute. The reaction was stopped with 50 μl/well 2N H₂SO₄ and the absorbance read at 450 nm. Results are shown in Table 17.

	TABLE 17
		EC50 in hTNF	EC50 in cynoTNF
	IgG Name	ELISA (nM)	ELISA (nM)
	AE11-5-AM1	1.06	2.14
	AE11-5-AM2	522.5	>845
	AE11-5-AM3	1.57	1.55
	AE11-5-AM4	18.32	750.3
	AE11-5-AM5	17.7	2.2
	AE11-5-AM6	1.37	>720
	AE11-5-AM7	10.32	1.26
	AE11-5-AM8	250.2	58.58
	AE11-5-AM9	16.72	5.29
	AE11-5-AM10	0.98	0.28

1.4 TNF Neutralization Potency of TNF Antibodies by L929 Bioassay

Human TNF was prepared at Abbott Bioresearch Center (Worcester, Mass., US) and received from the Biologics Pharmacy. Mouse TNF was prepared at Abbott Bioresearch Center and received from the Biologics Pharmacy. Rat TNF was prepared at Abbott Bioresearch Center and received from the Biologics Pharmacy. Rabbit TNF was purchased from R&D Systems. Rhesus/Macaque TNF (rhTNF) was purchased from R&D Systems. Actinomycin was purchased from Sigma Aldrich and resuspended at a stock concentration of 10 mg/mL in DMSO.

Assay Media: 10% FBS (Hyclone#SH30070.03), Gibco reagents: RPMI 1640 (#21870), 2 mM L-glutamine (#25030), 50 units/mL penicillin/50 μg/mL streptomycin (#15140), 0.1 mM MEM non-essential amino acids (#11140) and 5.5×10⁻⁵ M 2-mercaptoethanol (#21985-023).

L929 cells were grown to a semi-confluent density and harvested using 0.05% tryspin (Gibco#25300). The cells were washed with PBS, counted, and resuspended at 1E6 cells/mL in assay media containing 4 μg/mL actinomycin D. The cells were seeded in a 96-well plate (Costar#3599) at a volume of 50 μL and 5E4 cells/well. Wells received 50 μL of assay media, bringing the volume to 100 μL.

A test sample was prepared as follows. The test and control IgG proteins were diluted to a 4× concentration in assay media and serial 1:3 dilutions were performed. TNF species were diluted to the following concentrations in assay media: 400 pg/mL huTNF, 200 pg/mL muTNF, 600 pg/mL ratTNF, and 100 pg/mL rabTNF. Antibody sample (200 μL) was added to the TNF (200 μL) in a 1:2 dilution scheme and allowed to incubate for 0.5 hour at room temperature.

To measure huTNF neutralization potency in this assay, the antibody/TNF solution was added to the plated cells at 100 μL for a final concentration at 375 nM-0.019 nM. The final concentration of TNF was as follows: 100 pg/mL huTNF, 50 pg/mL muTNF, 150 pg/mL ratTNF, and 25 pg/mL rabTNF. The plates were incubated for 20 hours at 37° C., 5% CO₂. To quantitate viability, 100 μL was removed from the wells and 10 μL of WST-1 reagent (Roche cat#11644807001) was added. Plates were incubated under assay conditions for 3.5 hours, centrifuged at 500×g, and 75 μL of supernatant transferred to an ELISA plate (Costar cat#3369). The plates were read at OD 420-600 nm on a Spectromax 190 ELISA plate reader. The neutralization potency of selected TNF/IL-17 DVD-Ig binding proteins is shown in Table 18.

TABLE 18
	hu TNF neutralization	rhesus TNF neutralization IC50
IgG Name	IC50 (nM)	(nM)
AE11-5 AM1	0.439	0.251
AE11-5 AM2	1.241	0.756
AE11-5 AM3	0.291	0.165
AE11-5 AM4	0.259	0.109
AE11-5 AM5	0.968	0.613
AE11-5 AM6	2.029	0.652
AE11-5 AM7	0.049	0.104
AE11-5 AM8	1.356	3.040
AE11-5 AM9	0.391	0.123
AE11-5 AM10	0.678	0.140

Example 2

Affinity Maturation of a Humanized Anti-Human TNF Antibody hMAK-195

The mouse anti-human TNF antibody MAK-195 was humanized and affinity-matured to generate a panel of humanized MAK195 variants that have cross-reactivity to cyno-TNF and improved affinity and binding kinetics against both human and cyno TNF.

To improve the affinity of hMAK195 to TNF, hypermutated CDR residues were identified from other human antibody sequences in the IgBLAST database that also shared high identity to germlines VH3-53 and IGKV1-39. The corresponding hMAK195 CDR residues were then subjected to limited mutagenesis by PCR with primers having low degeneracy at these positions to create three antibody libraries in the scFv format. The first library contained mutations at residues 31, 32, 33, 35, 50, 52, 53, 54, 56 and 58 in the VH CDR1 and 2 (Kabat numbering); the second library at residues 95 to 100, 100a, 101, and 102 in VH CDR3; and the third library at residues 28, 30, 31, 32, 50, 53, 92, 93, 94, and 95 in the three VL CDRs. To further increase the identity of hMAK195 to the human germline framework sequences, a binary degeneracy at VH positions 60 (D/A), 61 (S/D), 62 (T/S), 63 (L/V), and 65 (S/G) were introduced into the first library. Also, a binary degeneracy at VL positions 24 (K/R), 33 (V/L), 54 (R/L), 55 (H/Q), 56 (T/S), 91 (H/S) and 96 (F/Y) were introduced into the third library.

These hMAK195 variants were selected against a low concentration of biotinylated TNF for improved on-rate, off-rate, or both were carried out and antibody protein sequences of affinity-modulated hMAK195 were recovered for converting back to IgG for further characterization. All three libraries were selected separately for the ability to bind human or cynomolgus monkey TNF in the presence of decreasing concentrations of biotinylated human or cynomolgus monkey TNF antigens. All mutated CDR sequences recovered from library selections were recombined into additional libraries and the recombined libraries were subjected to more stringent selection conditions before individual antibodies are identified.

Table 19 provides a list of amino acid sequences of VH and VL of the humanized MAK-195 which were subjected to the affinity maturation selection protocol Amino acid residues of individual CDRs of each VH and VL sequence are indicated in bold.

TABLE 19
List of amino acid sequences of affinity
matured hMAK195 VH variants
	SEQ ID
Clone	NO:	VH
rHC1_B8	496	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRGDGSTDYASTLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_H12	497	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRGDGSTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E1	498	EVQLVESGGGLVQPGGSLRLSCAASGFTFSAYGVNWVRQAPGK
		GLEWVSIIWGDGATDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_A2	499	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMISSDGFTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_H6	500	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIAADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
H1 + H2_D7	501	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGSTDYASSLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_D9	502	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRDDGSTDYADTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_A10	503	EVQLVESGGGLVQPGGSLRLSCAASGETFSHIGVSWVRQAPGK
		GLEWVSMISYAGSTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARLLHKGPIDYWGQGTLVTVSS
H1 + H2_A5	504	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVNWVRQAPGK
		GLEWVSMIWSDGSTDYADTVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_F8	505	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRADGSTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D1	506	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVQWVRQAPGK
		GLEWVSMIRGDGSTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARPSHHGLIDNWGQGTLVTVSS
rHC2_C2	507	EVQLVESGGGLVQPGGSLRLSCAASGFTFSELGVNWVRQAPGK
		GLEWVSYISDVGSTYYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWHHGRFDYWGQGTLVTVSS
rHC1_G4	508	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSLIRADGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_F3	509	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGFTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWQHGPSVYWGQGTLVTVSS
rHC1_B4	510	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIRADGVTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_G3	511	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVHWVRQAPGK
		GLEWVSMIGADGYTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D7	512	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMISADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D5	513	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRSDGFTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		TEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E4	514	EVQLVESGGGLVQPGGSLRLSCAASGFTFSEYGVNWVRQAPGK
		GLEWVSIIWHDGSTAYADTVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_E10	515	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSLIRGDGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B6	516	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNFGVSWVRQAPGK
		GLEWVSMIWGDGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_B7	517	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRDDGSTYYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLGYWGQGTLVTVSS
H1 + H2_G8	518	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVNWVRQAPGK
		GLEWVSMIWAGGSTAYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_G5	519	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSLIGADGSTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQYGPLAYWGQGTLVTVSS
H1 + H2_F1	520	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIEGDGGTHYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC19	521	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTHYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPAAYWGQGTLVTVSS
H1 + H2_A10	522	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAXGK
		GLEWVSMISADGTTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_B9	523	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIRGDGTTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLGYWGQGTLVTVSS
H1 + H2_F7	524	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHYGVGWVRQAPGK
		GLEWVSMIWGAGSTNYADTVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B1	525	EVQLVESGGGLVQPGGSLRLSCAASGFTFSSFGVNWVRQAPGK
		GLEWVSMIWADGTTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_H9	526	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSVIGGDGYTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
H1 + H2_A12	527	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGX
		GLEWVSMISSDGYTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_G8	528	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWSDGSTHYADTVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_B4	529	EVQLVESGGGLVQPGGSLRLSCAASGFTFSQLGVTWVRQAPGK
		GLEWVSTISDAGSTYYASSVKGRFTIIRINSKNTLYLQMNSLR
		AEDTAVYYCARDWHHGRFAYWGQGTLVTVSS
H1 + H2_G5	530	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRGDGSTYYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_C6	531	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVQWVRQAPGK
		GLEWVSMIRDDGSTSYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_F5	532	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIRGDGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
H1 + H2_B4	533	EVQLVESGGGLVQPGGSLRLSCAASGFTFSAYGVNWVRQAPGK
		GLEWVSMISGDGSTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_F6	534	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHFGVTWVRQAPGK
		GLEWVSNIWASGSTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_B6	535	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGSTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
H1 + H2_A3	536	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNFGVNWVRQAPGK
		GLEWVSVIWGDGSTAYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D10	537	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRGDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
rHC18	538	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWSDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
S4-18	539	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTHYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
rHC2_E6	540	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSLIRGDGSTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_D4	541	EVQLVESGGGLVQPGGSLRISCAASGFTFSAFGVSWVRQAPGK
		GLEWVSMIWGDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_F8	542	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDLGVNWVRQAPGK
		GLEWVSTISDIGSTYYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWHNGRFDYWGQGTLVTVSS
rHC1_F10	543	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRGDGFTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_C12	544	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIRADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_C11	545	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHFGVNWVRQAPGK
		GLEWVSIIWGDGSTAYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_C4	546	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVEWVRQAPGK
		GLEWVSKIWADGSTDYADSLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
H1 + H2_E12	547	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSLIWGDGTTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_C4	548	EVQLVESGGGLVQPGGSLRLSCAASGFTFSYFGVSWVRQAPGK
		GLEWVSMIWGDGSTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_F9	549	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRSDGSTDYADTLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
H1 + H2_B5	550	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVNWVRQAPGK
		GLEWVSIIWSDGSTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
S4-34	551	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWADGSTHYADTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
H1 + H2_C2	552	EVQLVESGGGLVQPGGSLRLSCAASGFTFSEFGVNWVRQAPGK
		GLEWVSMIWGNGATDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_F11	553	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVNWVRQAPGK
		GLEWVSMIWGDGTTAYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_E9	554	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B2	555	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVNWVRQAPGK
		GLEWVSMIWGDGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E9	556	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNFGVNWVRQAXGK
		GLEWVSMIWGDGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_A6	557	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIGSDGFTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
H1 + H2_C8	558	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQTPGK
		GLEWVSMIRGDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_C5	559	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVSWVRQAPGK
		GLEWVSQIWGDGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_D5	560	EVQLVESGGGLVQPGGSLRLSCAASGFTFSQLGVTWVRQAPGK
		GLEWVSTISDAGSTYYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWHHGRFAYWGQGTLVTVSS
rHC1_C7	561	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWQHGPLGYWGQGTLVTVSS
H1 + H2_C3	562	EVQLVESGGGLVQPGGSLRLSCAASGFTFSAYGVHWVRQAPGK
		GLEWVSMIWGDGSTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_G7	563	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGTTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWQHGPIGYWGQGTLVTVSS
rHC1_A5	564	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGYTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
H1 + H2_G9	565	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVEWVRQAPGK
		GLEWVSKIWGDGTTDYADTLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E2	566	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIGGEGRTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_C9	567	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNLGVNWVRQAPGK
		GLEWVSMIWDVGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWHHGLFDYWGQGTLVTVSS
rHC1_G6	568	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIMGDGYTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_C1	569	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRDDGATDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
rHC1_C2	570	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMISGDGYTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
H1 + H2_C1	571	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIRGDGSTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B10	572	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNFGVNWVRQAPGX
		GLEWVSMIWADGSTDYASTLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E3	573	EVQLVESGGGLVQPGGSLRLSCAASGFTFSAFGVCWVRQAPGK
		GLEWVSMIWADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_H4	574	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRSDGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWQHGPEGYWGQGTLVTVSS
rHC2_A1	575	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIRGDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_G11	576	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSLIRSDGSTHYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_D8	577	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIRGDGYTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_A3	578	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTHYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
S4-31	579	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVQWVRQAPGK
		GLEWVSGIGADGSTAYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHSGLAYWGQGTLVTVSS
rHC36	580	EVQLVESGGGLVQPGGSLILSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWADGSTHYASSLKGRFTISRDNFKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC2_G3	581	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIRGDGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_C10	582	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIAADGSTAYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC14	583	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTHYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPAAYWGQGTLVTVSS
rHC1_D4	584	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGSTDYADTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_D11	585	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIISGDGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_E11	586	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDWGVHWMRQAPGK
		GLEWVSTIWDDGSTYYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARHGHHGPFVYWGQGTLVTVSS
H1 + H2_E7	587	EVQLVESGGGLVQPGGSLRLSCAASXFTFSNFGVNWVRQAPGK
		GLEWVSMIWGDGSTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_A8	588	EVQLVESGGGLVQPGGSLRLSCAASGFTFSVYGVNWVRQAPGK
		GLEWVSMIGDEGSTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARHWHHGAVDYWGQGTLVTVSS
H1 + H2_B9	589	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSMIWADGSTHYADSLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
S4-19	590	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVEWVRQAPGK
		GLEWVSGIWADGSTHYADTVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
S4-74	591	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTHYADTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
rHC1_H2	592	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_E3	593	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGYTSYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC34	594	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTHYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPSAYWGQGTLVTVSS
H1 + H2_F2	595	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIRADGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D9	596	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGTTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
H1 + H2_E6	597	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNFGVHWVRQAPGK
		GLEWVSMIWADGSTVYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_F3	598	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIGSDGSTYYADSLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_G11	599	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLGYWGQGTLVTVSS
H1 + H2_D3	600	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVNWVRQAPGK
		GLEWVSMIWGDGHTAYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B12	601	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSMIWAHGATHYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B11	602	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSLIRDDGSTDYASTLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_A8	603	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWGDGSTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
S4-24	604	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTHYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_F11	605	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMISADGYTDYADSLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
H1 + H2_D10	606	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWADGSTHYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_D6	607	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIGADGYTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_G4	608	EVQLVESGGGLVQPGGSLRLSCAASGFTFSAFGVSWVRQAPGK
		GLEWVSMIWADGSTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_D11	609	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSLIRGDGSTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_E9	610	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGTTYYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
rHC1_A12	611	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVQWVRQAPGK
		GLEWVSRISGDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_A2	612	EVQLVESGGGLVQPGGSLRLSCAASGFSFSNFGVNWVRQAPGK
		GLEWVSMIWADGSTNYADTVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B7	613	EVQLVESGGGLVQPGGSLRLSCAASGFTFSAYGVSWVRQAPGK
		GLEWVSIISADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_H8	614	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_F12	615	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIGADGYTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_E5	616	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIRGDGSTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_A11	617	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSMIWGSGATDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D6	618	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMISADGFTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC2_G10	619	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIAADGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_H3	620	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSLIAADGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
H1 + H2_F10	621	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIRGDGSTAYADTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_C7	622	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIWGDGNTGYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_A9	623	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGSTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
H1 + H2_E5	624	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSMIWGDGSTEYADTLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC62	625	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWADGSTHYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
H1 + H2_F4	626	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVYWVRQAPGK
		GLEWVSMIWDDGSTEYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_H8	627	EVQLVESGGGLVQPGGSLRLSCAASGFTFSQLGVTWVRQAPGK
		GLEWVSTISDAGSTYYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARDWHHGRFAYWGQGTLVTVSS
rHC2_F4	628	EVQLVESGGGLVQPGGSLRLSCAASGFTFSGPGVNWVRQAPGK
		GLEWVSSIWDDGSTYYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCARHSHDGRFDYWGQGTLVTVSS
S4-50	629	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVEWVRQAPGK
		GLEWVSGIWADGSTHYADTVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
H1 + H2_F12	630	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSMIWGEGSTGYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_E6	631	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRDDGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_F2	632	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIGGDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
H1 + H2_G6	633	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDFGVNWVRQAPGK
		GLEWVSMIWADGTTDYDDSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC2_F5	634	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSGISADGSTAYDSSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_D6	635	EVQLVESGGGLVQPGGSLRLSCAASGFTFSSYGVSWVRQAPGK
		GLEWVSLIRGDGSTYYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_A9	636	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNFGVNWVRQAPGK
		GLEWVSMIWGDGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_A1	637	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHFGVNWVRQAPGK
		GLEWVSMIWADGSTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC60	638	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWADGSTHYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPAAYWGQGTLVTVSS
rHC1_C8	639	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVHWVRQAPGK
		GLEWVSMIAGDGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
rHC44	640	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWADGSTHYADTLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_G9	641	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSIIGADGATDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLGYWGQGTLVTVSS
H1 + H2_A6	642	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSGITGDGITAYASTLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_G2	643	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMISGDGFTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_G7	644	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSNIWGDGSTDYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E10	645	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIRADGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_E2	646	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGSTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_A4	647	EVQLVESGGGLVQPGGSLRLSCAASGFTFSAYGVSWVRQAPGK
		GLEWVSMIWRDGSTDYADSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_H3	648	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVHWVRQAPGK
		GLEWVSMIWGDGSTHYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_G1	649	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVHWVRQAPGK
		GLEWVSGISADGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E8	650	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHYGVNWVRQAPGK
		GLEWVSMIGGDGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_C9	651	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIRADGSTDYASSLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_F7	652	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVQWVRQAPGK
		GLEWVSVISADGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_F6	653	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIGADGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
rHC22	654	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTDYADTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC2_G5	655	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSLIRGDGYTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_C12	656	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHYGVSWVRQAPGK
		GLEWVSVIRADGVTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
rHC3	657	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIWADGSTHYASSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVAYWGQGTLVTVSS
rHC1_F1	658	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVQWVRQAPGK
		GLEWVSRINGDGSTDYASTLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_E11	659	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIRSDGFTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B8	660	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNFGVNWVRQAPGK
		GLEWVSMIWVDGSTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_G1	661	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGK
		GLEWVSMIWGDGSTYYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_B3	662	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHYGVSWVRQAPGK
		GLEWVSMIRSDGFTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D2	663	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMITGDGYTDYADTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
rHC1_E12	664	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRADGLTDYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_B5	665	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSLIRSDGSTDYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_D11	666	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGSTDYADSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPLAYWGQGTLVTVSS
H1 + H2_A7	667	EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVIWVRQAPGK
		GLEWVSMIGGDGSTYYDSSLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_G3	668	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVNWVRQAPGK
		GLEWVSMIGSDGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_D5	669	EVQLVESGGGLVQPGGSLRLSCAASGFTFSYYGVHWVRQAPGK
		GLEWVSGISGEGSTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_D1	670	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRGDGSTYYASSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWVKGTLVTVSS
rHC1_E7	671	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSIIRGDGSTDYASSLKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
rHC1_E11	672	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIRADGTTDYASSVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
S4-55	673	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVTWVRQAPGK
		GLEWVSMIWADGSTDYASTVKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWQHGPVGYWGQGTLVTVSS
H1 + H2_C10	674	EVQLVESGGGLVQPGGSLRLSCAASGFTFSNYGVSWVRQAPGK
		GLEWVSMIRGDGSTYYADTLKGRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
H1 + H2_G10	675	EVQLVESGGGLVQPGGSLRLSCAASGFTFSHFGVNWVRQAPGK
		GLEWVSMIWADGSTSYADSVKSRFTISRDNSKNTLYLQMNSLR
		AEDTAVYYCAREWHHGPVAYWGQGTLVTVSS

Table 20 provides a list of amino acid sequences of VL regions of affinity matured fully human TNF antibodies derived from hMAK195 Amino acid residues of individual CDRs of each VH sequence are indicated in bold.

TABLE 20
List of amino acid sequences of affinity matured
hMAK195 VL variants
	SEQ
	ID
Clone	NO:	VL
S3_92	676	DIQMTQSPSSLSASVGDRVTITCRASQKVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYHTPYTFGQGTKLEIK
S3_79	677	DIQMTQSPSSLSASVGDRVTITCKASQAVSTEVAWYQQK
		PGKAPKLLIYCASTRQTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQSYSAPYTFGQGTKLEIK
S3_68	678	DIQMTQSPSSLSASVGDRVTITCRASQVVSSAVAWYQQK
		PGKAPKLLIYWASKRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_60	679	DIQMTQSPSSLSASVGDRVTITCRASQAVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S4-63	680	DIQMTQSPSSLSASVGDRVTITCKASQKVSSALAWYQQK
		PGKAPKLLIYWASALHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRPPFTFGQGTKLEIK
S3_5	681	DIQMTQSPSSLSASVGDRVTITCRASQGVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYTTPFTFGQGTKLEIK
S3_44	682	DIQMTQSPSSLSASVGDRVTITCRASQGVSRALAWYQQK
		PGKAPKLLIYWASTLHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRAPFTFGQGTKLEIK
S3_53	683	DIQMTQSPSSLSASVGDRVTITCRASQAVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYHTPFTFGQGTKLEIK
S3_91	684	DIQMTQSPSSLSASVGDRVTITCKASQGVSSALAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S3_59	685	DIQMTQSPSSLSASVGDRVTITCKASQGVSSALAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPYTFGQGTKLEIK
S3_47	686	DIQMTQSPSSLSASVGDRVTITCKASQWVSSAVAWYQQK
		PGKAPKLLIYWASTRQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRIPFTFGQGTKLEIK
S3_70	687	DIQMTQSPSSLSASVGDRVTITCKASQAVSSALAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPYTFGQGTKLEIK
S3_56	688	DIQMTQSPSSLSASVGDRVTITCKASQRVSSAVAWYQQK
		PGKAPKLLIYWASTLHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPYTFGQGTKLEIK
S3_37	689	DIQMTQSPSSLSASVGDRVTITCKASQGVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYNTPFTFGQGTKLEIK
S3_36	690	DIQMTQSPSSLSASVGDRVTITCKASQKVSSAVAWYQQK
		PGKAPKLLIYWASARHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_67	691	DIQMTQSPSSLSASVGDRVTITCKASQTVXRAVAWYQQK
		PGKAPKLLIYWASTRQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQSYSTPFTFGQGTKLEIK
S3_40	692	DIQMTQSPSSLSASVGDRVTITCRASQRVSSAVAWSQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYTTPYTFGQGTKLEIK
S3_73	693	DIQMTQSPSSLSASVGDRVTITCKASQAVSSAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S4-50	694	DIQMTQSPSSLSASVGDRVTITCKASQLVSSAVAWYQQK
		PGKAPKLLIYWASALHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSSPYTFGQGTKLEIK
S4-6	695	DIQMTQSPSSLSASVGDRVTITCKASQLVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_19	696	DIQMTQSPSSLSASVGDRVTITCKASQKVSSAVAWYQQK
		PGKAPKLLIYWASARHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRSPFTFGQGTKLEIK
S3_83	697	DIQMTQSPSSLSASVGDRVTITCRASQAVSTALAWYQQK
		PGKAPKLLIYSASTLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRSPFTFGQGTKLEIK
S3_78	698	DIQMTQSPSSLSASVGDRVTITCKASQYVGGAVAWYQQK
		PGKAPKLLIYQASTLQTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHISKPFTFGQGTKLEIK
S4-19	699	DIQMTQSPSSLSASVGDRVTITCKASQLVSSAVAWYQQK
		PGKAPKLLIYWASTLHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S3_58	700	DIQMTQSPSSLSASVGDRVTITCKASQSVNGALAWYQQK
		PGKAPKLLIYRASTRQTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSIPFTFGQGTKLEIK
S4-31	701	DIQMTQSPSSLSASVGDRVTITCRASQGVSSALAWYQQK
		PGKAPKLLIYWASALHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSAPFTFGQGTKLEIK
S3_31	702	DIQMTQSPSSLSASVGDRVTITCKASQAVSSSVAWYQQK
		PGKAPKLLIYGASTLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYNEPYTFGQGTKLEIK
S3_13	703	DIQMTQSPSSLSASVGDRVTITCKASQKVSSAVAWYQQK
		PGKAPKLLIYWASARHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPYTFGQGTKLEIK
S4-40	704	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFSFGQGTKLEIK
S3_26	705	DIQMTQSPSSLSASVGDRVTITCRASQAVSSAVAWYQQK
		PGKAPKLLIYWASKRQTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYISPYTFGQGTKLEIK
S3_33	706	DIQMTQSPSSLSASVGDRVTITCKASQGVRSALAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQSYSAPYTFGQGTKLEIK
S3_28	707	DIQMTQSPSSLSASVGDRVTITCKASQTVSNAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S4-74	708	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASARHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S3_84	709	DIQMTQSPSSLSASVGDRVTITCKASQPVRSAVAWYQQK
		PGKAPKLLIYSASTRQTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQSYSIPFTFGQGTKLEIK
S4-54	710	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASARHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYKTPFSFGQGTKLEIK
S3_23	711	DIQMTQSPSSLSASVGDRVTITCRASQAVSSAVAWYQQK
		PGKAPKLLIYWASSRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_55	712	DIQMTQSPSSLSASVGDRVTITCKASQTVGRAVAWYQQK
		PGKAPKLLIYWASTRQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQSYSTPFTFGQGTKLEIK
S4-34	713	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S3_76	714	DIQMTQSPSSLSASVGDRVTITCRASQKVSNAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYNSPFTFGQGTKLEIK
S4-12	715	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASARHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYKTPFTFGQGTKLEIK
S3_86	716	DIQMTQSPSSLSASVGDRVTITCRASQRVSSAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYTTPYTFGQGTKLEIK
S3_61	717	DIQMTQSPSSLSASVGDRVTITCKASQRVSSAVAWYQQK
		PGKAPKLLIYWASNRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_18	718	DIQMTQSPSSLSASVGDRVTITCKASQLVSSALAWYQQK
		PGKAPKLLIYWASTRQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S3_72	719	DIQMTQSPSSLSASVGDRVTITCKASQLVSSALAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRNPFTFGQGTKLEIK
S3_41	720	DIQMTQSPSSLSASVGDRVTITCKASQAVSSALAWYQQK
		PXKAPKLLIYWASSRQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S4-24	721	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASTLHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S4-17	722	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S3_90	723	DIQMTQSPSSLSASVGDRVTITCKASQPVSGAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRASYTFGQGTKLEIK
S3_87	724	DIQMTQSPSSLSASVGDRVTITCRASQKVSSAVAWYQQK
		PGKAPKLLIYWASARHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPYTFGQGTKLEIK
S3_66	725	DIQMTQSPSSLSASVGDRVTITCRASQRVSSAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYTTPYTFGQGTKLEIK
S4-18	726	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASTLHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_4	727	DIQMTQSPSSLSASVGDRVTITCRASQAVSSAVAWYQQK
		PGKAPKLLIYWASARHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSSPYTFGQGTKLEIK
S3_64	728	DIQMTQSPSSLSASVGDRVTITCKASQPVSSAVAWYQQK
		PGKAPKLLIYWASTLHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPFTFGQGTKLEIK
S3_62	729	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPYTFGQGTNLEIK
S3_29	730	DIQMTQSPSSLSASVGDIVTITCKASQLVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRTPYTFGQGTKLEIK
S3_65	731	DIQMTQSPSSLSASVGDRVTITCKASQLVSSAVAWYQQK
		PGKAPKLLIYWASMRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSSPFTFGQGTKLEIK
S3_81	732	DIQMTQSPSSLSASVGDRVTITCKASQTVSSAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYRAPYTFGQGTKLEIK
S3_39	733	DIQMTQSPSSLSASVGDRVTITCKASQRVSSALAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_49	734	DIQMTQSPSSLSASVGDRVTITCRASQLVSNAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSSPFTFGQGTKLEIK
S3_85	735	DIQMTQSPSSLSASVGDRVTITCRASQLVSSAVAWYQQK
		PGKAPKLLIYWASARHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK
S3_82	736	DIQMTQSPSSLSASVGDRVTITCKASQLVSSAVAWYQQK
		PGKAPKLLIYWASTRHSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYTTPFTFGQGTKLEIK
S3_93	737	DIQMTQSPSSLSASVGDRVTITCKASQRVSSAVAWYQQK
		PGKAPKLLIYWASTRHTGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQHYSTPFTFGQGTKLEIK

TABLE 21
Amino acid residues observed in affinity matured hMAK-195.
hMAK195 Heavy chain variable region (SEQ ID NO: 1075)
hMAK195VH EVQLVESGGGLVQPGGSLRLSCAASGFTFSDYGVNWVRQAPGKGLEWVSMIWGDGSTD
          NFS T              I RAG T A
          HLN S              V GSE F H
          YS  H              L SDA A V
          IR  Q              R AEV Y S
          Y              K LVG W N
          S  NY   G
          YDSTLKSRFTISRDNSKNTLYLQMNSLRAEDTAVYYCAREWHHGPVAYWGQGTLVTVSS
          ADSV G                                HSQQRTLDS
          QLRPASGVF
          LCLLVQDGC
          YRYNWAETN
          DFPYEKW P
          NDARS R I
          TYVTP P H
          PPDDI A
          AICA  I
          SG C
          R
hMAK195 Light chain variable region (SEQ ID NO: 1076)
hMAK195VL DIQMTQSPSSLSASVGDRVTITCKASQAVSSAVAWYQQKPGKAPKLLIYWASTRHTG
          R   S RRPL                S  SLQS
          V TNT                 R  I T
          G IGG                 L  L A
          D NCV                 C  K E
          T CTS                 Q  A F
          P KIR                 G  R
          VPSRFSGSGSGTDFTLTISSLQPEDFATYYCQQHYSTPFTFGQGTKLEIK
          SNRSTY
          FGPR
          DTML
          GIIQ
          HCAA
          S

The tables below provide a list of humanized MAK-195 antibodies that were converted into IgG proteins for characterization.

TABLE 22
VH sequences of IgG converted clones
Protein		Sequence
region	SEQ ID NO:	123456789012345678901234567890
A8		738	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVNWVRQAPGKGLEWVSMIAADGFTDYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWHHGPVAYWGQGTLVTVSS
A8	CDR-H1	Residues 31-35	NYGVN
VH		of SEQ ID
		NO.: 738
A8	CDR-H2	Residues 50-65	MIAADGFTDYASSVKG
VH		of SEQ ID
		NO.: 738
A8	CDR-H3	Residues 98-106	EWHHGPVAY
VH		of SEQ ID
		NO.: 738
B5		739	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSLIRGDGSTDYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWHHGPVAYWGQGTLVTVSS
B5	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 739
B5	CDR-H2	Residues 50-65	LIRGDGSTDYASSLKG
VH		of SEQ ID
		NO.: 739
B5	CDR-H3	Residues 98-106	EWHHGPVAY
VH		of SEQ ID
		NO.: 739
rHC44		740	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSMIWADGSTHYA
			DTLKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC44	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 740
rHC44	CDR-H2	Residues 50-65	MIWADGSTHYADTLKS
VH		of SEQ ID
		NO.: 740
rHC44	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 740
rHC22		741	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTDYA
			DTVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC22	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 741
rHC22	CDR-H2	Residues 50-65	MIWADGSTDYADTVKG
VH		of SEQ ID
		NO.: 741
rHC22	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 741
rHC81		742	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			DSVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
rHC81	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 742
rHC81	CDR-H2	Residues 50-65	MIWADGSTHYADSVKS
VH		of SEQ ID
		NO.: 742
rHC81	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 742
rHC18		743	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWSDGSTDYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC18	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 743
rHC18	CDR-H2	Residues 50-65	MIWSDGSTDYASSVKG
VH		of SEQ ID
		NO.: 743
rHC18	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 743
rHC14		744	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPAAYWGQGTLVTVSS
rHC14	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 744
rHC14	CDR-H2	Residues 50-65	MIWADGSTHYASSLKG
VH		of SEQ ID
		NO.: 744
rHC14	CDR-H3	Residues 98-106	EWQHGPAAY
VH		of SEQ ID
		NO.: 744
rHC3		745	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSMIWADGSTHYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC3	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 745
rHC3	CDR-H2	Residues 50-65	MIWADGSTHYASSLKG
VH		of SEQ ID
		NO.: 745
rHC3	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 745
rHC19		746	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPAAYWGQGTLVTVSS
rHC19	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 746
rHC19	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 746
rHC19	CDR-H3	Residues 98-106	EWQHGPAAY
VH		of SEQ ID
		NO.: 746
rHC34		747	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPSAYWGQGTLVTVSS
rHC34	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 747
rHC34	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 747
rHC34	CDR-H3	Residues 98-106	EWQHGPSAY
VH		of SEQ ID
		NO.: 747
rHC83		748	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
rHC83	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 748
rHC83	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 748
rHC83	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 748
S4-19		749	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVEWVRQAPGKGLEWVSGIWADGSTHYA
			DTVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-19	CDR-H1	Residues 31-35	NYGVE
VH		of SEQ ID
		NO.: 749
S4-19	CDR-H2	Residues 50-65	GIWADGSTHYADTVKS
VH		of SEQ ID
		NO.: 749
S4-19	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 749
S4-50		750	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVEWVRQAPGKGLEWVSGIWADGSTHYA
			DTVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVGYWGQGTLVTVSS
S4-50	CDR-H1	Residues 31-35	NYGVE
VH		of SEQ ID
		NO.: 750
S4-50	CDR-H2	Residues 50-65	GIWADGSTHYADTVKS
VH		of SEQ ID
		NO.: 750
S4-50	CDR-H3	Residues 98-106	EWQHGPVGY
VH		of SEQ ID
		NO.: 750
S4-63		751	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVEWVRQAPGKGLEWVSGIWADGSTHYA
			DTVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVGYWGQGTLVTVSS
S4-63	CDR-H1	Residues 31-35	NYGVE
VH		of SEQ ID
		NO.: 751
S4-63	CDR-H2	Residues 50-65	GIWADGSTHYADTVKS
VH		of SEQ ID
		NO.: 751
S4-63	CDR-H3	Residues 98-106	EWQHGPVGY
VH		of SEQ ID
		NO.: 751
S4-55		752	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTDYA
			STVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVGYWGQGTLVTVSS
S4-55	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 752
S4-55	CDR-H2	Residues 50-65	MIWADGSTDYASTVKG
VH		of SEQ ID
		NO.: 752
S4-55	CDR-H3	Residues 98-106	EWQHGPVGY
VH		of SEQ ID
		NO.: 752
S4-6		753	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-6	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 753
S4-6	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 753
S4-6	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 753
S4-18		754	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			DSVKSRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
S4-18	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 754
S4-18	CDR-H2	Residues 50-65	MIWADGSTHYADSVKS
VH		of SEQ ID
		NO.: 754
S4-18	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 754
S4-31		755	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVQWVRQAPGKGLEWVSGIGADGSTAYA
			SSLKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHSGLAYWGQGTLVTVSS
S4-31	CDR-H1	Residues 31-35	NYGVQ
VH		of SEQ ID
		NO.: 755
S4-31	CDR-H2	Residues 50-65	GIGADGSTAYASSLKG
VH		of SEQ ID
		NO.: 755
S4-31	CDR-H3	Residues 98-106	EWQHSGLAY
VH		of SEQ ID
		NO.: 755
S4-34		756	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVSWVRQAPGKGLEWVSMIWADGSTHYA
			DTVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
S4-34	CDR-H1	Residues 31-35	NYGVS
VH		of SEQ ID
		NO.: 756
S4-34	CDR-H2	Residues 50-65	MIWADGSTHYADTVKG
VH		of SEQ ID
		NO.: 756
S4-34	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 756
S4-74		757	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			DTVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPLAYWGQGTLVTVSS
S4-74	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 757
S4-74	CDR-H2	Residues 50-65	MIWADGSTHYADTVKG
VH		of SEQ ID
		NO.: 757
S4-74	CDR-H3	Residues 98-106	EWQHGPLAY
VH		of SEQ ID
		NO.: 757
S4-12		758	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-12	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 758
S4-12	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 758
S4-12	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 758
S4-54		759	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-54	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 759
S4-54	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 759
S4-54	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 759
S4-17		760	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-17	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 760
S4-17	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 760
S4-17	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 760
S4-40		761	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-40	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 761
S4-40	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 761
S4-40	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 761
S4-24		762	EVQLVESGGGLVQPGGSLRLSCAASGFTFS
VH			NYGVTWVRQAPGKGLEWVSMIWADGSTHYA
			SSVKGRFTISRDNSKNTLYLQMNSLRAEDT
			AVYYCAREWQHGPVAYWGQGTLVTVSS
S4-24	CDR-H1	Residues 31-35	NYGVT
VH		of SEQ ID
		NO.: 762
S4-24	CDR-H2	Residues 50-65	MIWADGSTHYASSVKG
VH		of SEQ ID
		NO.: 762
S4-24	CDR-H3	Residues 98-106	EWQHGPVAY
VH		of SEQ ID
		NO.: 762

TABLE 23
VL sequences of IgG converted clones
Protein		Sequence
region	SEQ ID NO:	123456789012345678901234567890
hMAK195		763	DIQMTQSPSSLSASVGDRVTITCKASQAVS
VL.1			SAVAWYQQKPGKAPKLLIYWASTRHTGVPS
VL			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSTPFTFGQGTKLEIKR
hMAK195	CDR-L1	Residues 24-34	KASQAVSSAVA
VL.1		of SEQ ID
VL		NO.: 763
hMAK195	CDR-L2	Residues 50-56	WASTRHT
VL.1		of SEQ ID
VL		NO.: 763
hMAK195	CDR-L3	Residues 89-97	QQHYSTPFT
VL.1		of SEQ ID
VL		NO.: 763
S4-24		764	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-24	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 764
S4-24	CDR-L2	Residues 50-56	WASTLHT
VL		of SEQ ID
		NO.: 764
S4-24	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 764
S4-40		765	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFSFGQGTKLEIKR
S4-40	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 765
S4-40	CDR-L2	Residues 50-56	WASTRHS
VL		of SEQ ID
		NO.: 765
S4-40	CDR-L3	Residues 89-97	QQHYRTPFS
VL		of SEQ ID
		NO.: 765
S4-17		766	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-17	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 766
S4-17	CDR-L2	Residues 50-56	WASTRHS
VL		of SEQ ID
		NO.: 766
S4-17	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 766
S4-54		767	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASARHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYKTPFSFGQGTKLEIKR
S4-54	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 767
S4-54	CDR-L2	Residues 50-56	WASARHT
VL		of SEQ ID
		NO.: 767
S4-54	CDR-L3	Residues 89-97	QQHYKTPFS
VL		of SEQ ID
		NO.: 767
S4-12		768	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASARHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYKTPFTFGQGTKLEIKR
S4-12	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 768
S4-12	CDR-L2	Residues 50-56	WASARHT
VL		of SEQ ID
		NO.: 768
S4-12	CDR-L3	Residues 89-97	QQHYKTPFT
VL		of SEQ ID
		NO.: 768
S4-74		769	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASARHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-74	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 769
S4-74	CDR-L2	Residues 50-56	WASARHT
VL		of SEQ ID
		NO.: 769
S4-74	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 769
S4-34		770	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-34	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 770
S4-34	CDR-L2	Residues 50-56	WASTRHT
VL		of SEQ ID
		NO.: 770
S4-34	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 770
S4-31		771	DIQMTQSPSSLSASVGDRVTITCRASQGVS
VL			SALAWYQQKPGKAPKLLIYWASALHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSAPFTFGQGTKLEIKR
S4-31	CDR-L1	Residues 24-34	RASQGVSSALA
VL		of SEQ ID
		NO.: 771
S4-31	CDR-L2	Residues 50-56	WASALHS
VL		of SEQ ID
		NO.: 771
S4-31	CDR-L3	Residues 89-97	QQHYSAPFT
VL		of SEQ ID
		NO.: 771
S4-18		772	DIQMTQSPSSLSASVGDRVTITCRASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSTPFTFGQGTKLEIKR
S4-18	CDR-L1	Residues 24-34	RASQLVSSAVA
VL		of SEQ ID
		NO.: 772
S4-18	CDR-L2	Residues 50-56	WASTLHS
VL		of SEQ ID
		NO.: 772
S4-18	CDR-L3	Residues 89-97	QQHYSTPFT
VL		of SEQ ID
		NO.: 772
S4-6		773	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTRHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSTPFTFGQGTKLEIKR
S4-6	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 773
S4-6	CDR-L2	Residues 50-56	WASTRHT
VL		of SEQ ID
		NO.: 773
S4-6	CDR-L3	Residues 89-97	QQHYSTPFT
VL		of SEQ ID
		NO.: 773
S4-55		774	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-55	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 774
S4-55	CDR-L2	Residues 50-56	WASTLHT
VL		of SEQ ID
		NO.: 774
S4-55	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 774
S4-63		775	DIQMTQSPSSLSASVGDRVTITCKASQKVS
VL			SALAWYQQKPGKAPKLLIYWASALHSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRPPFTFGQGTKLEIKR
S4-63	CDR-L1	Residues 24-34	KASQKVSSALA
VL		of SEQ ID
		NO.: 775
S4-63	CDR-L2	Residues 50-56	WASALHS
VL		of SEQ ID
		NO.: 775
S4-63	CDR-L3	Residues 89-97	QQHYRPPFT
VL		of SEQ ID
		NO.: 775
S4-50		776	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASALHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYSSPYTFGQGTKLEIKR
S4-50	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 776
S4-50	CDR-L2	Residues 50-56	WASALHT
VL		of SEQ ID
		NO.: 776
S4-50	CDR-L3	Residues 89-97	QQHYSSPYT
VL		of SEQ ID
		NO.: 776
S4-19		777	DIQMTQSPSSLSASVGDRVTITCKASQLVS
VL			SAVAWYQQKPGKAPKLLIYWASTLHTGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			HYRTPFTFGQGTKLEIKR
S4-19	CDR-L1	Residues 24-34	KASQLVSSAVA
VL		of SEQ ID
		NO.: 777
S4-19	CDR-L2	Residues 50-56	WASTLHT
VL		of SEQ ID
		NO.: 777
S4-19	CDR-L3	Residues 89-97	QQHYRTPFT
VL		of SEQ ID
		NO.: 777

TABLE 24
Heavy and light chain pairs of hMAK195 affinity matured clones
Clone name	HC	LC	Protein name
A8	hMAK195-A8	hMAK195 VL.1	hMAK195-AM11
B5	hMAK195-B5	hMAK195 VL.1	hMAK195-AM13
rHC3	hMAK195 rHC3	hMAK195 VL.1	hMAK195-AM14
rHC18	hMAK195 rHC18	hMAK195 VL.1	hMAK195-AM15
rHC19	hMAK195 rHC19	hMAK195 VL.1	hMAK195-AM16
rHC22	hMAK195 rHC22	hMAK195 VL.1	hMAK195-AM17
rHC34	hMAK195 rHC34	hMAK195 VL.1	hMAK195-AM18
rHC60	hMAK195 rHC60	hMAK195 VL.1	hMAK195-AM19
S4-6	hMAK195 S4-6	hMAK195 S4-6	hMAK195-AM20
S4-12	hMAK195 S4-12	hMAK195 S4-12	hMAK195-AM21
S4-17	hMAK195 S4-17	hMAK195 S4-17	hMAK195-AM22
S4-18	hMAK195 S4-18	hMAK195 S4-18	hMAK195-AM23
S4-19	hMAK195 S4-19	hMAK195 S4-19	hMAK195-AM24
S4-24	hMAK195 S4-24	hMAK195 S4-24	hMAK195-AM25
S4-34	hMAK195 S4-34	hMAK195 S4-34	hMAK195-AM26

2.1 TNF Enzyme-Linked Immunosorbent Assay Result

TABLE 25
IgG Name     EC50 in hTNFa ELISA (nM)
hMAK195-AM11 0.2
hMAK195-AM13 0.2
hMAK195-AM14 0.051
hMAK195-AM15 0.052
hMAK195-AM16 0.056
hMAK195-AM17 0.056
hMAK195-AM18 0.052
hMAK195-AM19 0.057
hMAK195-AM20 0.043
hMAK195-AM21 0.042
hMAK195-AM22 0.052
hMAK195-AM23 0.055
hMAK195-AM24 0.053
hMAK195-AM25 0.052
hMAK195-AM26 0.061

2.2 TNF Neutralization Potency of TNF Antibodies by L929 Bioassay

TABLE 26
	hu TNF neutralization IC50	rhesus TNF
IgG Name	(nM)	neutralization IC50 (nM)
hMAK195-AM11	0.259	>25
hMAK195-AM13	1.218	4.64
hMAK195-AM14	0.0401	4.61
hMAK195-AM15	0.036	>150
hMAK195-AM16	0.0105	0.803
hMAK195-AM17	0.0031	>25
hMAK195-AM18	0.0145	0.4412
hMAK195-AM19	0.0126	1.206
hMAK195-AM20	0.0037	0.596
hMAK195-AM21	0.009	0.09
hMAK195-AM22	0.00345	0.2705
hMAK195-AM23	0.0468	2.627
hMAK195-AM24	0.015	0.557
hMAK195-AM25	0.0114	0.262
hMAK195-AM26	0.0061	0.2495

Example 3

Affinity Maturation of a Humanized Anti-Human TNF Antibody hMAK-199

The mouse anti-human TNF antibody MAK-199 was humanized and affinity-matured to generate a panel of humanized MAK195 variants that have improved affinity and binding kinetics against both human and cyno TNF. Several libraries were made according to specifications below:

Three HC libraries were made after the V2I back-mutation was first introduced and confirmed that it did not impact scFv affinity to TNF.H1+H2 (DDK) library:

Limited mutagenesis at 7 residues (T30, N31, N35, T52a, T54, E56, T58)

Germline toggle: M34I and F63L

H1+H2 (QKQ) library:

Limited mutagenesis at 7 residues (T30, N31, N35, T52a, T54, E56, T58)

Germline toggle: M34I and F63L

Germline back-mutations: D61Q, D62K, K64Q, F67V, F69M, L71T

H3 library:

Limited mutagenesis at 12 residues 95-100, 100a-100f

Germline toggle: F91Y

LC library: library

Limited mutagenesis at 11 residues 28, 30-32, 50, 53, 91-94, 96

Germline toggles: T51A, Y71F, F87Y, and T43A/V44P (these two co-evolve)

Recombined libraries:VH libraries will be recombined with and without VL library after library diversity is reduced after at least 3 rounds of selection.

All four libraries were selected separately for the ability to bind human or cynomolgus monkey TNF in the presence of decreasing concentrations of biotinylated human or cynomolgus monkey TNF antigens. All mutated CDR sequences recovered from library selections were recombined into additional libraries and the recombined libraries were subjected to more stringent selection conditions before individual antibodies are identified.

Table 27 provides a list of amino acid sequences of VH of the hMAK-199 antibody which were subjected to the affinity maturation selection protocol Amino acid residues of individual CDRs of each VH sequence are indicated in bold.

TABLE 27
List of amino acid sequences of affinity matured
hMAK199 VH variants
Clone	SEQ ID NO:	VH
J644M2S1-10VH	778	EVQLVQSGAEVKKPGASVKVSCKASGYTFNDYGITWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-11VH	779	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-12VH	780	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGISWVRQ
		APGQGLEWMGWINTYTGEPHYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-13VH	781	EVQLVQSGAEVKKPGASVKVSCKASGYTFDNYGIQWVRQ
		APGQGLEWMGWINTYTGAPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-14VH	782	EVQLVQSGAEVKKPGASVKVSCKASGYTFTDYGINWVRQ
		APGQGLEWMGWINTYTGKPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-15VH	783	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGMNWVRQ
		APGQGLEWMGWINTYTGESTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-16VH	784	EVQLVQSGAEVKKPGASVKVSCKASGYTFKNYGMTWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-17VH	785	EVQLVQSGAEVKKPGASVKVSCKASGYAFTDYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-18VH	786	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGEPAYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-1VH	787	EVQLVQSGAEVKKPGASVKVSCKASGYTFRNYGINWVRQ
		APGQGLEWMGWINTYTGQPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-22VH	788	EVQLVQSGAEVKKPGASVKVSCKASGYTFTDYGINWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-23VH	789	EVQLVQSGAEVKKPGASVKVSCKASGYTFKNYGIIWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-24VH	790	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGVPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-25VH	791	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGKPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-27VH	792	EVQLVQSGAEVKKPGASVKVSCKASGYTFKNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-28VH	793	EVQLVQSGAEVKKPGASVKVSCKASGYTFRNYGINWVRQ
		APGQGLEWMGWINTYTGKPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-2VH	794	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGIXWVRQ
		APGQGLEWMGWINTYXGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-31VH	795	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGEPHYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-33VH	796	EVQLVQSGAEVKKPGASVKVSCKASGYTFTHYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-34VH	797	EVQLVQSGAEVKKPGASVKVSCKASGYTFTHYGINWVRQ
		APGQGLEWMGWINTYTGQPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-35VH	798	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGITWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-36VH	799	EVQLVQSGAEVKKPGASVKVSCKASGYTFGNYGINWVRQ
		APGQGLEWMGWINTYTGKPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-37VH	800	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGRPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-38VH	801	EVQLVQSGAEVKKPGASVKVSCKASGYTFKNYGINWVRQ
		APGQGLEWMGWINTYTGEPHYAQGFTGRVTMTTDTSTST
		AYIELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-3VH	802	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGEPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-40VH	803	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-41VH	804	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGIGWVRQ
		APGQGLEWMGWINTYTGKPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-43VH	805	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGVPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-44VH	806	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGIAWVRQ
		APGQGLEWMGWINTYTGVPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-45VH	807	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGVPHYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-46VH	808	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGIXWVRQ
		APGQGLEWMGWINTYTGEPXYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-47VH	809	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGVPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-48VH	810	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGQPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-4VH	811	EVQLVQSGAEVKKPGASVKVSCKASGYTFTDYGITWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-50VH	812	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGVPQYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-51VH	813	EVQLVQSGAEVKKPGASVKVSCKASGYTFQNYGINWVRQ
		APGQGLEWMGWINTYTGVPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-53VH	814	EVQLVQSGAEVKKPGASVKVSCKASGYTFTQYGINWVRQ
		APGQGLEWMGWINTYTGDPHYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-54VH	815	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGLPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-55VH	816	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYNGKPMYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-56VH	817	EVQLVQSGAEVKKPGASVKVSCKASGYTFRNYGITWVRQ
		APGQGLEWMGWINTYTGEPAYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-59VH	818	EVQLVQSGAEVKKPGASVKVSCKASGYTFNHYGINWVRQ
		APGQGLEWMGWINTYTGRPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-5VH	819	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-60VH	820	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-64VH	821	EVQLVQSGAEVKKPGASVKVSCKASGYTFDNYGINWVRQ
		APGQGLEWMGWINTYTGVPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-65VH	822	EVQLVQSGAEVKKPGASVKVSCKASGYTFNDYGIIWVRQ
		APGQGLEWMGWINTYTGKPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-66VH	823	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-67VH	824	EVQLVQSGAEVKKPGASVKVSCKASGYTFANYGMNWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-68VH	825	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGEPSYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-6VH	826	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGVPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-71VH	827	EVQLVQSGAEVKKPGASVKVSCKASGYTFDHYGMNWVRQ
		APGQGLEWMGWINTYTGKPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-72VH	828	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGIGWVRQ
		APGQGLEWMGWINTYTGKPSYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-73VH	829	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-74VH	830	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGMNWVRQ
		APGQGLEWMGWINTYTGKPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-75VH	831	EVQLVQSGAEVKKPGASVKVSCKASGYTFDNYGMNWVRQ
		APGQGLEWMGWINTYTGVPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-76VH	832	EVQLVQSGAEVKKPGASVKVSCKASGYTFNSYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-77VH	833	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGITWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-79VH	834	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYNGQPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-7VH	835	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGIIWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-81VH	836	EVQLVQSGAEVKKPGASVKVSCKASGYTFANYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-82VH	837	EVQLVQSGAEVKKPGASVKVSCKASGYTFSDYGIQWVRQ
		APGQGLEWMGWINTYTGRPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-83VH	838	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGISWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-84VH	839	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGIQWVRQ
		APGQGLEWMGWINTYTGVPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-85VH	840	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGVPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-87VH	841	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYSGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-88VH	842	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGQPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-8VH	843	EVQLVQSGAEVKKPGASVKVSCKASGYTFPNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-90VH	844	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGKTNYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-91VH	845	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGEPNYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-92VH	846	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGITWVRQ
		APGQGLEWMGWINTYTGEPHYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-93VH	847	EVQLVQSGAEVKKPGASVKVSCKASGYTFKNYGINWVRQ
		APGQGLEWMGWINTYTGQPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-94VH	848	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGIPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-95VH	849	EVQLVQSGAEVKKPGASVKVSCKASGYTFTDYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-96VH	850	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYSGVPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J644M2S1-9VH	851	EVQLVQSGAEVKKPGASVKVSCKASGYTFTDYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-11VH	852	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFWRTVVGTDNAMDYWGQG
		TTVTVSS
J647M2-12VH	853	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKYSTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-13VH	854	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDSAMDYWGQG
		TTVTVSS
J647M2-15VH	855	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFMTTMAVTDFAMDYWGQG
		TTVTVSS
J647M2-16VH	856	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLTTVVATDNAMDYWGQG
		TTVTVSS
J647M2-17VH	857	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLTTVIVTDNAMDYWGQG
		TTVTVSS
J647M2-19VH	858	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFFTPVVVTDNAMDYWGQG
		TTVTVSS
J647M2-1VH	859	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLMTTVVVTDHAMDYWGQG
		TTVTVSS
J647M2-20VH	860	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKYLTTVVVTDSAMDYWGQG
		TTVTVSS
J647M2-21VH	861	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFRSSVAVTDNAMDYWGQG
		TTVTVSS
J647M2-22VH	862	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLFTTVVVTDSAMDYWGQG
		TTVTVSS
J647M2-23VH	863	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKYLMPVVVTDYAMDYWGQG
		TTVTVSS
J647M2-24VH	864	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKLLDAVMVTDYAMDYWGQG
		TTVTVSS
J647M2-26VH	865	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLTTVVVNDYAMDYWGQG
		TTVTVSS
J647M2-44VH	866	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLTTVAVTDYAMDYWGQG
		TTVTVSS
J647M2-45VH	867	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLKTVVATDDAMDYWGQG
		TTVTVSS
J647M2-47VH	868	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLNTAVVTDYAMDYWGQG
		TTVTVSS
J647M2-48VH	869	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARRFLTTVDVTDNAMDYWGQG
		TTVTVSS
J647M2-4VH	870	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKYLTPVVATDFAMDYWGQG
		TTVTVSS
J647M2-51VH	871	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKCMTTIVETDNAMDYWGQG
		TTVTVSS
J647M2-52VH	872	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFMNTVDVTDNAMDYWGQG
		TTVTVSS
J647M2-53VH	873	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLFTTVVVTDDAMDYWGQG
		TTVTVSS
J647M2-54VH	874	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLMTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-55VH	875	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLPTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-56VH	876	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKLLTTVVVTDNAMDYWGQG
		TTVTVSS
J647M2-58VH	877	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKILTTVVVTDNAMDYWGQG
		TTVTVSS
J647M2-70VH	878	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKVMATEVVTDYAMDYWGQG
		TTVTVSS
J647M2-71VH	879	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLVTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-72VH	880	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFRKPVSVTDYAMDYWGQG
		TTVTVSS
J647M2-73VH	881	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLWTTVVVTDNAMDYWGQG
		TTVTVSS
J647M2-74VH	882	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLTPVVVTDYAMDYWGQG
		TTVTVSS
J647M2-75VH	883	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFRTTVVETDYCMDYWGQG
		TTVTVSS
J647M2-76VH	884	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKYFTTVAVTDYAMDYWGQG
		TTVTVSS
J647M2-78VH	885	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARRFLTTVEVTDLAMDYWGQG
		TTVTVSS
J647M2-79VH	886	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLRTEVMTDYAMDYWGQG
		TTVTVSS
J647M2-7VH	887	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLSTVAVTDSAMDYWGQG
		TTVTVSS
J647M2-80VH	888	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKVLNTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-83VH	889	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFMNTAMVTDYAMDYWGQG
		TTVTVSS
J647M2-84VH	890	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFSTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-85VH	891	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKYFTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2-86VH	892	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLNTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-12VH	893	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFMPTVVETDYAMDYWGQG
		TTVTVSS
J647M2S1-13VH	894	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGNPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-14VH	895	EVQLVQSGAEVKKPGASVKVSCKASGYTFADYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-15VH	896	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLTTVVVTDCAMDYWGQG
		TTVTVSS
J647M2S1-17VH	897	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-18VH	898	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLTTVVVTDNAMDYWGQG
		TTVTVSS
J647M2S1-19VH	899	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLNTVVGTDYAMDYWGQG
		TTVTVSS
J647M2S1-21VH	900	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKLLTTEAVTDYAMDYWGQG
		TTVTVSS
J647M2S1-22VH	901	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKYSTPVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-23VH	902	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGEPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-26VH	903	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKCLNTVAVTEHRMDYWGQG
		TTVTVSS
J647M2S1-28VH	904	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLTTVVHTDYAMDYWGQG
		TTVTVSS
J647M2S1-30VH	905	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGQPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-31VH	906	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-32VH	907	EVQLVQSGAEVKKPGASVKVSCKASGYTFANYGINWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-33VH	908	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFRTTVVLTDSAMDYWGQG
		TTVTVSS
J647M2S1-35VH	909	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGEPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-36VH	910	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFQTPVVDTDYAMDYWGQG
		TTVTVSS
J647M2S1-39VH	911	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFMKTRVVTDNAMDYWGQG
		TTVTVSS
J647M2S1-40VH	912	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGIVWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-41VH	913	EVQLVQSGAEVKKPGASVKVSCKASGYTFPNYGISWVRQ
		APGQGLEWMGWINTYTGEPSYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-43VH	914	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGEPSYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-45VH	915	EVQLVQSGAEVKKPGASVKVSCKASGYTFTKYGINWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-47VH	916	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKYLTTVVATDYAMDYWGQG
		TTVTVSS
J647M2S1-48VH	917	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLNTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-65VH	918	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLTPVVVTDCAMDYWGQG
		TTVTVSS
J647M2S1-66VH	919	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGEPRYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-67VH	920	EVQLVQSGAEVKKPGASVKVSCKASGYTFRDYGINWVRQ
		APGQGLEWMGWINTYTGLPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-69VH	921	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFWTTIVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-6VH	922	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKLLTTVSATDNAMDYWGQG
		TTVTVSS
J647M2S1-70VH	923	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLNTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-72VH	924	EVQLVQSGAEVKKPGASVKVSCKASGYTFTDYGINWVRQ
		APGQGLEWMGWINTYNGEPSYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-75VH	925	EVQLVQSGAEVKKPGASVKVSCKASGYTFATYGIAWVRQ
		APGQGLEWMGWINTYSGVPKYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-76VH	926	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFRTTAVPTDNAMDYWGQG
		TTVTVSS
J647M2S1-77VH	927	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFLTTVVNTDSAMDYWGQG
		TTVTVSS
J647M2S1-78VH	928	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGRG
		TTVTVSS
J647M2S1-79VH	929	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLKTRVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-7VH	930	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-80VH	931	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLTTVVATDYAMDYWGQG
		TTVTVSS
J647M2S1-84VH	932	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGEPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-85VH	933	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGQPTYAQGFTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-87VH	934	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFFPTMVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-88VH	935	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKFVTTMVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-8VH	936	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYAQGLTGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQG
		TTVTVSS
J647M2S1-92VH	937	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYFCARKLLTTIVATDNAMDYWGQG
		TTVTVSS
J647M2S1-93VH	938	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLMSTVVETDNAMDYWGQG
		TTVTVSS
J647M2S1-94VH	939	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLFTVVQTDYAMDYWGQG
		TTVTVSS
J647M2S1-96VH	940	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQ
		APGQGLEWMGWINTYTGEPTYADDFKGRFTFTLDTSTST
		AYMELSSLRSEDTAVYYCARKLLNTVVDTDYAMDYWGQG
		TTVTVSS
J662M2S3-14VH	941	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGIIWVRQ
		APGQGLEWMGWINTYTGEPHYAQKLQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKLFTVEDVTDCAMDYWGQG
		TTVTVSS
J662M2S3-18VH	942	EVQLVQSGAEVKKPGASVKVSCKASGYTFDNYGMNWVRQ
		APGQGLEWMGWINTYNGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKLFLVEAVTDYAMDYWGQG
		TTVTVSS
J662M2S3-28VH	943	EVQLVQSGAEVKKPGASVKVSCKASGYTFRNYGIIWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKLFTTVDVTDNAMDYWGQG
		TTVTVSS
J662M2S3-29VH	944	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGIIWVRQ
		APGQGLEWMGWINTYTGVPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKLFNTVDVTDNAMDYWGQG
		TTVTVSS
J662M2S3-30VH	945	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGIIWVRQ
		APGQGLEWMGWINTYTGEPHYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKLFKTMAVTDAAMDYWGQG
		TTVTVSS
J662M2S3-34VH	946	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFRNTVAVTDYAMDYWGQG
		TTVTVSS
J662M2S3-3VH	947	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGIIWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKLFNTVAVTDNAMDYWGQG
		TTVTVSS
J662M2S3-41VH	948	EVQLVQSGAEVKKPGASVKVSCKASGYTFTNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKLFFTEDVTDYAMDYWGQG
		TTVTVSS
J662M2S3-45VH	949	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGINWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKFFTPVVVTDNAMDYWGQG
		TTVTVSS
J662M2S3-55VH	950	EVQLVQSGAEVKKPGASVKVSCKASGYTFRNYGITWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKLFTTMDVTDNAMDYWGQG
		TTVTVSS
J662M2S3-5VH	951	EVQLVQSGAEVKKPGASVKVSCKASGYTFANYGIIWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKLFTTMDVTDNAMDYWGQG
		TTVTVSS
J662M2S3-65VH	952	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGIIWVRQ
		APGQGLEWMGWINTYTGKPTYAQKLQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKLFNTVDVTDNAMDYWGQG
		TTVTVSS
J662M2S3-78VH	953	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGIIWVRQ
		APGQGLEWMGWINTYTGKPSYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKLFNTVDVTDNAMDYWGQG
		TTVTVSS
J662M2S3-84VH	954	EVQLVQSGAEVKKPGASVKVSCKASGYTFSNYGINWVRQ
		APGQGLEWMGWINTYTGQPSYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKLFKTEAVTDYAMDYWGQG
		TTVTVSS
J662M2S3-87VH	955	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGIIWVRQ
		APGQGLEWMGWINTYSGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYFCARKLFTTMDVTDNAMDYWGQG
		TTVTVSS
J662M2S3-96VH	956	EVQLVQSGAEVKKPGASVKVSCKASGYTFNNYGIIWVRQ
		APGQGLEWMGWINTYTGKPTYAQKFQGRVTMTTDTSTST
		AYMELSSLRSEDTAVYYCARKFFTTMAVTDNAMDYWGQG
		TTVTVSS

Table 28 provides a list of amino acid sequences of VL regions of affinity matured fully human TNF antibodies derived from hMAK199 Amino acid residues of individual CDRs of each VL sequence are indicated in bold.

TABLE 28
List of amino acid sequences
of affinity matured hMAK199 VL variants
Clone	SEQ ID NO:	VL
J644M2S1-11Vk	957	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J644M2S1-73Vk	958	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J647M2-11Vk	959	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKTVKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J647M2S1-10Vk	960	DIQMTQSPSSLSASVGDRVTITCRASQDIWNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNRYPPTFGQGTKLEIK
J647M2S1-16Vk	961	DIQMTQSPSSLSASVGDRVTITCRASQDICTYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNSPPPTFGQGTKLEIK
J647M2S1-1Vk	962	DIQMTQSPSSLSASVGDRVTITCRASQAIGNYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J647M2S1-20Vk	963	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTRPPTFGQGTKLEIK
J647M2S1-24Vk	964	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSLLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTGPPTFGQGTKLEIK
J647M2S1-25Vk	965	DIQMTQSPSSLSASVGDRVTITCRASQDIYNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J647M2S1-29Vk	966	DIQMTQSPSSLSASVGDRVTITCRASQDISHYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPATFGQGTKLEIK
J647M2S1-2Vk	967	DIQMTQSPSSLSASVGDRVTITCRASQDISSYLNWYQQK
		PGKTVKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTPPPTFGQGTKLEIK
J647M2S1-34Vk	968	DIQMTQSPSSLSASVGDRVTITCRASQDISSYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J647M2S1-37Vk	969	DIQMTQSPSSLSASVGDRVTITCRASQEISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTMPTTFGQGTKLEIK
J647M2S1-38Vk	970	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYFASRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTPPTTFGQGTKLEIK
J647M2S1-3Vk	971	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPSTFGQGTKLEIK
J647M2S1-42Vk	972	DIQMTQSPSSLSASVGDRVTITCRASQVISNTLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNALPPTFGQGTKLEIK
J647M2S1-44Vk	973	DIQMTQSPSSLSASVGDRVTITCRASQDISTYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTPPPTFGQGTKLEIK
J647M2S1-46Vk	974	DIQMTQSPSSLSASVGDRVTITCRASQDISQYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J647M2S1-50Vk	975	DIQMTQSPSSLSASVGDRVTITCRASQDITNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTAPPTFGQGTKLEIK
J647M2S1-52Vk	976	DIQMTQSPSSLSASVGDRVTITCRASQGISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTMPPTFGQGTKLEIK
J647M2S1-56Vk	977	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J647M2S1-59Vk	978	DIQMTQSPSSLSASVGDRVTITCRASQDISKYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTRPPTFGQGTKLEIK
J647M2S1-71Vk	979	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSLLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTQPPTFGQGTKLEIK
J647M2S1-74Vk	980	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNSQPPTFGQGTKLEIK
J647M2S1-78Vk	981	DIQMTQSPSSLSASVGDRVTITCRASQDISKYLNWYQQK
		PGKAPKLLIYNASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J647M2S1-7Vk	982	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSLLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNIWPPTFGQGTKLEIK
J647M2S1-9Vk	983	DIQMTQSPSSLSASVGDRVTITCRASQDISHYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J652M2S1-10Vk	984	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTFPPTFGQGTKLEIK
J652M2S1-13Vk	985	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J652M2S1-14Vk	986	DIQMTQSPSSLSASVGDRVTITCRASQDISNVLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J652M2S1-15Vk	987	DIQMTQSPSSLSASVGDRVTITCRASQDIYKYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTMPPTFGQGTKLEIK
J652M2S1-17Vk	988	DIQMTQSPSSLSASVGDRVTITCRASQEIFSYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNMGPPTFGQGTKLEIK
J652M2S1-18Vk	989	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTQPPTFGQGTKLEIK
J652M2S1-1Vk	990	DIQMTQSPSSLSASVGDRVTITCRASQDISSYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTWPPTFGQGTKLEIK
J652M2S1-22Vk	991	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTRPPTFGQGTKLEIK
J652M2S1-23Vk	992	DIQMTQSPSSLSASVGDRVTITCRASQDISNFLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTFPPTFGQGTKLEIK
J652M2S1-25Vk	993	DIQMTQSPSSLSASVGDRVTITCRASQDISNFLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTRPPTFGQGTKLEIK
J652M2S1-26Vk	994	DIQMTQSPSSLSASVGDRVTITCRASQDINNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J652M2S1-27Vk	995	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYASGLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTWPPTFGQGTKLEIK
J652M2S1-28Vk	996	DIQMTQSPSSLSASVGDRVTITCRASQDISRYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTQPPTFGQGTKLEIK
J652M2S1-29Vk	997	DIQMTQSPSSLSASVGDRVTITCRASQDIATYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTMPPTFGQGTKLEIK
J652M2S1-31Vk	998	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTFPPTFGQGTKLEIK
J652M2S1-33Vk	999	DIQMTQSPSSLSASVGDRVTITCRASQRIGNYLNWYQQK
		PGKTVKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J652M2S1-34Vk	1000	DIQMTQSPSSLSASVGDRVTITCRASQEISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNSQPPTFGQGTKLEIK
J652M2S1-35Vk	1001	DIQMTQSPSSLSASVGDRVTITCRASQDIANYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J652M2S1-37Vk	1002	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTFPPTFGQGTKLEIK
J652M2S1-38Vk	1003	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTQPPTFGQGTKLEIK
J652M2S1-3Vk	1004	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTPPPTFGQGTKLEIK
J652M2S1-40Vk	1005	DIQMTQSPSSLSASVGDRVTITCRASQDISNFLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J652M2S1-41Vk	1006	DIQMTQSPSSLSASVGDRVTITCRASQDIGNFLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTRPPTFGQGTKLEIK
J652M2S1-42Vk	1007	DIQMTQSPSSLSASVGDRVTITCRASQDITNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTPPPTFGQGTKLEIK
J652M2S1-45Vk	1008	DIQMTQSPSSLSASVGDRVTITCRASQDISDYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNMWPPTFGQGTKLEIK
J652M2S1-47Vk	1009	DIQMTQSPSSLSASVGDRVTITCRASQDISSYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTMPPTFGQGTKLEIK
J652M2S1-48Vk	1010	DIQMTQSPSSLSASVGDRVTITCRASQDISHYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J652M2S1-49Vk	1011	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTMPPTFGQGTKLEIK
J652M2S1-51Vk	1012	DIQMTQSPSSLSASVGDRVTITCRASQDISQYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTRPPTFGQGTKLEIK
J652M2S1-52Vk	1013	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNMRPPTFGQGTKLEIK
J652M2S1-53Vk	1014	DIQMTQSPSSLSASVGDRVTITCRASQDISTYLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J652M2S1-55Vk	1015	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTGPPTFGQGTKLEIK
J652M2S1-56Vk	1016	DIQMTQSPSSLSASVGDRVTITCRASQNINNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTMPPTFGQGTKLEIK
J652M2S1-57Vk	1017	DIQMTQSPSSLSASVGDRVTITCRASQDISKYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTPPPTFGQGTKLEIK
J652M2S1-61Vk	1018	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTVPPTFGQGTKLEIK
J652M2S1-62Vk	1019	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSKLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNIFPPTFGQGTKLEIK
J652M2S1-64Vk	1020	DIQMTQSPSSLSASVGDRVTITCRASQGIYNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J652M2S1-67Vk	1021	DIQMTQSPSSLSASVGDRVTITCRASQDISSYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J652M2S1-69Vk	1022	DIQMTQSPSSLSASVGDRVTITCRASQEISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTGPPTFGQGTKLEIK
J652M2S1-6Vk	1023	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTPPPTFGQGTKLEIK
J652M2S1-71Vk	1024	DIQMTQSPSSLSASVGDRVTITCRASQDISDYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTWPPTFGQGTKLEIK
J652M2S1-73Vk	1025	DIQMTQSPSSLSASVGDRVTITCRASQDIWKYLNWYQQK
		PGKAPKLLIYYASRLQSVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTLPPTFGQGTKLEIK
J652M2S1-75Vk	1026	DIQMTQSPSSLSASVGDRVTITCRASQDISTYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTWPPTFGQGTKLEIK
J652M2S1-77Vk	1027	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTPPPTFGQGTKLEIK
J652M2S1-78Vk	1028	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNAPPPTFGQGTKLEIK
J652M2S1-79Vk	1029	DIQMTQSPSSLSASVGDRVTITCRASQDIYKFLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J652M2S1-80Vk	1030	DIQMTQSPSSLSASVGDRVTITCRASQDIFNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J652M2S1-82Vk	1031	DIQMTQSPSSLSASVGDRVTITCRASQDISNTLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTLPPTFGQGTKLEIK
J652M2S1-84Vk	1032	DIQMTQSPSSLSASVGDRVTITCRASQHISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J652M2S1-86Vk	1033	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNMPPPTFGQGTKLEIK
J652M2S1-87Vk	1034	DIQMTQSPSSLSASVGDRVTITCRASQDITNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTVPPTFGQGTKLEIK
J652M2S1-8Vk	1035	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYFTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGNTQPPTFGQGTKLEIK
J652M2S1-90Vk	1036	DIQMTQSPSSLSASVGDRVTITCRASQDISKFLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYYCQQGNTRPPTFGQGTKLEIK
J652M2S1-91Vk	1037	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTFPPTFGQGTKLEIK
J652M2S1-92Vk	1038	DIQMTQSPSSLSASVGDRVTITCRASQDIYNVLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGITLPPTFGQGTKLEIK
J652M2S1-93Vk	1039	DIQMTQSPSSLSASVGDRVTITCRASQHISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTWPPTFGQGTKLEIK
J652M2S1-95Vk	1040	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTQPSTFGQGTKLEIK
J652M2S1-9Vk	1041	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J662M2S3-13Vk	1042	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNSWPPTFGQGTKLEIK
J662M2S3-15Vk	1043	DIQMTQSPSSLSASVGDRVTITCRASQDIYNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J662M2S3-21Vk	1044	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTWPPTFGQGTKLEIK
J662M2S3-22Vk	1045	DIQMTQSPSSLSASVGDRVTITCRASQDISQYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTWPPTFGQGTKLEIK
J662M2S3-34Vk	1046	DIQMTQSPSSLSASVGDRVTITCRASQDIYDVLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYYCQQGITLPPTFGQGTKLEIK
J662M2S3-3Vk	1047	DIQMTQSPSSLSASVGDRVTITCRASQDIENYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J662M2S3-41Vk	1048	DIQMTQSPSSLSASVGDRVTITCRASQNIENFLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTWPPTFGQGTKLEIK
J662M2S3-56Vk	1049	DIQMTQSPSSLSASVGDRVTITCRASQDIYNYLNWYQQK
		PGKAPKLLIYYTSRLQGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTPPPTFGQGTKLEIK
J662M2S3-64Vk	1050	DIQMTQSPSSLSASVGDRVTITCRASQDIASYLNWYQQK
		PGKAPKLLIYYTSRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J662M2S3-78Vk	1051	DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQK
		PGKVPKLLIYYTSRLQSGVPSRFSGSGSGTDYTLTISSL
		QPEDFATYFCQQGNTQPPTFGQGTKLEIK
J662M2S3-84Vk	1052	DIQMTQSPSSLSASVGDRVTITCRASQNIYNVLNWYQQK
		PGKAPKLLIYYASRLQSGVPSRFSGSGSGTDFTLTISSL
		QPEDFATYFCQQGNTMPPTFGQGTKLEIK

TABLE 29
Amino acid residues observed in affinity matured hMAK-199 antibodies
MAK199 Heavy chain variable region (SEQ ID NO: 1077)
MAK199VH.2a 1234567890123456789012345678901234567890123456789012a345678901
            EIQLVQSGAEVKKPGASVKVSCKASGYTFTNYGMNWVRQAPGQGLEWMGWINTYTGEPTYAD
            V                           ND  II                   N K S  Q
            AH   T                   S V H
            ST   Q                     Q N
            RS   S                     R M
            DQ   G                     L K
            KK   A                     S A
            P    V                     N R
            Q                          I Q
            M                          D D
            G                          A
            E
            234567890123456789012abc345678901234567890abcdefg1234567890123
            DFKG              RFTFTLDTSTSTAYMELSSLRSEDTAVYFCARKFLTTVVVTDYAMDYWGQGTTVTVSS
            GLT  V M T                      Y   RLFNPMDASENT
            K Q                                 NYMKVEAEM SR
            IRSSAEMN CC
            VSRARSD  H
            CWL IMG  D
            QP QII  I
            VF GPQ  F
            ND D P  V
            GM   N  L
            CA   L  A
            H
Mak199 Light chain variable region (SEQ ID NO: 1078)
Mak199Vk.1a 1234567890123456789012345678901234567890123456789012345678901
            DIQMTQSPSSLSASVGDRVTITCRASQDISNYLNWYQQKPGKTVKLLIYYTSRLQSGVPSR
            N YQV          AP     FA L
            E ESF          V      N  K
            H AKT                    G
            G TT
            V WH
            R GD
            A NR
            F
            C
            234567890123456789012345678901234567890123456a
            FSGSGSGTDYTLTISSLQPEDFATYFCQQGNTLPPTFGQGTKLEIK
            F               Y    ISW T
            MQ S
            IP A
            AM
            RR
            F
            G
            V
            Y
            A

TABLE 30
Individual hMAK-199 VH sequences from converted clones
Protein		Sequence
region	SEQ ID NO:	123456789012345678901234567890
J662M2S3		1053	EVQLVQSGAEVKKPGASVKVSCKASGYTFA
#10 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
10 VH		of SEQ ID
		NO.: 1053
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
10 VH		of SEQ ID
		NO.: 1053
J662M2S3#	CDR-H3	Residues 99-112	RASQDISQYLN
10 VH		of SEQ ID
		NO.: 1053
J662M2S3#		1054	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
13 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKLQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFNTVDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
13 VH		of SEQ ID
		NO.: 1054
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKLQG
13 VH		of SEQ ID
		NO.: 1054
J662M2S3#	CDR-H3	Residues 99-112	KLFNTVDVTDNAMD
13 VH		of SEQ ID
		NO.: 1054
J662M2S3#		1055	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
15 VH			NYGIIWVRQAPGQGLEWMGWINTYTGVPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFNTVDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
15 VH		of SEQ ID
		NO.: 1055
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGVPTYAQKFQG
15 VH		of SEQ ID
		NO.: 1055
J662M2S3#	CDR-H3	Residues 99-112	KLFNTVDVTDNAMD
15 VH		of SEQ ID
		NO.: 1055
J662M2S3#		1056	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
16 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFNTVAVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
16 VH		of SEQ ID
		NO.: 1056
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
16 VH		of SEQ ID
		NO.: 1056
J662M2S3#	CDR-H3	Residues 99-112	KLFNTVAVTDNAMD
16 VH		of SEQ ID
		NO.: 1056
J662M2S3#		1057	EVQLVQSGAEVKKPGASVKVSCKASGYTFR
21 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFTTVDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
21 VH		of SEQ ID
		NO.: 1057
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
21 VH		of SEQ ID
		NO.: 1057
J662M2S3#	CDR-H3	Residues 99-112	KLFTTVDVTDNAMD
21 VH		of SEQ ID
		NO.: 1057
J662M2S3#		1058	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
34 VH			NYGINWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKFRNTVAVTDYAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGIN
34 VH		of SEQ ID
		NO.: 1058
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
34 VH		of SEQ ID
		NO.: 1058
J662M2S3#	CDR-H3	Residues 99-112	KFRNTVAVTDYAMD
34 VH		of SEQ ID
		NO.: 1058
J662M2S3#		1059	EVQLVQSGAEVKKPGASVKVSCKASGYTFR
36 VH			NYGITWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGIT
36 VH		of SEQ ID
		NO.: 1059
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
36 VH		of SEQ ID
		NO.: 1059
J662M2S3#	CDR-H3	Residues 99-112	KLFTTMDVTDNAMD
36 VH		of SEQ ID
		NO.: 1059
J662M2S3#		1060	EVQLVQSGAEVKKPGASVKVSCKASGYTFA
45 VH			NYGIIWVRQAPGQGLEWMGWINTYTGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
45 VH		of SEQ ID
		NO.: 1060
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGKPTYAQKFQG
45 VH		of SEQ ID
		NO.: 1060
J662M2S3#	CDR-H3	Residues 99-112	KLFTTMDVTDNAMD
45 VH		of SEQ ID
		NO.: 1060
J662M2S3#		1061	EVQLVQSGAEVKKPGASVKVSCKASGYTFS
58 VH			NYGINWVRQAPGQGLEWMGWINTYTGQPSY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYYCARKLFKTEAVTDYAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGIN
58 VH		of SEQ ID
		NO.: 1061
J662M2S3#	CDR-H2	Residues 50-66	WINTYTGQPSYAQKFQG
58 VH		of SEQ ID
		NO.: 1061
J662M2S3#	CDR-H3	Residues 99-112	KLFKTEAVTDYAMD
58 VH		of SEQ ID
		NO.: 1061
J662M2S3#		1062	EVQLVQSGAEVKKPGASVKVSCKASGYTFN
72 VH			NYGIIWVRQAPGQGLEWMGWINTYSGKPTY
			AQKFQGRVTMTTDTSTSTAYMELSSLRSED
			TAVYFCARKLFTTMDVTDNAMDYWGQGTTV
			TVSS
J662M2S3#	CDR-H1	Residues 31-35	NYGII
72 VH		of SEQ ID
		NO.: 1062
J662M2S3#	CDR-H2	Residues 50-66	WINTYSGKPTYAQKFQG
72 VH		of SEQ ID
		NO.: 1062
J662M2S3#	CDR-H3	Residues 99-112	KLFTTMDVTDNAMD
72 VH		of SEQ ID
		NO.: 1062

TABLE 31
Individual hMAK-199 clones VL sequences
Protein		Sequence
region	SEQ ID NO:	123456789012345678901234567890
J662M2S3#		1063	DIQMTQSPSSLSASVGDRVTITCRASQDIS
10 VL			QYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#10	CDR-L1	Residues 24-34	RASQDISQYLN
VL		of SEQ ID
		NO.: 1063
J662M2S3#10	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1063
J662M2S3#10	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 1063
J662M2S3#13		1064	DIQMTQSPSSLSASVGDRVTITCRASQDIS
VL			NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNSWPPTFGQGTKLEIK
J662M2S3#13	CDR-L1	Residues 24-34	RASQDISNYLN
VL		of SEQ ID
		NO.: 1064
J662M2S3#13	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1064
J662M2S3#13	CDR-L3	Residues 89-97	QQGNSWPPT
VL		of SEQ
		ID NO.: 1064
J662M2S3#15		1065	DIQMTQSPSSLSASVGDRVTITCRASQDIY
VL			NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTQPPTFGQGTKLEIK
J662M2S3#15	CDR-L1	Residues 24-34	RASQDIYNYLN
VL		of SEQ ID
		NO.: 1065
J662M2S3#15	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1065
J662M2S3#15	CDR-L3	Residues 89-97	QQGNTQPPT
VL		of SEQ
		ID NO.: 1065
J662M2S3#16		1066	DIQMTQSPSSLSASVGDRVTITCRASQDIE
VL			NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTQPPTFGQGTKLEIK
J662M2S3#16	CDR-L1	Residues 24-34	RASQDIENYLN
VL		of SEQ ID
		NO.: 1066
J662M2S3#16	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1066
J662M2S3#16	CDR-L3	Residues 89-97	QQGNTQPPT
VL		of SEQ
		ID NO.: 1066
J662M2S3#21		1067	DIQMTQSPSSLSASVGDRVTITCRASQDIS
VL			NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#21	CDR-L1	Residues 24-34	RASQDISNYLN
VL		of SEQ ID
		NO.: 1067
J662M2S3#21	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1067
J662M2S3#21	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 1067
J662M2S3#34		1068	DIQMTQSPSSLSASVGDRVTITCRASQDIY
VL			DVLNWYQQKPGKAPKLLIYYASRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYYCQQ
			GITLPPTFGQGTKLEIK
J662M2S3#34	CDR-L1	Residues 24-34	RASQDIYDVLN
VL		of SEQ ID
		NO.: 1068
J662M2S3#34	CDR-L2	Residues 50-56	YASRLQS
4 VL		of SEQ ID
		NO.: 1068
J662M2S3#34	CDR-L3	Residues 89-97	QQGITLPPT
VL		of SEQ
		ID NO.: 1068
J662M2S3#36		1069	DIQMTQSPSSLSASVGDRVTITSRASQDIS
VL			NYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#36	CDR-L1	Residues 24-34	RASQDISNYLN
VL		of SEQ ID
		NO.: 1069
J662M2S3#36	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1069
J662M2S3#36	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 1069
J662M2S3#45		1070	DIQMTQSPSSLSASVGDRVTITSRASQDIS
VL			QYLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTWPPTFGQGTKLEIK
J662M2S3#45	CDR-L1	Residues 24-34	RASQDISQYLN
VL		of SEQ ID
		NO.: 1070
J662M2S3#45	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1070
J662M2S3#45	CDR-L3	Residues 89-97	QQGNTWPPT
VL		of SEQ
		ID NO.: 1070
J662M2S3#58		1071	DIQMTQSPSSLSASVGDRVTITSRASQNIY
VL			NVLNWYQQKPGKAPKLLIYYASRLQSGVPS
			RFSGSGSGTDFTLTISSLQPEDFATYFCQQ
			GNTMPPTFGQGTKLEIK
J662M2S3#58	CDR-L1	Residues 24-34	RASQNIYNVLN
VL		of SEQ ID
		NO.: 1071
J662M2S3#58	CDR-L2	Residues 50-56	YASRLQS
VL		of SEQ ID
		NO.: 1071
J662M2S3#58	CDR-L3	Residues 89-97	QQGNTMPPT
VL		of SEQ
		ID NO.: 1071
J662M2S3#72		1072	DIQMTQSPSSLSASVGDRVTITSRASQDIS
VL			NFLNWYQQKPGKAPKLLIYYTSRLQSGVPS
			RFSGSGSGTDYTLTISSLQPEDFATYFCQQ
			GNTQPPTFGQGTKLEIK
J662M2S3#72	CDR-L1	Residues 24-34	RASQDISNFLN
VL		of SEQ ID
		NO.: 1072
J662M2S3#72	CDR-L2	Residues 50-56	YTSRLQS
VL		of SEQ ID
		NO.: 1072
J662M2S3#72	CDR-L3	Residues 89-97	QQGNTQPPT
VL		of SEQ
		ID NO.: 1072

TABLE 32
hMAK199 affinity matured scFv clones converted to full length IgG
ScFv			Full length IgG
clone name	HC plasmid	LC plasmid	(protein) name
J662M2S3#10	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM1
	J662M2S3#10	M2S3#10
J662M2S3#13	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM2
	J662M2S3#13	M2S3#13
J662M2S3#15	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM3
	J662M2S3#15	M2S3#15
J662M2S3#16	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM4
	J662M2S3#16	M2S3#16
J662M2S3#21	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM5
	J662M2S3#21	M2S3#21
J662M2S3#34	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM6
	J662M2S3#34	M2S3#34
J662M2S3#36	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM7
	J662M2S3#36	M2S3#36
J662M2S3#45	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM8
	J662M2S3#45	M2S3#45
J662M2S3#58	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM9
	J662M2S3#58	M2S3#58
J662M2S3#72	pHybE-hCg1,z,non-a V2	pHybE-hCk V3 J662	hMAK199-AM10
	J662M2S3#72	M2S3#72

3.1 TNF Enzyme-Linked Immunosorbent Assay Result

TABLE 33
hMAK199 affinity matured full length IgG
IgG Name     EC50 in hTNFa ELISA (nM)
hMAK199-AM1  0.016
hMAK199-AM2  0.016
hMAK199-AM3  0.019
hMAK199-AM4  0.050
hMAK199-AM5  0.078
hMAK199-AM6  0.035
hMAK199-AM7  0.100
hMAK199-AM8  0.219
hMAK199-AM9  0.032
hMAK199-AM10 0.014

3.2 TNF Neutralization Potency of TNF Antibodies by L929 Bioassay

TABLE 34
	hu TNF	rhesus TNF neutralization
IgG Name	neutralization IC50 (nM)	IC50 (nM)
hMAK199-AM1	0.054	0.012
hMAK199-AM2	0.029	0.010
hMAK199-AM3	0.051	0.019
hMAK199-AM4	0.028	0.005
hMAK199-AM5	0.087	0.020
hMAK199-AM6	0.033	0.004
hMAK199-AM7	0.095	0.051
hMAK199-AM8	0.247	0.204
hMAK199-AM9	0.163	0.089
hMAK199-AM10	0.048	0.034

Example 4

Example 4.4

Affinity Determination Using BIACORE Technology

TABLE 35
Reagent for Biacore Analyses
	Antigen	Vendor Designation	Vendor	Catalog #
	TNFα	Recombinant Human TNF-	R&D	210-TA
		α/TNFSF1A	systems

BIACORE Methods:

The BIACORE assay (Biacore, Inc. Piscataway, N.J.) determines the affinity of binding proteins with kinetic measurements of on-rate and off-rate constants. Binding of binding proteins to a target antigen (for example, a purified recombinant target antigen) is determined by surface plasmon resonance-based measurements with a Biacore® 1000 or 3000 instrument (Biacore®AB, Uppsala, Sweden) using running HBS-EP (10 mM HEPES [pH 7.4], 150 mM NaCl, 3 mM EDTA, and 0.005% surfactant P20) at 25° C. All chemicals are obtained from Biacore® AB (Uppsala, Sweden) or otherwise from a different source as described in the text. For example, approximately 5000 RU of goat anti-mouse IgG, (Fey), fragment specific polyclonal antibody (Pierce Biotechnology Inc, Rockford, Ill., US) diluted in 10 mM sodium acetate (pH 4.5) is directly immobilized across a CM5 research grade biosensor chip using a standard amine coupling kit according to manufacturer's instructions and procedures at 25 μg/ml. Unreacted moieties on the biosensor surface are blocked with ethanolamine. Modified carboxymethyl dextran surface in flowcell 2 and 4 is used as a reaction surface. Unmodified carboxymethyl dextran without goat anti-mouse IgG in flow cell 1 and 3 is used as the reference surface. For kinetic analysis, rate equations derived from the 1:1 Langmuir binding model are fitted simultaneously to association and dissociation phases of all eight injections (using global fit analysis) with the use of Biaevaluation 4.0.1 software. Purified antibodies are diluted in HEPES-buffered saline for capture across goat anti-mouse IgG specific reaction surfaces. Antibodies to be captured as a ligand (25 μg/ml) are injected over reaction matrices at a flow rate of 5 μl/minute. The association and dissociation rate constants, k_on (M¹ s¹) and k_off (s⁻¹), are determined under a continuous flow rate of 25 μl/minute. Rate constants are derived by making kinetic binding measurements at different antigen concentrations ranging from 10-200 nM. The equilibrium dissociation constant (M) of the reaction between antibodies and the target antigen is then calculated from the kinetic rate constants by the following formula: K_D=k_off/k_on. Binding is recorded as a function of time and kinetic rate constants are calculated. In this assay, on-rates as fast as 10⁶M⁻¹ s⁻¹ and off-rates as slow as 10⁻⁶ s⁻¹ can be measured.

The binding proteins herein are expected to have beneficial properties in this regard, including high affinity, slow off rate, and high neutralizing capacity.

Example 4.5

Neutralization of Human TNF-α

L929 cells are grown to a semi-confluent density and harvested using 0.25% trypsin

(Gibco#25300). The cells are washed with PBS, counted and resuspended at 1E6 cells/mL in assay media containing 4 μg/mL actinomycin D. The cells are seeded in a 96-well plate (Costar#3599) at a volume of 100 μL and 5E4 cells/well. The binding proteins and control IgG are diluted to a 4× concentration in assay media and serial 1:4 dilutions are performed. The huTNF-α is diluted to 400 pg/mL in assay media. Binding protein sample (200 μL) is added to the huTNF-α (200 μL) in a 1:2 dilution scheme and allowed to incubate for 0.5 hour at room temperature.

The binding protein/human TNF-α solution is added to the plated cells at 100 μL for a final concentration of 100 pg/mL huTNF-α and 150 nM-0.0001 nM binding protein. The plates are incubated for 20 hours at 37° C., 5% CO₂. To quantitate viability, 100 μL is removed from the wells and 10 μL of WST-1 reagent (Roche cat#11644807001) is added. Plates are incubated under assay conditions for 3.5 hours. The plates are read at OD 420-600 nm on a Spectromax 190 ELISA plate reader.

The binding proteins herein are expected to have beneficial properties in this regard, including high affinity, slow off rate, and high neutralizing capacity.

Example 4.6

Treatment

A patient requiring treatment with a TNF-α binding protein may have a disease with immune and inflammatory elements, such as autoimmune diseases, particularly those associated with inflammation, including Crohn's disease, psoriasis (including plaque psoriasis), arthritis (including rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis), multiple sclerosis, and ankylosing spondylitis. Therefore, the binding proteins herein may be used to treat these disorders.

Administration of the TNF-α binding protein may occur by subcutaneous injection. If the patient has rheumatoid arthritis, psoratic arthritis, or ankylosing spondyitis, the patient may receive 40 mg every other week as a starting dose and 40 mg every week, if necessary to achieve treatment goals. If the patient has juvenile idiopathic arthritis and weighs from 15 kg to <30 kg, the patient may receive 20 mg every other week, and if >30 kg, 40 mg every other week. If the patient has Crohn's disease, the patient may receive an initial dose of 160 mg (four 40 mg injections in one day or two 40 mg injections per day for two consecutive days) followed by 80 mg two weeks later, and another two weeks later begin a maintenance dose of 40 mg every other week. If the patient has plaque psoriasis, the patient may receive an 80 mg initial dose, followed by 40 mg every other week starting one week after initial dose.

The binding protein may be provided in a single-use prefilled pen (40 mg/0.8 mL), a single-use prefilled glass syringe (40 mg/0.8 mL or 20 mg/0.4 mL).

INCORPORATION BY REFERENCE

The contents of all cited references (including literature references, patents, patent applications, and websites) that are cited throughout this application are hereby expressly incorporated by reference in their entirety, as are the references cited therein. The practice disclosed herein will employ, unless otherwise indicated, conventional techniques of immunology, molecular biology and cell biology, which are well known in the art.

EQUIVALENTS

The invention may be embodied in other specific forms without departing from the spirit or essential characteristics thereof. The foregoing embodiments are therefore to be considered in all respects illustrative rather than limiting of the invention described herein. Scope of the invention is thus indicated by the appended claims rather than by the foregoing description, and all changes that come within the meaning and range of equivalency of the claims are therefore intended to be embraced herein.

Claims

1-18. (canceled)

19. A method for treating a mammal comprising administering to the mammal an effective amount of a pharmaceutical composition comprising a binding protein that binds human TNFα, the binding protein comprising at least one heavy chain variable region (VH region) and at least one light chain variable region (VL region), wherein the VH region comprises the amino acid sequences of the three complementarity determining regions (CDRs) from SEQ ID NO: 1077 or the amino acid sequence of SEQ ID NO: 1077,wherein the VL region comprises the amino acid sequence of the three CDRs from SEQ ID NO: 1078 or the amino acid sequence of SEQ ID NO: 1078.

20. (canceled)

21. A method for reducing human TNF-α activity in a human subject suffering from a disorder in which TNF-α activity is detrimental, the method comprising administering to the human subject a binding protein of claim 19 such that human TNF-α activity in the human subject is reduced and/or treatment is achieved.

22. A method for treating a patient suffering from a disorder in which TNF-α is detrimental comprising administering to the patient the binding protein of claim 19 either before, concurrent, or after the administration to the patient of a second agent, wherein the second agent is selected from the group consisting of an antibody, or fragment thereof, capable of binding human IL-12; PGE2; LPA; NGF; CGRP; SubP; RAGE; histamine; a histamine receptor blocker; bradykinin; IL-1alpha; IL-1beta; VEGF; PLGF; methotrexate; a corticosteroid, a glucocorticoid receptor modulator; cyclosporin, rapamycin, FK506, and a non-steroidal anti-inflammatory agent.

23. The method of claim 21, wherein the disorder is an autoimmune and/or inflammatory disorder.

24. The method of claim 23, wherein the disorder is selected from the group consisting of Crohn's disease, psoriasis, plaque psoriasis, arthritis, rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis, multiple sclerosis, and ankylo sing spondylitis.

25. The method of claim 23, wherein the disorder is selected from the group consisting of a respiratory disorder; asthma; allergic and nonallergic asthma; asthma due to infection; asthma due to infection with respiratory syncytial virus (RSV); chronic obstructive pulmonary disease (COPD); a condition involving airway inflammation; eosinophilia; fibrosis and excess mucus production; cystic fibrosis; pulmonary fibrosis; an atopic disorder; atopic dermatitis; urticaria; eczema; allergic rhinitis; allergic enterogastritis; an inflammatory and/or autoimmune condition of the skin; an inflammatory and/or autoimmune condition of gastrointestinal organs; inflammatory bowel diseases (IBD); ulcerative colitis; Crohn's disease; an inflammatory and/or autoimmune condition of the liver; liver cirrhosis; liver fibrosis; liver fibrosis caused by hepatitis B and/or C virus; scleroderma; tumors or cancers; hepatocellular carcinoma; glioblastoma; lymphoma; Hodgkin's lymphoma; a viral infection; a bacterial infection; a parasitic infection; HTLV-1 infection; suppression of expression of protective type 1 immune responses, and suppression of expression of a protective type 1 immune response during vaccination.

26-29. (canceled)

30. The method of claim 22, wherein the disorder is an autoimmune and/or inflammatory disorder.

31. The method of claim 30, wherein the disorder is selected from the group consisting of Crohn's disease, psoriasis, plaque psoriasis, arthritis, rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis, multiple sclerosis, and ankylo sing spondylitis.

32. The method of claim 30, wherein the disorder is selected from the group consisting of a respiratory disorder; asthma; allergic and nonallergic asthma; asthma due to infection; asthma due to infection with respiratory syncytial virus (RSV); chronic obstructive pulmonary disease (COPD); a condition involving airway inflammation; eosinophilia; fibrosis and excess mucus production; cystic fibrosis; pulmonary fibrosis; an atopic disorder; atopic dermatitis; urticaria; eczema; allergic rhinitis; allergic enterogastritis; an inflammatory and/or autoimmune condition of the skin; an inflammatory and/or autoimmune condition of gastrointestinal organs; inflammatory bowel diseases (IBD); ulcerative colitis; Crohn's disease; an inflammatory and/or autoimmune condition of the liver; liver cirrhosis; liver fibrosis; liver fibrosis caused by hepatitis B and/or C virus; scleroderma; tumors or cancers; hepatocellular carcinoma; glioblastoma; lymphoma; Hodgkin's lymphoma; a viral infection; a bacterial infection; a parasitic infection; HTLV-1 infection; suppression of expression of protective type 1 immune responses, and suppression of expression of a protective type 1 immune response during vaccination.

33. A method for treating a mammal comprising administering to the mammal an effective amount of a pharmaceutical composition comprising a binding protein that binds human TNFα, the binding protein comprising at least one heavy chain variable region (VH region), wherein the VH region comprises the amino acid sequences of the three complementarity determining regions (CDRs) from SEQ ID NO: 1077 or the amino acid sequence of SEQ ID NO: 1077.

34. A method for reducing human TNF-α activity in a human subject suffering from a disorder in which TNF-α activity is detrimental, the method comprising administering to the human subject the binding protein of claim 33 such that human TNF-α activity in the human subject is reduced and/or treatment is achieved.

35. A method for treating a patient suffering from a disorder in which TNF-α is detrimental comprising administering to the patient the binding protein of claim 33 either before, concurrent, or after the administration to the patient of a second agent, wherein the second agent is selected from the group consisting of an antibody, or fragment thereof, capable of binding human IL-12; PGE2; LPA; NGF; CGRP; SubP; RAGE; histamine; a histamine receptor blocker; bradykinin; IL-1alpha; IL-1beta; VEGF; PLGF; methotrexate; a corticosteroid, a glucocorticoid receptor modulator; cyclosporin, rapamycin, FK506, and a non-steroidal anti-inflammatory agent.

36. The method of claim 34, wherein the disorder is an autoimmune and/or inflammatory disorder.

37. The method of claim 36, wherein the disorder is selected from the group consisting of Crohn's disease, psoriasis, plaque psoriasis, arthritis, rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis, multiple sclerosis, and ankylo sing spondylitis.

38. The method of claim 36, wherein the disorder is selected from the group consisting of a respiratory disorder; asthma; allergic and nonallergic asthma; asthma due to infection; asthma due to infection with respiratory syncytial virus (RSV); chronic obstructive pulmonary disease (COPD); a condition involving airway inflammation; eosinophilia; fibrosis and excess mucus production; cystic fibrosis; pulmonary fibrosis; an atopic disorder; atopic dermatitis; urticaria; eczema; allergic rhinitis; allergic enterogastritis; an inflammatory and/or autoimmune condition of the skin; an inflammatory and/or autoimmune condition of gastrointestinal organs; inflammatory bowel diseases (IBD); ulcerative colitis; Crohn's disease; an inflammatory and/or autoimmune condition of the liver; liver cirrhosis; liver fibrosis; liver fibrosis caused by hepatitis B and/or C virus; scleroderma; tumors or cancers; hepatocellular carcinoma; glioblastoma; lymphoma; Hodgkin's lymphoma; a viral infection; a bacterial infection; a parasitic infection; HTLV-1 infection; suppression of expression of protective type 1 immune responses, and suppression of expression of a protective type 1 immune response during vaccination.

39. The method of claim 35, wherein the disorder is an autoimmune and/or inflammatory disorder.

40. The method of claim 39, wherein the disorder is selected from the group consisting of Crohn's disease, psoriasis, plaque psoriasis, arthritis, rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis, multiple sclerosis, and ankylo sing spondylitis.

41. The method of claim 39, wherein the disorder is selected from the group consisting of a respiratory disorder; asthma; allergic and nonallergic asthma; asthma due to infection; asthma due to infection with respiratory syncytial virus (RSV); chronic obstructive pulmonary disease (COPD); a condition involving airway inflammation; eosinophilia; fibrosis and excess mucus production; cystic fibrosis; pulmonary fibrosis; an atopic disorder; atopic dermatitis; urticaria; eczema; allergic rhinitis; allergic enterogastritis; an inflammatory and/or autoimmune condition of the skin; an inflammatory and/or autoimmune condition of gastrointestinal organs; inflammatory bowel diseases (IBD); ulcerative colitis; Crohn's disease; an inflammatory and/or autoimmune condition of the liver; liver cirrhosis; liver fibrosis; liver fibrosis caused by hepatitis B and/or C virus; scleroderma; tumors or cancers; hepatocellular carcinoma; glioblastoma; lymphoma; Hodgkin's lymphoma; a viral infection; a bacterial infection; a parasitic infection; HTLV-1 infection; suppression of expression of protective type 1 immune responses, and suppression of expression of a protective type 1 immune response during vaccination.

42. A method for treating a mammal comprising administering to the mammal an effective amount of a pharmaceutical composition comprising a binding protein that binds human TNFα, the binding protein comprising at least one light chain variable region (VL region), wherein the VL region comprises the amino acid sequences of the three complementarity determining regions (CDRs) from SEQ ID NO: 1078 or the amino acid sequence of SEQ ID NO: 1078.

43. A method for reducing human TNF-α activity in a human subject suffering from a disorder in which TNF-α activity is detrimental, the method comprising administering to the human subject the binding protein of claim 40 such that human TNF-α activity in the human subject is reduced and/or treatment is achieved.

44. A method for treating a patient suffering from a disorder in which TNF-α is detrimental comprising administering to the patient the binding protein of claim 40 either before, concurrent, or after the administration to the patient of a second agent, wherein the second agent is selected from the group consisting of an antibody, or fragment thereof, capable of binding human IL-12; PGE2; LPA; NGF; CGRP; SubP; RAGE; histamine; a histamine receptor blocker; bradykinin; IL-1alpha; IL-1beta; VEGF; PLGF; methotrexate; a corticosteroid, a glucocorticoid receptor modulator; cyclosporin, rapamycin, FK506, and a non-steroidal anti-inflammatory agent.

45. The method of claim 43, wherein the disorder is an autoimmune and/or inflammatory disorder.

46. The method of claim 45, wherein the disorder is selected from the group consisting of Crohn's disease, psoriasis, plaque psoriasis, arthritis, rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis, multiple sclerosis, and ankylo sing spondylitis.

47. The method of claim 45, wherein the disorder is selected from the group consisting of a respiratory disorder; asthma; allergic and nonallergic asthma; asthma due to infection; asthma due to infection with respiratory syncytial virus (RSV); chronic obstructive pulmonary disease (COPD); a condition involving airway inflammation; eosinophilia; fibrosis and excess mucus production; cystic fibrosis; pulmonary fibrosis; an atopic disorder; atopic dermatitis; urticaria; eczema; allergic rhinitis; allergic enterogastritis; an inflammatory and/or autoimmune condition of the skin; an inflammatory and/or autoimmune condition of gastrointestinal organs; inflammatory bowel diseases (IBD); ulcerative colitis; Crohn's disease; an inflammatory and/or autoimmune condition of the liver; liver cirrhosis; liver fibrosis; liver fibrosis caused by hepatitis B and/or C virus; scleroderma; tumors or cancers; hepatocellular carcinoma; glioblastoma; lymphoma; Hodgkin's lymphoma; a viral infection; a bacterial infection; a parasitic infection; HTLV-1 infection; suppression of expression of protective type 1 immune responses, and suppression of expression of a protective type 1 immune response during vaccination.

48. The method of claim 44, wherein the disorder is an autoimmune and/or inflammatory disorder.

49. The method of claim 48, wherein the disorder is selected from the group consisting of Crohn's disease, psoriasis, plaque psoriasis, arthritis, rheumatoid arthritis, psoratic arthritis, osteoarthritis, or juvenile idiopathic arthritis, multiple sclerosis, and ankylo sing spondylitis.

50. The method of claim 48, wherein the disorder is selected from the group consisting of a respiratory disorder; asthma; allergic and nonallergic asthma; asthma due to infection; asthma due to infection with respiratory syncytial virus (RSV); chronic obstructive pulmonary disease (COPD); a condition involving airway inflammation; eosinophilia; fibrosis and excess mucus production; cystic fibrosis; pulmonary fibrosis; an atopic disorder; atopic dermatitis; urticaria; eczema; allergic rhinitis; allergic enterogastritis; an inflammatory and/or autoimmune condition of the skin; an inflammatory and/or autoimmune condition of gastrointestinal organs; inflammatory bowel diseases (IBD); ulcerative colitis; Crohn's disease; an inflammatory and/or autoimmune condition of the liver; liver cirrhosis; liver fibrosis; liver fibrosis caused by hepatitis B and/or C virus; scleroderma; tumors or cancers; hepatocellular carcinoma; glioblastoma; lymphoma; Hodgkin's lymphoma; a viral infection; a bacterial infection; a parasitic infection; HTLV-1 infection; suppression of expression of protective type 1 immune responses, and suppression of expression of a protective type 1 immune response during vaccination.

51. The method of claim 19, wherein the binding protein: (a) modulates a biological function of the TNF-α;(b) neutralizes the TNF-α;(c) diminishes the ability of the TNF-α to bind to its receptor;(d) diminishes the ability of pro-human TNF-α, mature-human TNF-α, or truncated-human TNF-α to bind to its receptor; and/or(e) reduces one or more of TNF-dependent cytokine production, TNF-dependent cell killing, TNF-dependent inflammation, TNF-dependent bone erosion, and TNF-dependent cartilage damage.

52. The method of claim 19, wherein the binding protein comprises: (a) a heavy chain constant region comprising an amino acid sequence of SEQ ID NO:2 or SEQ ID NO: 3; and(b) a light chain constant region comprising an amino acid sequence of SEQ ID NO:4 or SEQ ID NO: 5.

53. The method of claim 19, the at least one heavy chain variable region (VH region) comprising: (a) three CDRs from any one of SEQ ID NOs: 74-83 and 778-956; or (b) any one of SEQ ID NOs: 74-83 and 778-956.

54. The method of claim 19, the at least one light chain variable region (VL region) comprising: (a) three CDRs from any one of SEQ ID NOs: 84-93 and 957-1052; or (b) any one of SEQ ID NOs: 84-93 and 957-1052.

55. The method of claim 19, the at least one heavy chain variable region (VH region) comprising: (a) three CDRs from any one of SEQ ID NOs: 74-83, 778-956; or (b) the sequence of any one of SEQ ID NOs: 74-83 and 778-956; and the at least one light chain variable region (VL region) comprising: (c) three CDRs from any one of SEQ ID NOs: 84-93 and 957-1052; or (d) the sequence of any one of SEQ ID NOs: 84-93 and 957-1052.

56. The method of claim 55, wherein the VH region comprises the sequence of SEQ ID NO: 74 and the VL region comprises the sequence of SEQ ID NO: 84.