TREA

Anti-PD-L1 antibody for detecting PD-L1

Follow

Information

  • Patent Grant
  • 10865246
  • Patent Number
    10,865,246
  • Date Filed
    Friday, March 23, 2018
    6 years ago
  • Date Issued
    Tuesday, December 15, 2020
    4 years ago
Information
Abstract
The present invention provides an anti-PD-L1 antibody capable of staining tumor cells such as melanoma cells.
Description
PRIORITY APPLICATIONS

This application is a U.S. National Stage Filing under 35 U.S.C. 371 from International Application No. PCT/JP2018/011895, filed on Mar. 23, 2018, and published as WO2018/181064 on Oct. 4, 2018, which claims the benefit of priority to Japanese Application No. 2017-061389, filed on Mar. 27, 2017; the benefit of priority of each of which is hereby claimed herein, and which applications and publication are hereby incorporated herein by reference in their entirety.


TECHNICAL FIELD

The present invention relates to an anti-PD-L1 antibody for detecting PD-L1.


BACKGROUND ART

Malignant melanoma originating from melanocytes is one of the most commonly observed malignant tumors in the canine oral cavity (Non-Patent Document No. 1: Todoroff et al., J Am Vet Med Assoc. 1979 Sep. 15: 175(6):567-71). Since this type of melanoma generally tends to be highly invasive and metastatic, early diagnosis and treatment are desired. On the other hand, malignant melanoma has a wide tissue variation, presenting various morphologies such as epithelial-like, round cell-like or fibrosarcoma-like morphology. Thus, malignant melanoma is one of those tumors which involve difficulty in tissue diagnosis. Although confirmation of melanin pigment is important for their diagnosis, a large number of malignant melanomas do not have melanin pigment and, sometimes, diagnosis cannot be made with histological observations alone. This has led to searches for diagnostic markers that can be used in immunohistochemical techniques. Among such markers, Melan A/MART-1, vimentin, S100, neuron-specific enolase and the like have been reported to be useful (Non-Patent Document No. 2: Ramos-Vara et al., Vet Pathol. 2000 November; 37(6):597-608). However, even Melan A/MART-1, the most widely used diagnostic marker, has a positive rate not higher than about 60% which varies among reports (Non-Patent Document No. 3: Koenig et al., Vet Pathol. 2001 July; 38(4):427-35). Because of this sensitivity problem, the utility of Melan A/MART-1 in actual diagnosis is still arguable. Further. Melan A/MART-1 is not stained in amelanotic melanoma (Non-Patent Document No. 3: Koenig et al., Vet Pathol. 2001 July; 38(4):427-35), so its application to diagnosis is limited. Under these circumstances, it is desired to develop highly sensitive, novel diagnostic markers to malignant melanoma.


PRIOR ART LITERATURE
Non-Patent Documents

Non-Patent Document No. 1: Todoroff et al., J Am Vet Med Assoc. 1979 Sep. 15; 175(6):567-71


Non-Patent Document No. 2: Ramos-Vara et al., Vet Pathol. 2000 November; 37(6):597-608


Non-Patent Document No. 3: Koenig et al., Vet Pathol. 2001 July; 38(4):427-35


DISCLOSURE OF THE INVENTION
Problem for Solution by the Invention

It is an object of the present invention to provide a PD-L1 antibody capable of staining tumor cells such as melanoma cells.


Means to Solve the Problem

The present inventors have established a number of monoclonal antibodies which react with the PD-L1 protein of various animals. It has been revealed that, among those monoclonal antibodies, a rat anti-bovine PD-L1 monoclonal antibody (6C11-3A11) is capable of staining melanoma tumor cells very strongly. Currently, this monoclonal antibody is used for selecting candidate dogs for therapy with chimeric antibodies. The subject PD-L1 antibody (6C11-3A11) is also capable of immunohistochemically staining ovine, porcine and bovine PD-L1 proteins. Further, the present inventors have determined the CDRs (complementarity-determining regions) of the variable regions of the subject PD-L1 antibody (6C11-3A11). The present invention has been achieved based on these findings.


A summary of the present invention is as described below.

  • (1) An anti-PD-L1 antibody comprising (a) a light chain comprising CDR1 having the amino acid sequence of KSISKY (SEQ ID NO: 1), CDR2 having the amino acid sequence of SGS and CDR3 having the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2) and (b) a heavy chain comprising CDR1 having the amino acid sequence of GYTFTDYI (SEQ ID NO: 3), CDR2 having the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and CDR3 having the amino acid sequence of ARGITMMVVISHWKFDF (SEQ ID NO: 5).
  • (2) The antibody of (1) above, which is derived from rat.
  • (3) The antibody of (2) above, which is a rat anti-bovine PD-L1 antibody.
  • (4) The antibody of (3) above, wherein the light chain variable region has the amino acid sequence as show in SEQ ID NO. 6 and the heavy chain variable region has the amino acid sequence as shown in SEQ ID NO: 7.
  • (5) The antibody of any one of (1) to (4) above, wherein the light chain constant region has the amino acid sequence of the constant region of kappa chain.
  • (6) The antibody of any one of (1) to (5) above, wherein the heavy chain constant region has the amino acid sequence of the constant region of IgG2a.
  • (7) The antibody of (5) or (6) above, wherein the light chain constant region has the amino acid sequence as shown in any one of SEQ ID NOS: 8, 10 to 12 and the heavy chain constant region has the amino acid sequence as shown in SEQ ID NO: 9 or 13.
  • (8) The antibody of anyone of (1) to (7) above which has a four-chain structure comprising two light chains and two heavy chains.
  • (9) A composition for detecting PD-L1, comprising the antibody of any one of (1) to (8) above as an active ingredient.
  • (10) The composition of (9) above for use in diagnosis of cancers and/or inflammations.
  • (11) The composition of (10) above, wherein the cancers and/or inflammations are selected from the group consisting of neoplastic diseases, leukemia, Johne's disease, anaplasmosis, bacterial mastitis, mycotic mastitis, mycoplasma infections (such as mycoplasma mastitis, mycoplasma pneumonia or the like), tuberculosis, Theileria orientalis infection, cryptosporidiosis, coccidiosis, trypanosomiasis and leishmaniasis.
  • (12) The composition of (9) above for use in selecting subject animals suitable for therapy with anti-PD-L1 antibodies.
  • (13) A DNA encoding the anti-PD-L1 antibody of (1) above.
  • (14) A vector comprising the DNA of (13) above.
  • (15) A host cell transformed with the vector of (14) above.
  • (16) A method of preparing an antibody, comprising culturing the host cell of (15) above and collecting an anti-PD-L1 antibody from the resultant culture.
  • (17) A DNA encoding the light chain of an anti-PD-L1 antibody, said light chain comprising CDR1 having the amino acid sequence of KSISKY (SEQ ID NO: 1), CDR2 having the amino acid sequence of SGS and CDR3 having the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2).
  • (18) A DNA encoding the heavy chain of an anti-PD-L1 antibody, said heavy chain comprising CDR1 having the amino acid sequence of GYTFTDYI (SEQ ID NO: 3), CDR2 having the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and CDR3 having the amino acid sequence of ARGTMMVVISHWKFDF (SEQ ID NO: 5).


Effect of the Invention

According to the present invention, a novel anti-PD-L1 antibody capable of staining tumor cells, such as melanoma cells, has been obtained.


The present specification encompasses the contents disclosed in the specification and/or the drawings of Japanese Patent Application No. 2017-61389 based on which the present patent application claims priority.





BRIEF DESCRIPTION OF THE DRAWINGS

The patent or application file contains at least one drawing executed in color. Copies of this patent or patent application publication with color drawing(s) will be provided by the Office upon request and payment of the necessary fee.



FIG. 1 Binding specificity of rat anti-bovine PD-L1 antibody 6C11-3A11. Rat anti-bovine PD-L1 antibody 6C11-3A11 did not bind to EGFP expressing cells, but specifically bound to canine PD-L1-EGFP expressing cells.



FIG. 2 Predicted CDR regions of rat anti-bovine PD-L1 antibody 6C11-3A11. The regions of CDR1. CDR2 and CDR3 in the light chain variable region and the heavy chain variable region of rat anti-bovine PD-L1 antibody 6C1-3A11 are shown.



FIG. 3 Comparative immunohistochemical staining images of canine melanoma. Left: stained with a commercial antibody (MelanA antibody). Tumor cells were stained very weakly. Right: stained with the PD-L1 antibody 6C11-3A11 established by the present inventors. Tumor cells were stained very strongly.



FIG. 4 Immunohistochemical staining image of canine melanoma.



FIG. 5-1 Immunohistochemical staining images of other tumors. Upper left: case of canine lymphoma. Upper right: case of canine osteosarcoma. Lower left: case 1 of canine renal cell carcinoma. Lower right: case 2 of canine renal cell carcinoma.



FIG. 5-2 Immunohistochemical staining images of other tumors. Left: case of canine squamous cell carcinoma. Right: case of canine fibrosarcoma.



FIG. 6 Immunohistochemical staining image of a case of ovine listeriosis. Left: PD-L1 staining image of a brain lesion of ovine listeriosis exhibiting neurologic symptoms. Right: enlarged photograph of the left image.



FIG. 7 Immunohistochemical staining images of porcine infections. Left: case of porcine circovirus type 2 infection. Right: case of porcine mycoplasma pneumonia.



FIG. 8 Alignment of amino acid sequences of the constant region of rat Ig kappa chain (light chain).



FIG. 9 Alignment of amino acid sequences of the constant region of rat IgG2a chain (heavy chain).



FIG. 10 Schematic drawing of pDC6 vector and a rat-human chimeric anti-PD-L1 antibody.



FIG. 11 Binding of rat anti-bovine PD-L1 antibodies 6C11-3A11 and 6G7-E1 to canine PD-L1-EGFP expressing cells. 6C11-3A11 specifically bound to canine PD-L1-EGFP expressing cells.



FIG. 12 Immunohistochemical staining images of skin squamous cell carcinoma, nasal adenocarcinoma and transitional cell carcinoma in dogs. No specific signals were detected with 6G7-E1. Tumor cells were stained with 6C11-3A11.



FIG. 13 Immunohistochemical staining images of anal sac gland carcinoma, soft tissue sarcoma and osteosarcoma in dogs. In anal sac gland carcinoma and soft tissue sarcoma, no specific signals were detected with 6G7-E1, but tumor cells were stained with 6C11-3A11. In osteosarcoma, both antibodies stained tumor cells, but stronger signals were obtained with 6C11-3A11.



FIG. 14 Immunohistochemical staining images of oral malignant melanoma, mammary adenocarcinoma, histiocytic sarcoma, diffuse large B-cell lymphoma and transmissible venereal tumor in dogs using 6C11-3A11. In the tumor species other than transmissible venereal tumor, PD-L1 on tumor cells was stained.



FIG. 15 Binding of rat anti-bovine PD-L1 antibody 6C11-3A11 to bovine PD-L1-EGFP expressing cells. 6C11-3A11 specifically bound to bovine PD-L1-EGFP expressing cells.



FIG. 16 Immunohistochemical staining images of ileal lesions of cattle naturally and experimentally infected with Mycobacterium avium subsp. paratuberculosis, using (a) 6C11-3A11 and (b) Ziehl-Neelsen staining. 6C11-3A11 detected PD-L1 expression in cells infected with M. avium subsp. paratuberculosis (positive in Ziehl-Neelsen staining).





BEST MODES FOR CARRYING OUT THE INVENTION

Hereinbelow, the present invention will be described in detail.


The present invention provides an anti-PD-L1 antibody comprising (a) a light chain comprising CDR1 having the amino acid sequence of KSISKY (SEQ ID NO: 1), CDR2 having the amino acid sequence of SGS and CDR3 having the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2) and (b) a heavy chain comprising CDR1 having the amino acid sequence of GYTFTDYI (SEQ ID NO: 3), CDR2 having the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and CDR3 having the amino acid sequence of ARGITMMVVISHWKFDF (SEQ ID NO: 5).


CDR1, CDR2 and CDR3 in the light chain variable region (VL) of rat anti-bovine PD-L1 antibody 6C11-3A11 (monoclonal antibody) established by the present inventors are a region consisting of the amino acid sequence of KSISKY (SEQ ID NO: 1), a region consisting of the amino acid sequence of SGS and a region consisting of the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2), respectively (see FIG. 2).


Further. CDR1, CDR2 and CDR3 in the heavy chain variable region (VH) of rat anti-bovine PD-L1 antibody 6C1-3A1 are a region consisting of the amino acid sequence of GYTFTDYI (SEQ ID NO: 3), a region consisting of the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and a region consisting of the amino acid sequence of ARGITMMVVISHWKFDF (SEQ ID NO: 5), respectively (see FIG. 2).


In the amino acid sequences of KSISKY (SEQ ID NO: 1), SGS and QQHNEYPLT (SEQ ID NO: 2), as well as the amino acid sequences of GYTFTDYI (SEQ ID NO: 3), INPDSGGN (SEQ ID NO: 4) and ARGITMMVVISHWKFDF (SEQ ID NO: 5), one, two, three, four or five amino acids may be deleted, substituted or added. Even when such mutations have been introduced, the resulting amino acid sequences are capable of having the function as CDR of VL or CDR of VH of the PD-L1 antibody.


As used herein, the term “antibody” is a concept encompassing not only full-length antibodies but also antibodies of smaller molecular sizes such as Fab, F(ab)′2. ScFv, Diabody, VH, VL. Sc(Fv)2, Bispecific sc(Fv)2, Minibody, scFv-Fc monomer and scFv-Fc dimer.


The anti-PD-L1 antibody of the present invention may be derived from rat. For example, the anti-PD-L1 antibody may be a rat anti-bovine PD-L1 antibody.


The amino acid sequence of the VL and the amino acid sequence of the VH of rat anti-bovine PD-L1 antibody 6C11-3A11 (monoclonal antibody) are shown in SEQ ID NOS: 6 and 7, respectively. The amino acid sequences as shown in SEQ ID NOS: 6 and 7 may have deletion(s), substitution(s) or addition(s) of one or several (e.g., up to five, about 10 at the most) amino acids. Even when such mutations have been introduced, the resulting amino acid sequences are capable of having the function as VL or VH of the PD-L1 antibody.


There are two types of immunoglobulin light chain, which are called Kappa chain (κ) and Lambda chain (λ). In the anti-PD-L1 antibody of the present invention, the light chain constant region (CL) may have the amino acid sequence of the constant region of either Kappa chain or Lambda chain. However, the relative abundance of Lambda chain is higher in ovine, feline, canine and equine, and that of Kappa chain is higher in mouse, rat, human and porcine. Rat anti-bovine PD-L1 antibody 6C11-3A11 (monoclonal antibody) is a rat-derived IgG2a, and the CL thereof has the amino acid sequence of the constant region of Kappa chain.


The heavy chain constant region (CH) of the anti-PD-L1 antibody of the present invention may have the amino acid sequence of the constant region of rat IgG2a. Immunoglobulin heavy chain is classified into γ chain, μ chain, α chain, δ chain and ε chain depending on the difference in constant region. According to the type of heavy chain present, five classes (isotypes) of immunoglobulin are formed, they are IgG, IgM, IgA, IgD and IgE.


Immunoglobulin G (IgG) accounts for 70-75% of human immunoglobulins and is the most abundantly found monomeric antibody in plasma. IgG has a four-chain structure consisting of two light chains and two heavy chains. Human IgG1, IgG2 and IgG4 have molecular weights of about 146,000, whereas human IgG3 has a long hinge region that connects Fab region and Fc region and has a larger molecular weight of 170,000. Human IgG1 accounts for about 65%, human IgG2 about 25%, human IgG3 about 7%, and human IgG4 about 3% of human IgG. They are uniformly distributed inside and outside of blood vessels. Having a strong affinity for Fc receptors and complement factors on effector cell surfaces, human IgG1 induces antibody-dependent cell cytotoxicity (ADCC) and also activates complements to induce complement-dependent cell cytotoxicity (CDC). Human IgG2 and IgG4 are low at ADCC and CDC activities because their affinity for Fc receptors and complement factors is low.


Immunoglobulin M (IgM), which accounts for about 10% of human immunoglobulins, is a pentameric antibody consisting of five basic four-chain structures joined together. It has a molecular weight of 970,000. Usually occurring only in blood, IgM is produced against infectious microorganisms and takes charge of early stage immunity.


Immunoglobulin A (IgA) accounts for 10-15% of human immunoglobulins. It has a molecular weight of 160,000. Secreted IgA is a dimeric antibody consisting of two IgA molecules joined together. IgA1 is found in serum, nasal discharge, saliva and breast milk. In intestinal juice, IgA2 is found abundantly.


Immunoglobulin D (IgD) is a monomeric antibody accounting for no more than 1% of human immunoglobulins. IgD is found on B cell surfaces and involved in induction of antibody production.


Immunoglobulin E (IgE) is a monomeric antibody that occurs in an extremely small amount, accounting for only 0.001% or less of human immunoglobulins. Immunoglobulin E is considered to be involved in immune response to parasites but in advanced countries where parasites are rare. IgE is largely involved in bronchial asthma and allergy among other things.


With respect to rat, sequences of IgG1, IgG2a, IgG2b and IgG2c have been identified as the heavy chain of IgG. Rat anti-bovine PD-L1 antibody 6C11-3A11 has the amino acid sequence of the CH of IgG2a.


In the antibody of the present invention, it is more preferable that the CL has the amino acid sequence of the constant region of Kappa chain and that the CH has the amino acid sequence of the constant region of IgG2a.


The amino acid sequence and the nucleotide sequence of the VL of rat anti-bovine PD-L1 antibody 6C11-3A1 identified by the present inventors are shown in SEQ ID NOS: 6 and 14, respectively.


The amino acid sequence and the nucleotide sequence of the VH of rat anti-bovine PD-L1 antibody 6C11-3A11 identified by the present inventors are shown in SEQ ID NOS: 7 and 15, respectively.


The amino acid sequence and the nucleotide sequence of the CL (Kappa chain) of rat anti-bovine PD-L1 antibody 6C11-3A11 identified by the present inventors are shown in SEQ ID NOS: 8 and 16, respectively. These sequences are identical with the sequences registered at GenBank (a nucleotide sequence database provided by National Center for Biotechnology Information (NCBI)) under accession numbers #XM_008775358.2. #BC062802.1, #3C088255.1, #L22653.1. #L22655.1 and #M14434.1.


The amino acid sequence and the nucleotide sequence of the CH (IgG2a) of rat anti-bovine PD-L1 antibody 6C11-3A11 identified by the present inventors are shown in SEQ ID NOS: 9 and 17, respectively. These sequences are identical with the sequences registered at GenBank under accession numbers #BC088240.1. #BC091257.1. #BC091272.1. #BC088423.1, #L22652.1 and #L22654.1.


Amino acid sequences and nucleotide sequences of CLs and CHs for rat antibodies other than the above may be obtained from known databases for use in the present invention.


As an amino acid sequence and a nucleotide sequence of rat Ig Kappa chain, the sequence registered at GenBank under accession number #V01241.1 is shown in SEQ ID NOS: 10 and 18.


As an amino acid sequence and a nucleotide sequence of rat Ig Kappa chain, the sequence registered at GenBank under accession number #X16129.1 is shown in SEQ ID NOS: 11 and 19.


As an amino acid sequence and a nucleotide sequence of rat Ig Kappa chain, the sequence registered at GenBank under accession number #DQ402471.1 is shown in SEQ ID NOS: 12 and 20.


As the CH of rat IgG2a, the sequence registered at GenBank under accession number #DQ402472.1 is shown in SEQ ID NOS: 13 and 21.


The anti-PD-L1 antibody of the present invention may be an anti-PD-L1 antibody in which the CL has the amino acid sequence as shown in any one of SEQ ID NOS: 8 and 10 to 12 and the CH has the amino acid sequence as shown in SEQ ID NO: 9 or 13.


The amino acid sequences as shown in SEQ ID NOS: 8 to 13 may have deletion(s), substitution(s) or addition(s) of one or several (e.g., up to five, about 10 at the most) amino acids. Even when such mutations have been introduced, the resulting amino acid sequences are capable of having the function as CL or CH of the PD-L antibody.


Alignments of amino acid sequences of the CL and the CH of a rat anti-PD-L1 antibody are shown in FIG. 8 and FIG. 9, respectively. The above-described mutations such as deletion, substitution or addition of amino acids may suitably have occurred at the mutation sites as shown in FIGS. 8 and 9 or at the vicinity thereof.


The anti-PD-L1 antibody of the present invention may be a chimeric antibody. The VL and the VH of the antibody may be suitably derived from rat. For example, the VL may be the VL of a rat anti-PD-L1 antibody (e.g., 6C11-3A11); the VH may be the VH of a rat anti-PD-L1 antibody, and the CL and the CH may be derived from an animal other than rat. For example, when a rat antibody is chimerized using the constant regions of a mouse antibody, the resulting chimeric antibody will be useful for testing and diagnosis because various secondary antibodies to mouse antibodies are commercially available. Amino acid sequences and nucleotide sequences of the CLs and the CHs of antibodies of animals other than rat may be obtained from known databases for use in the present invention.


Amino acid sequences and nucleotide sequences of CLs and CHs for human, mouse, bovine, canine, ovine, porcine and water buffalo are summarized in the table below.
















TABLE












GenBank









Accession















Species
Ig Domain
Nucleotide Sequence
Amino Acid Sequence
No.
IMGT Database
Reference

















Human
Human
IgG4
GCACCTGAGTTCCTGGCGGGAOCATCAGTCTTCCTC
KPKDTLMISRTPEVTCVCCDVSQEDPE
K01316
http://www.
Ellison


(Scientific
Ig
variant
TTCCCCCCAAAACCCAAGGACACTCTCATGATCTCC
VQFNWYVDCVEVHNAKTKPREEGFNS

imgt.org/
J. et al


Name:
heavy
1
GGGACCGCTGAGGTCACGTGCGTGGTGGTGGACGTG
TYRWSVLTVLHQDWLNGKEYKCKVS

IMGT
DNA, 1



Homo

chain

AGGCAGGAAGACCCCGAGGTCCAGTTCAACTGGTAC
NKGLPSSIEKTISKAKGQPREPQVYTLP

reportoire/
11-16



sapiens)
re-

GTGGATGGCGTGGAGGTGCATAATGCCAAGACAAAG
PSGEEMTKNQVSLTCLVKGFYPSDIAV

index.
(1981)



gion

CCGCGGGAGGAGCAGTTCAACAGCACGTACCGTGTG
EWESNGQPENNYKTTPPVLDSDGSFFL

ghp?section
PMID:



(CH1

GTCAGCGTCCTCACCGTCCTGCACCAGGACTGGCTG
YSRLTVDKSRWQEGNVFSCSVMHEAL

=locus
6299662



CH3)

AACGGCAAGGAGTACAAGTGCAAGGTCTCCAACAAA
HNHYTQKSLSLSLGK*

Genes&






GGCCTCCCGTCCTCCATCGAGAAAACCATCTCCAAA
(SEQ ID NO: 30)

reportoire=






GCCAAAGGGCAGCCCCGAGAGCCACAGGTGTACACC


genetable&






CTGCCCCCATCCCAGGAGGAGATGACCAAGAACCAG


species=






GTCAGCCTGACCTGCCTGGTCAAAGGCTTCTACCCC


human&






AGCGACATCGCCGTGGAGTGGGAGAGCAATGGGCAG


gcf=IGHC






CCGGAGAACAACTACAAGACCACGCCTCCCGTGCTG









GACTCCGACGGCTCCTTCTTCCTCTACAGCAGGCTA









ACCGTGGACAAGAGCAGGTGGCAGGAGGGGAATGTC









TTCTCATGCTCCGTGARGCATGAGGCTCTGCACAAC









CACTACACACAGAAGAGCCTCTCCCTGTCTCTGGGT









AAATGA









(SEQ ID NO: 31)








IgG4
GAGTCCAAATATGGTCCCCCGTGGCCATCATGGCCA
ESKYGPPCPSCPAPEFLGGPSVFLFPP
AJ001583

Brusco




variant
GCACCTGAGTTCCTGGGGGGACCATCAGTCTTCCTG
KPKDTLMISRTPEVTCVVVDVSGEDPE


A. et al.




2
TTCCCCCCAAAACCCAAGGACACTCTGATGATCTCC
VQFNWYVDGVEVHNAKTKPREEQFNS


Eur. J.





CGGACCCCTGAGGTCACGTGCGTGGTGGTGGACGTG
TYRVVSVLTVVHQDWLNGKEYKCKVS


Immuno





AGCCAGGAAGACCCCGAGGTCCAGTTCAACTGGTAC
NKGLPSSIEKTISKAKGQPREPQVYTLP


genol.,





GTGGATGGCGTGGAGGTGCATAATGCCAAGACAAAG
PSQEEMTKNQVSLTCLVKGFYPSDIAV


25,





CCGCGGGAGGAGCAGTTCAACAGCACGTACCGTGTG
EWESNGQPENNYKTTPPVLDSDGSFFL


348-355 





GTCAGCGTGCTCACGGTCGTGCACCAGGACTGGCTG
YSRLTVDKSRWQEGNVFSCSVMHEAL


(1998).





AACGGCAAGGAGTACAAGTGCAAGGTCTCCAACAAA
HNHYTQKSLSLSLGK*


PMID:





GGCCTCCCGTCCTCCATCGAGAAAACCATCTCCAAA
(SEQ ID NO: 32)


9805657





GCCAAAGGCCACCCCCGAGAGCCACAGCTGTACACC









CTGCCCCCATCCCAGGAGGAGATGACCAAGAACCAG









GTCAGCCTGACCTGCCTGGTCAAAGGCTTCTACCCC









AGCGACATCGCCGTGGAGTGGGAGAGCAATGGGCAG









CCGGAGAACAACTACAAGACCACGCCTCCCGTGOTG









GACTCCGACGGCTCCTTCTTCCTCTACAGCAGGCTA









ACGGTGGACAAGAGCAGGTGGCAGGAGGGGAATGTC









TTCTCATGCTCCGTGATGCATGAGGCTCTGCACAAC









CACTACACGCAGAAGAGCCTCTCCCTGTCTCTGGGT









AAATGA









(SEQ ID NO: 33)








IgG4
GCACCTGAGTTCCTGGGGGGACCATCAGTCTTCCTG
APEFLGGPSVFLFPPKPKDTLMISRTPE
AJ001564






variant
TTCCCCCCAAAACCCAAGGACACTCTCATGATCTCC
VTCVVVDVSQEDPEVQFNWYVDGVEV







3
CGGACCCCTGAGGTCACGTCCGTGGTGGTGGACGTG
HNAKTKPREEQFNSTYRVVSVLTVLHQ








AGCCAGGAAGACCCCGAGGTCCAGTTCAACTGGTAC
DWLNGKEYKCKVSNKGLPSSIEKTISKA








GTGGATGGCGTGGAGGTGCATAATGCCAAGACAAAG
KGQPREPQVYTIPPSQEEMTKNQVSL








CCGCGGGAGGAGCAGTTCAACAGCACGTACCGTGTG
TCLVKGFYPSDIAVEWESNGQPENNYK








GTCAGCGTCCTCACCGTCCTGCACCAGGACTGGCTG
TTPPVLDSDGSFFLYSKLTVDKSRWQE








AACGGCAAGGAGTACAAGTGCAAGGTCTCCAACAAA
GNVFSCSVMHEALHNHYTQKSLSLSLG








GGCCTCCCGTCCTCCATCGAGAAAACCATCTCCAAA
K*








GCCAAAGGGCAGCCCCGAGAGCCACAGGTGTACACC
(SEQ ID NO 34)








CTGCCCCCATCCCAGGAGGAGATGACCAAGAACCAG









GTCAGCCTGACCTGCGTGGTCAAAGGCTTCTACCCC









AGCGACATCGCGGTGGAGTGGGAGAGCAATGGGCAG









CCGGAGAACAACTACAAGACCACGCCTCCCGTGCTG









GACTCCGACGGCTCCTTCTTCCTCTACAGCAAGCTC









ACCGTGGACAAGAGCAGGTGGCAGGAGGGGAACGTC









TTCTCATGCTCCGTGATGCATGAGGCTCTGCACAAC









CACTACACGCAGAAGAGCCTCTCCCTGTCTCTGGGT









AAATGA









(SEQ ID NO: 33)







Human
Ig
ACTGTGGCTGCACCATCTGTCTTCATCTTCCCGCCA
TVAAPSVFIFPPSDEQLKSGTASVVCL
X96754
http://www.
GL



Ig
kappa
TCTGATGAGCAGTTGAAATCTGGAACTGCCTCTGTT
LNNFYPRCAKVQWKVDNALQSGNSQE

imgt.org/




light
(CK)
GTGTGCCTGCTGAATAACTTCTATCCCAGAGAGGCC
SVTEQDSKDSTYSLSSTLTLSKAQYEK

IMGT




con-

AAAGTACAGTGGAAGGTGGATAACGCCCTCCAATCG
HKVYACEVTHQCLSSPVTKSFNRGEC*

reportoire/




stant

GGTAACTCCCAGGAGAGTGTCACAGAGCAGGACAGG
(SEQ ID NO: 28)

index.




region

AAGGACAGCACCTACAGCCTCAGCAGGACCCTGACG


ghp?section






CTGAGCAAAGCAGACTACGAGAAACACAAAGTCTAC


=locus






GCCTGCGAAGTCACCCATCAGGGCCTGAGCTCGCCC


Genes&






GTCACAAAGAGCTTCAACAGGGGAGAGTGTTAG


reportoire=






(SEQ ID NO: 29)


genetable&









species=









human&









gcf=IGHC






Mouse
Mouse
IgG1
GCCAAAACGACACCCCCATCTGTCTATCCACTGGCCC
AKTTPPSVYPLAPGSAAQTNSMVTLG
J00453
http://www.
Honjo T.


(Scientific
Ig
variant
CTGGATCTGCTGCCCAAACTAACTCCATGGTGACCCT
CLVKGYFPEPVTVTWNSGSLSSGVHTF
AH005309
imgt.org/
et al.


Name: Mus
heavy
1
GGGATGCCTGGTCAAGGGCTATTTCCCTGAGCCAGT
PAVLESDLYTLSSSVTVPSSPRPSETV
V00793
IMGT
Ceit



Musculus)
chain

GACAGTGACCTGGAACTCTGGATCCCTGTCCAGCGG
TCNVAHPASSTKVDKKIVPRDCGCKPC
D78344
reportoire/
18, 558-



region

TGTGCACACCTTCCCAGCTGTCCTGGAGTCTGACCTC
ICTVPEVSSVFIFPPKPKDVLTITLTPK

index.
568 (1979)



(CH1

TACACTCTGAGCAGCTCAGTGACTGTCCCCTCCAGCC
VTCVVVDISKDDPEVQFSWFVDDVEVHT

ghp?section
PMID:



CH3)

CTCGGCCCAGCGAGACCGTCACCTGCAACGTTGCCC
AQTQPREEQFNSTFRSVSELPIMHQDW

=locus
115593





ACCCGGCGACCAGCACCAAGGTGGACAAGAAAATTG
LNGKEFKCRVNSAAFPAPIEKTISKTKG

Genes&
Akohoni Y.





TGCCCAGGGATTGTGGTTGTAAGCCTTGCATATGTAC
RPKAPQVYTIPPPKEQMAKDKVSLTCM

reportoire=
and





AGTCCCAGAAGTATCATCTGTCTTCATCTTCCCCCCA
ITDFFPEDITVEWQWNGQPAENYKNTQ

genetable&
Kursawa Y.





AAGCCCAAGGATGTGCTCACCATTACTCTCACTCCTA
PIMNTNGSYFVYSKLNVQKSNWEAGNT

species=
Genomes,





AGGTCACGTGTGTTGTGGTAGACATCAGCAAGGATGA
FTCSVLHEGLHNHHTEKSLSHSPGK

human&
41, 100-





TCCCGAGGTCCAGTTCAGCTGGTTTGTAGATGATGTG
(SEQ ID NO: 44)

gcf=IGHC
104 (1997)





GAGGTGCACAGAGCTCAGACGCAAGCGCGGGAGGAG



PMID:





GAGTTCAACAGCACTTTGGGCTCAGTCAGTGAACTTC



9126488





CCATCATGCACCACGACTGCCTCAATCGCAAGCAGTT









CAAATGCAGGGTCAACAGTCCAGCTTTCCCTGCCCCC









ATCGAGAAAACCATCTCCAAAACCAAAGGCAGACCG









AAGGCTCCACAGGTGTACAGCATTCCACCTCCCAAGG









AGCAGATGGCCAAGGATAAAGTCAGTCTGACCTGCAT









GATAACAGACTTCTTCCCTGAAGACATTACTGTGGAG









TCGCACTGGAATGCGCAGCCAGCCGAGAACTACAAG









AACACTCAGCCCATCATGAACACGAATGGCTCTTACT









TCGTCTACAGCAAGCTCAATGTGCAGAAGAGCAACTG









GGAGGCAGGAAATACTTTCACCTGCTCTGTGTTACAT









GAGGGCCTGCACAACCACCATACTGAGAAGAGCCTC









TCCCACTCTCCTGGTAAATGA









(SEQ ID NO: 45)








IgG1
GCCAAAAGGACACCCCCATCTGTCTATCCACTGGCCC
AKTTPPSVYPLAPGSAAQTNSMVTLG
L35252

Honjo T.




variant
CTGGATCTGCTGCCCAAACTAACTCCATGGTGACCCT
CLVKGYFPEPVTVTWNSGSLSSGVHTF


et al,




2
GGCATGCCTGGTCAAGGGCTATTTCCCTGACCCAGT
PAVLQSDLYTLSSSVTVPSSTWSQTV


Ceit, 18





GACACTGACCTGGAACTCTGGATCCCTGTCCAGCGG
TCNVAHPASSTKVDKKIVPRDCGCKPC


558-568





TGTGCACACCTTCCCAGCTGTCCTGCAGTCTGACCTC
ICTVPEVSSVFIFPPKPKDVLTITLTPK


(1979)





TACACTCTGAGCAGCTCAGTGACTGTCCCCTCCAGCA
VTCVVVDISKDDPEVQFSWFVDDVEVHT


PMID:





CCTGGCCCAGCCAGACCGTCACCTGCAACGTTGCCC
AQTKPREEQINSTFRSVSELPIMHQDWL


115593





ACCCGGCCAGCAGCACCAAGGTCGACAAGAAAATTG
NGKEFKCRVNSAAFPAPIEKTISKTKGR








TGCCCAGGGATTGTGGTTGTAAGCCTTGCATATGTAC
PKAPQVYTIPPPKEQMAKDKVSLTCMI








AGTCCCAGAAGTATCATCTGTCTTCATCTTCCCCCCA
TNFFPEDITVEWQNGQPAENYKNTQP








AAGCCCAAGGATGTGCTCACCATTACTCTGACTCCTA
IMDTDGSYFVYSKLNVQKSNWEAGNTF








AGGTCACGTGTGTTGTGGTAGACATCAGCAAGGATGA
TCSVLHEGLHNHHTEKSLSHSPGK








TCCCGAGGTCCAGTTCAGCTGGTTTGTAGATGATGTG
(SEQ ID NO: 46)








GAGGTGCACACAGCTCAGACGAAACCCCGGGAGGAG









CAGATCAACAGCACTTTCCGTTCAGTCAGTGAACTTC









CCATCATGCACCAGGACTGGCTCAATGGCAAGGAGTT









CAAATGCAGGGTCAACAGTGCAGCTTTCCCTGCCCCC









ATCGAGAAAACCATCTCCAAAACCAAAGGCAGACCG









AAGGCTCCACAGGTGTACACCATTCCACCTCCCAAGG









AGCAGATGGCCAAGGATAAAGTGAGTGTGACCTGCAT









GATAACAAACTTGTTCCCTGAAGAGATTACTGTGGAG









TGGCAGTGGAATGGGCAGCCAGCGGAGAACTACAAG









AACACTCAGCCCATCATGGACACAGATGGCTCTTACT









TTCGTCTACAGCAAGCTCAATGTGCAGAAGAGCAACTG









GGAGGCAGGAAATACTTTCACCTCCTCTGTGTTACAT









TGAGGGCCTGCACAACCACCATACTGAGAAGAGCCTC









TCCCACTCTCCTGGTAAATGA









(SEQ ID NO: 47)








IgG2a
GCCAAAACAACAGCCCCATCGGTCTATCCACTGGCC
AKTTAPSVYPLAPVCGDTTGSSVTLGC
J00470

Yamawaki




variant
CCTGTGTGTGGAGATACAACTGGCTCCTCGGTGACTC
LVKGYFPEPVTLTWNSGSLSSGVHTFP
AH003509

Kataska




1
TAGGATGCCTGGTCAAGGGTTATTTCCCTGAGCCAGT
AVLQSDLYTLSSSVTVTSSTWPSQSIT
V00825

Y. et al,





GACCTTGACCTGGAACTCTGGATCCCTGTCCAGTGGT
CNVAHPASSTKVDKKIEPRGPTIKPCPP
V00766

Nucleic





GTGCACACCTTCCCAGCTGTCCTGCAGTCTGACCTCT
CKCPAPNLLGGPSVFFPPKIKDVLMISL
D78344

Acids





ACACCCTCAGCAGCTCAGTGACTGTAAGCTCGAGCAC
SPIVTCVVVDVSEDDPDVQISWFVNNV


Res. 9,





CTCGCCCAGCCAGTCCATCACCTGCAATGTGGCCCA
EVHTAQTQTHREDYNSTLRVVSALPIQ


1365-1381





CCCGGCAAGCAGCACCAAGGTGGACAAGAAAATTGA
HQDWMSGKEFKCKVNNKDLPAPIERTI


(1981).





GCCCAGAGGGCCCACAATCAAGCCCTGTCCTCCATG
SKPKGSVRAPQVYVLPPPEEEMTKKQV


PMID:





CAAATGCCCAGCACCTAACCTCTTGGGTGGACCATCC
TLTCMVTDFMPEDIYVEWTNNGKTELN


6262729





GTCTTCATCTTCCCTCCAAAGATCAAGGATGTACTCA
YKNTEPVLDSDGSYFMYSKLRVEKKNE


Oto F. et





TGATCTCCCTGAGCCCCATAGTCACATCTGTGGTGGT
VERNSYSCSVVHEGLHNHHTTKSFSRT


al, Proc





GGATGTGAGCGAGGATGACCCAGATGTCCAGATGAG
PGK


Natl.





CTGGTTTGTGAACAACGTGGAAGTACACACAGCTCAG
(SEQ ID NO: 48)


Acad Sci.





ACACAAACCCATAGAGAGGATTACAACAGTACTCTCC



U.S.A, 78,





GGGTGGTCAGTGCCCTCCCCATCCAGCACCAGGACT



2442-2446





GGATGAGTGGCAAGGAGTTCAAATGCAAGGTCAACA



(1981),





ACAAAGACCTCCCAGCGCCCATGGAGAGAACCATCT



PMID:





CAAAACCCAAAGGGTGAGTAAGAGGTCCACAGGTATA



0787604





TGTCTTGCCTCCACCAGAAGAAGAGATGACTAAGAAA



Sikorev J.





CAGGTCACTCTGACCTGCATGGTCACAGACTTCATGC



et al,





CTGAAGACATTTACGTGGAGTGGACCAACAACGGGA



Nucleic





AAACAGAGCTAAACTACAAGAACACTGAACCAGTCCT



Acids Res.





GGACTCTGATGGTTCTTACTTCAFGTACAGCAAGCTG



8, 3143-





AGAGTGGAAAAGAAGAACTGGGTGGAAAGAAATAGC



3155 (1980)





TACTCCTGTTCAGTGGTCCACGAGGGTCTGCACAATC



PMID:





ACCACACGACTAAGAGCTTCTCCCGGACTCCGGGTA



6777755





AATGA



Akahon Y.





(SEQ ID NO: 49)



and









Kurwaska









Y.









Genomic,









41, 100-









104 (1997)









PMID:









9128488




IgG2a
GCCAAAACAACAGCCCCATCGGTCTATCCACTGGCC
AKTTAPSVYPLAPVCGDTTGSSVTLGC
X16997

Morgado




variant
CCTGTGTGTGGAGATACAACTGGCTCCTCGGTGACTC
LVKGYFPEPVTLTWNSGSLSSGVHTFP


M.G. et




2
TAGGATGCCTGGTCAAGGGTTATTTCCCTGAGCCAGT
AVLQSDLYTLSSSVTVTSSTWPSQSIT


al, EMBO





GACCTTGACCTGGAACTCTGCATCCCTGTCCAGTGGT
CNVAHPASSTKVDKKIEPRGPTIKPCPP


J. S.





GTACACACCTTCCCAGCTGTCCTGCAGTCTGACCTCT
CKCPAPNLLGGPSVFIFPPKIKDVLMIS


3245-





ACACCCTCAGCAGCTCAGTGACTGTAACCTCGAGCAC
LSPMVTCVVVDVSEDDPDVQISWFVNN


3251 





CTGGCCGACCCAGTCGATCACCTGCAATGTGGCCCA
VEVLTAQTQTHREDYNSTLRVVSALPI


(1989)





CCGGGCAAGCAGCACCAAGGTGGACAAGAAAATTGA
QHQDWMSGKEFKCKVNNKALPAPIERT


PMID:





GCCCAGAGGGCCCACAATCAAGCCCTGTCCTCCATG
ISKPKGSVRAPQVYVLPPPEEEMTKKQ


2510996





CAAATGCCCAGCACCTAACCTCTTGGGTGGACCATCC
VTLTCMVTDFMPEDIYVEWTNNGKTEL








GTCTTCATCTTCCCTCCAAAGATCAAGGATGTACTCA
NYKNTEPVLDSDGSYFMYSKLRVEKKN








TGATCTCCCTGACTCCCATGCTCACATGTGTGGTGGT
WVERNSYSCSVVHEGLHNHHTTKSFSR








GGATGTGAGCGAGGATGACCCAGATGTCCAGATCAG
TPGK








CTGGTTCGTGAACAACGTGGAAGTACTCACAGCTCAG
(SEQ ID NO: 50)








ACACAAACCCATAGAGAGGATTACAACAGTACTCTCC









GGGTGGTCAGTGCCCTCCCCATCCAGCACCAGGACT









TGGATGAGTGGCAAGGAGTTCAAATGCAAGGTCAACA









ACAAAGCCCTCCCAGCGCCCATCGAGAGAACCATCT









TCAAAACCCAAAGGGTCAGTAAGAGCTCCACAGGTATA









TGTCTTGCCTCCACCAGAAGAAGAGATGACTAAGAAA









CAGGTCACTCTGACCTGCATGGTCACAGACTTCATGC









CTGAAGACATTTACGTGGAGTGGACCAACAACGGGA









AAACAGAGCTAAACTACAAGAACACTCAACCAGTCCT









GGACTCTGATGGTTCTTACTTCATGTACACCAAGCTG









AGAGTGGAAAAGAAGAACTGGGTGGAAAGAAATAGC









TACTCCTGTTCAGTGGTCCACGAGGGTCTGCACAATC









ACCACACGACTAAGAGCTTCTCCCGGACTCCGGGTA









AATGA









(SEQ ID NO: 51)








IgG2b
GCCAAAACAACACCCCCATCAGTCTATCGACTGGCCC
AKTTPPSVYPLAPGCGDTTGSSVYLGG
J00461

Yamawaki




variant
CTGGGTGTGGAGATACAACTGGTTCCTCCGTGACTCT
LVKGYFPESVTVTVWSGSLSSSVHTFP
AH005300

Kataoka Y.




1
GGGATGCCTGGTCAAGGGCTACTTCGCTGAGTCAGT
ALLQSGLYTMSSSVTVPSSTWPSQTVT
V00801

et al,





GACTGTGACTTGGAACTCTGGATCCCTGTCCAGCAGT
CSVAHPASSTTVDKKLEPSGPISTINPC
D78344

Nature,





GTGCACACCTTCCGAGCTCTCCTGCAGTCTGGACTCT
PPCKECHKCPAPNLEGGPSVFIFPPNIK


283,





ACACTATGAGCAGCTCAGTGACTGTCCCCTCCAGCAC
DVLMISLTPKVTCVVVDVSEDDPDVQI


786-789





TTTGGCCAAGTCAGACCGTCACCTGCAGCGTTGCTCAC
SWFVNNVEVHTAQTQTHREDYMSTIRV


(1980)





CGAGGCAGCAGCACCACGGTGGACAAAAAACTTGAG
VSTLPIQHQDWMSGKEFKCKVNNKDLP


PMID:





CCCAGCGGGCCCATTTCAAGAATCAACGCCTGTCCTC
SPIERTISKIKGLVRAPQVYILPPPAEQ


6766534





GATCCAAGGAGTGTCACAAATGCCCAGCTCCTAACCT
LSRKDVSLTCLVVGFNPGDISVEWTSNG


Oilo R.





CGAGGGTGGACCATCCGTCTTCATCTTCCCTCCAAAT
HTEENYKDTAPVLDSDGSYFIYSKLNM


and





ATCAAGGATGTACTCATGATCTCCCTGACACCCAAGG
KTSKWEKTDSFSCNVRHEGLKNYYLKK


Raugeon F.





TCACGTGTGTGGTGGTGGATGTGAGCGAGGATGACC
TISRSPGK


Nature,





CAGACGTCCAGATCAGCTGGTTTGTGAACAACGTGGA
(SEQ ID NO: 52)


298, 761-





AGTACACACAGCTCAGACACAAACCCATAGAGAGGAT



763 (1982)





TACAACAGTACTATCCGGGTGGTCAGCACCCTCCGCA



PMID:





TCCAGCACCAGGACTGGATGAGTGGCAAGGAGTTCA



6803173





AATGCAAGGTCAACAACAAAGACCTCCCATCACCCAT



Akahon Y





CGAGAGAACCATCTCAAAAATTAAAGGGCTAGTCAGA



and





GCTCCACAAGTATACATCTTGCCGCCACCAGCAGAGC



Kurosawa





AGTTGTCCAGGAAAGATGTCAGTCTCACTTGCCTGGT



Y





CGTGGGCTTCAACCCTGGAGACATCAGTGTGGAGTG



Genomics,





GACCAGCAATGGGCATACAGAGGAGAACTACAAGGA



41, 100-





CACCGCACCAGTCCTAGACTCTGACGGTTCTTACTTC



104 (1997)





ATATATAGCAAGCTCAATATGAAAACAAGCAAGTGGG



PMID:





AGAAAACAGATTCCTTCTCATGCAACGTGAGACACGA



9126488





GGGTCTGAAAAATTACTACCTGAAGAAGACCATCTCC









CGGTCTCCGGGTAAATGA









(SEQ ID NO: 53)








IgG2b
GCCAAAACAACACCCCCATCAGTCTATCCACTGGCCC
AKTTPPSVYPLAPGCGDTTGSSVTSG
V00763

Tuckor




variant
CTGGGTGTGGAGATAGAACTGGTTCCTCCGTGACCTC
CLVKGYFPEPVTVTWNSGSISSSVHTF


P.W. et




2
TGGGTGCCTGGTCAAGGGGTACTTCCCTGAGCCAGT
PALLQSGLYTMSSSVTVPSSTWPSQTV


al,





GACTGTGACTTGGAACTCTGGATCCCTGTCCAGCAGT
TCSVAHPASSTTVDKKLEPSGPISTINP


Science





GTGCACACCTTCCCAGCTCTCCTGCAGTCTGGACTCT
CPPCKECHKCPAPNLEGGPSVFIFPPNI


206





ACACTATGAGCAGCTCAGTGACTGTCCCCTCCAGCAC
KDVLMISLTPKVTCVVVDVSEDDPDVQ


1303-1306





CTGGCCAAGTCAGACCGTCACCTGCAGCGTTGGTCA
ISWFVNNVEVHTAQTQTHREDYNSTIRV


(1979)





CCCAGCCAGCAGCACCACGGTGGACAAAAAACTTGA
VSTLPIQHQDWMSGKEFKCKVNNKDLP


PMID





GCCCAGCGGGCCCATTTCAACAATCAACCCCTGTCCT
SPIERTISKIKGLVRAPQVYTLPPPAEQ


117549





CCATGCAAGGAGTGTCACAAATGCCCAGCTCCTAACC
LSRKDVSLTCLVVGFNPGDISVEWTSNG








TCGAGGGTGGACCATCCGTCTTCATCTTCCCTCCAAA
HTEENYKDTAPVLDSDGSYFIYSKLNM








TATCAAGGATGTACTCATGATCTCCCTGACACCCAAG
KTSKWEKTDSFSCNVRHEGLKNYYLKK








GTCACGTGTGTGGTGGTGGATGTGAGCGAGGATGAC
TISRSPGK








CCAGACGTCCAGATCAGCTGGTTTGTGAAGAACGTGG
(SEQ ID NO: 54)








AAGTACACACAGCTCAGACACAAACCCATAGAGAGG









ATTACAACAGTACTATCCGGGTGGTGAGCACCCTCCC









CATCCAGCACCAGGACTGCATGAGTGGCAAGGAGTT









CAAATGCAAGGTGAACAACAAAGACCTCCCATCACCC









ATCGAGAGAACCATCTCAAAAATTAAAGGGCTAGTCA









GAGCTCCACAAGTATACACTTTGCCGCCACCAGCAGA









GCAGTTGTCCAGGAAAGATGTCAGTCTCACTTGCCTG









GTCGTGGGCTTCAACCCTGGAGACATCAGTGTGGAGT









GGACCACCAATGGGCATACAGAGGAGAACTACAAGG









ACACCGCACCAGTTCTTGACTCTGACGGTTCTTACTT









CATATATAGCAAGCTCAATATGAAAACAAGCAAGTGG









GAGAAAAGAGATTCCTTCTCATGCAACGTGAGACACG









AGGGTCTGAAAAATTACTACCTGAAGAAGACCATCTC









CCGGTCTCCGGGTAAATGA









(SEQ ID NO: 55)








IgG2c
GCCAAAACAACAGCCCCATCGGTCTATCCACTGGCC
AKTTAPSVYPLAPVCGGTTGSSVTLGC
J00479

Olio R.




variant
CCTGTGTGTGGAGGTACAACTGGCTCCTCGGTCACTC
LVKGYFPEPVTLTWNSGSLSSGVHTFP


and




1
TAGGATGCCTGGTCAAGGGTTATTTCCCTGAGCCAGT
ALLQSGLYTLSSSVTVTSNTWPSQTIT


Rougeon F.





GACCTTGACCTGGAACTCTGGATCCCTGTCCAGTGGT
CNVAHPASSTKVDKKIEPRVPITQNPCP


Cell, 32





GTGCACACCTTCCCAGCTCTCCTGCAGTCTGGCGTCT
PLKECPPCAAPDLLGGPSVFIFPPKIKD


515-523





ACACCCTCAGCAGCTCAGTGACTGTAACCTCGAACAC
VLMISLSPMVTCVVVDVSEDDPDVQIS


(1983).





CTGGCCCAGCCAGACCATCACCTGCAATGTGGCCCA
WFVNNVEVHTAQTQTHREDYNSTLRV


PMID:





CCCGGCAAGCAGCACCAAAGTGGACAAGAAAATTGA
VSALPIQHQDWMSGKEFKCKVNNRALP


6297797





GCCCAGAGTGCCCATAACACAGAACCGGTGTCCTCC
SPIEKTISKPRGPVRAPQVYVLPPPAEE








ACTCAAAGAGTGTCCCCCATGCGCAGCTCCAGACCT
MTKKEFSLTCMITGFLPAEIAVDWTSNG








CTTGGGTGGACCATCCGTCTTCATCTTCCCTCCAAAG
RTEQNYKNTATVLDSDGSYFMYSKLRV








ATCAAGGATGTACTCATGATCTCCCTGAGCCCCATGG
QKSTWERGSLFACSVVHEVLHNHLTTK








TCACATGTGTGGTGGTGGATGTGAGCGAGGATGACC
TISRSLGK








CAGACGTCCAGATCAGCTGGTTTGTGAACAACGTGGA
(SEQ ID NO: 56)








AGTACACACAGCTCAGACACAAACCCATAGAGAGGAT









TACAACAGTACTCTCCGGGTGGTGAGTGCCCTCCCCA









TCCAGCACCAGGACTGGATGAGTGGCAAGGAGTTCA









AATGCAAGGTCAACAACAGAGCCCTCCCATCCCCCAT









CGAGAAAACCATCTCAAAACCCAGAGGGCCAGTAAG









AGCTCCACAGGTATATGTCTTGGCTCCACCAGCAGAA









GAGATGACTAAGAAAGAGTTCAGTCTGACCTGCATGA









TCACAGGCTTCTTACCTGCCGAAATTGCTGTGGACTG









GACCAGCAATGGGCGTACAGAGGAAAACTACAAGAA









CACCGCAACAGTCCTGGACTCTGATGGTTCTTACTTC









ATGTACAGCAAGCTCAGAGTACAAAAGAGCACTTGGG









AAAGAGGAAGTCTTTTCGCCTGCTCAGTGGTCCACGA









GGTGCTGCACAATCACCTTACGACTAAGACCATCTCC









CGGTCTCTGGGTAAATGA









(SEQ ID NO: 57)








IgG2c
GCCAAAACAACAGCCCCATCGGTCTATCCACTGGCC
AKTTAPSVYPLAPVCGGTTGSSVTLGC
X16998

Morgado




variant
CCTGTGTGTGGAGGTACAACTGGCTCCTCGGTGACTC
LVKGYFPEPVTLTWNSGSLSSGVHTFP


M.G. et




2
TAGGATGCCTGGTCAACGGTTATTTCCCTGAGCCAGT
ALLGSGLYTLSSSVTVTSNTWPSQTIT


al., EMBO





GACCTTGACCTGGAACTCTGGATCGCTGTCCAGTGGT
CNVAHPASSTKVDKKIESRRPIPPNSCP


J. 8,





GTGCACACCTTCCCAGCTCTCCTGCAGTCTGGCCTCT
PCKECSIFPAPDLLGGPSVFIFPPKIKD


3245-3251





ACACCCTGAGCAGCTCAGTGACTGTAACCTCGAACAC
VLMISLSPIVTCVVVDVSEDDPDVQISW


(1989).





CTGGCCCAGCCAGACCATCACCTGCAATGTGGCGCA
FVNNVEVHTAQTQTHREDYNSTLRVVS


PMID:





CCCGGCAAGCAGCACCAAAGTGGACAAGAAAATTGA
ALPIQHQDWMSGKEFKCKVNNRALPSP


2510996





ATCCAGAAGGCCCATACCACCCAACTCCTGTCCTCCA
IEKTISKPRGPVRAPQVYVLPPPAEEMT








TGCAAAGAGTGTTCCATATTCCCAGCTGCTGACCTCT
KKEFSLTCMITDFLPAEIAVDWTSMGHK








TGGGTGGACCATCCGTCTTCATCTTCCCTCCAAAGAT
ELNYKNTAPVLDTDGSYFMYSKLRVQK








CAAGGATGTACTCATGATCTCCCTGAGCCCCATAGTC
STWEKGSLFACSVVHEGLHNHHTTKTI








ACATGTGTGGTGGTGGATGTGAGCGAGGATGACCCA
SRSLGK








GATGTCCAGATCAGCTGGTTTGTGAACAACGTGGAAG
(SEQ ID NO: 58)








TACACACAGCTCAGACACAAACCCATAGAGAGGATTA









CAACAGTACTCTCCCGGTGGTCAGTGCCCTCCCCATC









CAGCACCAGGACTGGATGAGTGGCAAGGAGTTCAAA









TGCAAGGTCAACAACAGAGCCCTCCCATCCCCCATC









GAGAAAACCATCTCAAAACCCAGAGGGCCAGTAAGA









GCTCCACAGGTATATGTCTTGCGTCGACGAGCAGAAG









AGATGACTAAGAAAGAGTTCAGTCTGAGCTGCATGAT









CACAGACTTCTTACCTGCCGAAATTGCTGTGGACTGG









ACCAGCAATGGGCATAAAGAGCTGAACTACAAGAACA









CCGCACCAGTCCTGGACACTGATGGTTCTTACTTCAT









GTACAGCAAGCTCAGAGTGCAAAAGAGCACTTGGGA









AAAAGGAAGTCTTTTCGCCTGCTCAGTGGTCCACGAG









GGTCTGCACAATCACCATACGACTAAGACCATCTCCG









GGTCTCTGGGTAAATGA









(SEQ ID NO: 59)








IgG2c
GCCAAAACAACAGCCCCATCGGTCTATCCACTGGCC
AKTTAPSVYPLAPVCGGTTGSSVTLGC
Y10606

Martin R.M




variant
CCTGTGTGTCGAGGTACAACTGGCTCCTCGGTGACTC
LVKGYFPEPVTLTWNSGSLSSGVHTFP


et al,




3
TAGGATGCCTGGTCAAGGGTTATTTCGCTGAGCCAGT
ALLQSGLYTLSSSVTVTSNTWPSQTIT


Immuno-





GACCTTGACCTGGAACTCTGGATCCCTGTCCAGTGGT
CNVAHPASSTKVDKKIEPRVPITGNPCP


genics, 46,





GTGCACACCTTCCCAGCTCTCCTGCAGTCTGGCCTCT
PLKECPPCAAPDLLGGPSVFIFPPKIKD


157-168





ACAGGCTCAGCAGCTCAGTGACTGTAACCTCGAACAC
VLMISLSPMVTCVVVDVSEDDPDVQIS


(1997).





CTGGCCCAGCCAGACCATCACCTGCAATGTGGCCCA
WFVNNVEVHTAQTQTHREDYNSTLRV


PMID:





CCCGGCAAGCAGCACCAAAGTGGACAAGAAAATTGA
VSALPIQHQDWMSGKEFKCKVNNRALP


9162106





GGCCAGAGTGCCCATAACACAGAACCCCTGTCCTCC
SPIEKTISKPRGPVRAPQVYVLPPPAEE








ACTCAAAGAGTGTCCCCCATGCGCAGCTCCAGACCT
MTKKEFSLTQMITGFLPAEIAVDWTSNG








CTTGGGTGGACCATCCGTCTTCATCTTCCCTCCAAAG
RTEQNVKNTATVLDSDGSYFMYSKLRV








ATCAAGGATGTACTCATGATCTCCCTGAGCCCCATGG
QKSTWERGSLFACSVVHEGLHNHLTTK








TCACATGTGTGCTGCTGGATGTGAGCGAGGATGACC
TISRSLGK








CAGACGTCCAGATCAGCTGGTTTGTGAACAACGTGGA
(SEQ ID NO: 60)








AGTACACACAGCTCAGACAGAAACCCATAGAGAGGAT









TACAACAGTACTCTCCGGGTGGTCAGTGCCCTCCCCA









TCCAGCACCAGGACTGGATGAGTGGCAAGGAGTTCA









AATGCAAGGTCAACAACAGAGCCCTCCCATCCCGCAT









CGAGAAAACCATCTCAAAACCCAGAGGGCCAGTAAG









AGCTCCACAGGTATATGTCTTGGCTCCACCAGCAGAA









GAGATGACTAAGAAAGAGTTCAGTCTGACCTGCATGA









TCACAGGCTTCTTACCTGCCGAAATTGCTGTGGACTG









GACCAGCAATGCGCGTACAGAGCAAAACTACAAGAA









CACCGCAACAGTCCTGGACTCTGATGGTTCTTACTTC









ATGTACAGCAAGCTCAGAGTACAAAAGAGCACTTGGG









AAAGAGGAAGTCTTTTCGCCTGCTCAGTGGTCCACGA









GGGTCTGCACAATCACCTTACGACTAAGACCATCTCC









CGGTCTCTGGGTAAATGA









(SEQ ID NO: 61)








IgG3
GCTACAACAACAGCCCCATCTGTCTATCCCTTGGTCC
ATTTAPSVYPLVPGCSDTSGSSVTLGC
J00451

Stanton





CTGGCTGCAGTGACACATCTGGATGCTCGGTGACACT
LVKGYFPEPVTVKVNWYGALSSGVRTVS
AH005309

L.W.





GGGATGCCTTGTCAAAGGCTACTTCCCTGAGCCGGTA
SVLQSGFYSLSSLVTVPSSTWPSQTVI
X00915

and Marcus





ACTGTAAAATGGAACTATGGAGCCCTGTCCAGCGGTG
CNVAHPASKTELIKRIEPRIPKPSTPPG
D78343

K.B.





TGCGCACAGTCTCATCTGTCCTGCAGTCTGGGTTCTA
SSCPPGNILGGPSVFIFPPKPKDALMIS


Nucleic





TTGCGTCAGCAGCTTGGTGACTGTACCCTCCAGCACC
LTPKVTCVVVDVSEDDPDVHVSWFVDN


Acids Res.





TGGCCCAGCCAGACTGTCATCTGCAACGTAGCCCAC
KEVHTAWTQPREAQYNSTFRVVSALPI


10, 5993-





CCAGCGAGCAAGACTGAGTTGATCAAGAGAATCGAG
QHQDWMRGKFFKCKVNNKALPAPIERT


6006 (1982)





CCTAGAATACCCAAGCCCAGTACGCCCCCAGGTTCTT
ISKPKGRAQTPQVYTIPPPREQMSKKK


PMID:





CATGCCCACCTGGTAACATCTTGGGTGGACCATCCGT
VSLTCLVTNFFSEAISVEWWRNGELEQD


629864





CTTCATCTTCCCCCCAAAGCCCAAGGATGCACTCATG
YKNTPPILDSDGTYFLYSKLTVDTDSWL


Wels J.A.





ATCTCCCTAACCCCCAAGGTTACGTGTGTGGTGGTGG
QGEIFTCSVVHEALHNHHTQKNLSRSP


et al,





ATGTGAGCGAGGATGACCCAGATGTCCATGTCAGCTG
GK


EMBO J.





GTTTGTGGACAACAAAGAAGTACACACAGCCTGGACA
(SEQ ID NO: 62)


2041-2046





CAGCCGCGTGAAGGTCAGTACAACAGTACCTTCCGA



(1984)





GTGGTCAGTGCCCTCCCCATCCAGCACCAGGACTGG



PMID:





ATCAGGGGCAAGGAGTTCAAATGCAAGGTCAACAAC



6092053





AAAGCCCTCCCAGCCCCCATCGAGAGAACCATCTCA



Akahoni Y.





AAACCCAAAGGAAGAGCCCAGACACCTCAAGTATAC



and





ACCATACCCCCACCTCGTGAACAAATGTCCAAGAAGA



Kurosawa





AGGTTAGTCTGACCTGCCTGGTCACCAACTTCTTCTC



Y.





TGAAGCCATCAGTGTGGAGTGGGAAAGGAACGGAGA



Genomics,





ACTGGAGCAGGATTACAAGAACAGTCCAGCCATCCTG



41, 100-





GACTCAGATGGGACCTACTTCCTCTACAGCAACCTCA



10 (1997)





CTGTGGATACAGACAGTTGGTTGCAAGGAGAAATTTT



PMID:





TACCTGCTCCGTGGTGCATGAGGCTCTCCATAACCAC



9126498





CACACACAGAAGAACCTGTCTCGCTGCCCTGGTAAAT









GA









(SEQ ID NO: 63)







Mouse
Ig
GCTGATGCTGGACCAACTGTATCCATCTTCCCACCAT
ADAAPTVSIFPPSSEQLTSGGASVVCF
V00807
http://www.
Hieter



Ig
kappa
CCAGTGACCAGTTAACATCTGCACGTGCCTCAGTCGT
LNNFYPKDINVKWKIDGSERQNGVLNS
V00777
imgt.org/
P.A. et



light
(CK)
GTGCTTCTTGAAGAACTTCTACCCCAAAGACATCAAT
WTDQDSKDSTYSMSSTLTLTKDEYERH
V01569
IMGT
al. Cell,



con-

GTCAAGTGGAAGATTGATGGCAGTGAACGACAAAATG
NSYTCEATHKTSTSPIVKSFNRNEC
V00806
reportoire/
22, 197-



stant

GCGTCCTGAACAGTTGGACTGATCAGGACAGCAAAG
(SEQ ID NO: 36)
X67002
index.
207 (1980)



region

ACAGCACCTACAGCATGAGCAGCACCCTCACGTTGA

X67003
ghp?section
PMID:





CCAAGGACGAGTATGAACGAGATAACAGCTATACCTG

X67004
=locus
6775818





TGAGGCCACTCACAAGACATCAACTTCACCCATTGTC

X67005
Genes&
Max E.E





AAGAGCTTCAACAGGAATGAGTGTTAC

X67006
reportoire=
et al. J.





(SEQ ID NO: 37)

X67007
genetable&
Bio. Chem,







X67008
species=
256, 5116-







X67009

mus musculus&
5120 (1981)







X670010
group=IGKC
PMID:







X670011

6262318







X670012

Seidman









J.G. et al,









Nature,









280, 370-









375 (1979)









PMID:









111146









Solin M.L.









and









Kaartnen M.









Immuno-









genics, 37









401-407









(1983)









PMID:









8436414




Ig
GGCCAGCCCAAGTCTTCGCCATCAGTCACCCTGTTTC
GQPKSSPSVTLFPFSSEELETNKATLV
J00587
http://www.
Selsing E.




lambda
CACCTTCCTCTGAAGAGCTCGAGACTAACAAGGCCAC
CTITDFYPGVVTVDWKVDGTPVTQGME
AH005311
imgt.org/
et al. Proc




1 (CL)
ACTGCTGTGTACGATCACTCATTTCTACCCAGGTGTG
TTQPSKQSNNKYMASSYLTLTARAWER
X58411
IMGT
Natl. Acad





GTGACAGTGGACTGGAAGGTACATCCTACCCCTGTC
HSSYSCQVTHEGHTVEKSLSRADCS
V00814
reportoire/
Sci USA.





ACTCAGGGTATGGAGACAACCCAGCCTTGCAAACAG
(SEQ ID NO: 38)

index.
79, 4681-





AGCAACAAGAAGTACATGGCTAGCAGCTACCTGACCC


ghp?section
4685 (1982)





TGACAGCAAGACCATGGGAAAGGCATAGCAGTTACA


=locus
PMID:





GCTGCCAGGTCACTCATGAAGGTCACACTGTGGAGA


Genes&
8812053





AGAGTTTGTGCCGTGCTGACTGTTCCTAG


reportoire=
Weiss S.





(SEQ ID NO: 39)


genetable&
and W GE.








species=
EMBO J.









mus musculus&
6, 927-








group=IGKC
937 (1987)









PMID:









3105891









Bernard O.









et al.









Cell, 15,









1133-









144 (1978)









PMID:









103630





GGTCAGCCCAAGTCCACTCCCACTCTCACGGTGTTTC
GQPKSTPTLTVTPPSSEELKENKATLV
J00595

Selsing E.





CACCTTCCTCTGAGGAGCTCAAGGAAAAGAAAGCCAC
CLISNFSPSGVTVAWKANGTPITQGVD
AH001968

et al. Proc





ACTGGTGTGTCTGATTTCCAACTTTTCCCCGAGTGGT
TSNPTKEDNKYMASSFLHLTSDQWRSH
J00592

Natl. Acad





GTGACAGTGGCCTGGAAGGCAAATGGTACACCTATCA
NSFTCQVTHEGDTVEKSLSPAECL
AH001967

Sci USA.





CCCAGGGTGTGGACACTTCAAATCCCACCAAAGAGG
(SEQ ID NO: 40)
X58414

79, 4681-





GCAACAAGTTCATGGCCACCAGCTTCCTACATTTGAC



4685 (1982)





ATCGCACCAGTGGAGATCTCACAACAGTTTTACCTGT



PMID:





CAAGTTACACATGAAGCGGACAGTGTCGAGAAGAGT



8812053





CTGTCTCCTGGAGAATGTCTGTAA



Wu G.









et al, Cell









33, 77-









83 (1983)





(SEQ ID NO: 41)



PMID:









3109691





GGTCAGGCCAAGTGCACTCCCACACTGAGCATGTTTG
GQPKSTPTLTMFPPSSEELQENKATLV
J00585

Selsing E.





CACCTTCCCCTGAGGAGCTCCAGGAAAACAAAGCCA
CLISNFSPSGVTVAWKANGTPITQGVD
AH005311

et al. Proc





CACTCCTGTGTCTGATTTCCAATTTTTCCCCAAGTGG
TSNPTKEDNKYMASSFLHLTSDQWRSH
X58415

Natl. Acad





TGTGACAGTGGCCTGGAAGGCAAATGGTACACCTATC
NSFTCQVTHEGDTVEKSLSPAECL
X58411

Sci USA.





ACCCAGGGTGTGGACAGTTCAAATCCCACCAAAGAG
(SEQ ID NO: 42)


79, 4681-





GACAACAAGTACATGGGCAGCAGGTTCTTACATTTGA



4685 (1982)





CATCGGAGCAGTGGAGATCTCACAACAGTTTTAGCTG



PMID:





CCAAGTTACACATGAAGGGGACACTGTGGAGAAGAG



8812053





TCTGTCTCCTGCAGAATGTCTGTAA



Weiss S.





(SEQ ID NO: 43)



and W GE.









EMBO J.









6, 927-









937 (1987)









PMID:









3105891





Bovine
Bovine
IgG1
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGAGTTC
ASTTAPKVYPLSSCCGDKSSSTVTLGC
X62916
http://www.
Symons D.B


(Scientific
Ig
variant
TTGCTGCGGGGACAAGTCCAGCTCCACCGTGACCCTGG
LVSSYMPEPVTVTWNSGALKSGVHTFP

imgt.org/
et a;. J.


Name: Bos
heavy
1
GCTGCCTGGTCTCCAGCTACATGCCCGAGCCGGTGACC
AVLQSSGLYSLSSMVTVPGSTSGQTFT

IMGT
Immuno-



taurus)
chain

GTGACCTGGAACTCGGGTGCCCTGAAGAGCGGGGTGCA
CNVAHPASSTKVDKAVDPTCKPSPCD

reportoire/
genes, 14,



con-

CACCTTCCCGGCTGTCCTTCAGTCCTCCGGGCTGTACT
CCPPPELPGGPSVFIFPPKPKDTLTISG

index.
273-283



stant

CTCTCAGCAGCATGGTGACCGTGCCCGGCAGCACCTCA
TPEVTCVVVDVGHDDPEVKFSWFVDD

ghp?section
(1987)



region

GGACAGACCTTCACCTGCAACGTAGCCCACCCGGCCAG
VEVNTATTKPREEQFNSTYRVVSALRI

=locus
PMID:



(CH1

CAGCACCAAGGTGGACAAGGCTGTTGATCCCACATGCA
QHQDWTGGKEFKCKVHNEGLPAPIVRT

Genes&
341517



CH3)

AACCATCACCCTGTGACTGTTGCCCACCCCCTGAGCTC
ISRTKGPAREPQVYVLAPPQEELSKST

reportoire=
Symons D.B





GCCGGAGGACCCTCTGTCTTCATCTTCCCACCGAAACC
VSLTCMVTSFYPDYIAVEWQRNGQPES

genetable&
et al, Mol.





CAAGGACACCCTCAGAATCTCGGGAACGCCCGAGGTCA
EDKYGTTPPQLDADSSYFLYSKLRVDR

species=
Immno., 26





CGTGTGTGGTGGTGGAGGTGGGCCACGATGACCCCGAG
NSWQEGDTYTCVVMHEALHNHYTQKS


bovine taurus

341-350





GTGAAGTTCTCCTGGTTCGTGGACGACGTGGAGGTAAA
TSKSAGK*

&group=IGKC
(1989)





CACAGCCACGACGAAGCCCAGAGAGGAGCAGTTCAACA
(SEQ ID NO: 66)


PMID:





GCACCTACCGCGTGGTCAGCGCCCTGCGCATCCAGCAC



2513487





CAGGACTGGACTGGAGGAAAGGAGTTCAAGTGCAAGGT



Kacksovics





CCACAACGAAGGCCTCCCGGCCCCCATCGTGAGGACGA



I. and





TCTCCAGGACCAAAGGGCCGGGCCGCGAGCCGCAGGT



Butler J.E.





GTATGTCCTGGCCCCACCCCAGGAAGAGCTCAGCAAAA



Mol.





GCACGGTCAGCCTCACCTGCATGGTCACCAGCTTCTAC



Immunol, 33





CCAGACTACATCGCCGTGGAGTGGCAGAGAAAGGGGCA



189-195





GCCTGAGTCGGAGGACAAGTACGGCACCACCCCCGCC



(1999)





CAGCTGGACGCCGACAGCTCCTACTTCCTCTACAGCAA



PMID:





GCTCAGGGTGGACAGGAACAGCTGGCAGGAAGGAGAC



8849440





ACCTACACGTGTGTGGTGATGCACGAGGCCCTGCACAA



Rabbani H.





TCACTACACGCAGAAGTCCACCTCTAAGTCTGCGGGTA



et al.





AATGA



Immuno-





(SEQ ID NO: 67)



genetics,









46, 328-









331 (1997)









PMID:









9218535









Saini S.S.









et al









Searol J.









Immunol.









65, 32-8









(2007)









PMID:









17212754




IgG1
GGCTCCAGGACAGGCGCGAAAGTCTAGCCTGTGAGTTC
ASTTAPKVYPLSSCCGDKSSSTVTLGC
X16701






variant
TTGCTGCGGGGACAAGTCCAGCTCCACCGTGACCCTGG
LVSSYMPEPVVTVWNSGALKSGVHTFP
(M25278)






2
GCTGCCTGGTCTCCAGCTACATGCCCGAGCCGGTCACC
AVLQSSGLYSLSSMVTVPGSTSGQTFT








GTGACCTGGAACTCGGGTGCCCTGAAGAGCGGGGTGCA
CNVAHPASSTKVDKAVDPTCKPSPCD








CACCTTCCCCGCCGTCCTTCAGTCCTCCGGGCTGTACT
CCPPPELPGCPSVFIFPPKPKDTLTISG








CTCTCAGGAGCATGGTGACCGTGCCCGGCAGCACCTCA
TPEVTCVVVDVGHDDPEVKFSWFVDD








GGACAGAGCTTCACGTGCAACGTAGCCCACCCGGCCAG
VEVNTATTKPREEQFNSTYRVVSALRI








CAGCACCAAGGTGGACAAGGCTGTTGATCCCACATGCA
QHQDWTGGKEFKCKVHNEGLPAPIVRT








AACCATCACCCTGTGACTGTTGCCCACCCCCTGAGCTC
ISRTKGPAREPQVYVLAPPQEELSKST








CGCGGAGGACCCTCTGTCTTCATCTTCCCACCGAAACC
VSLTCMVTSFYPDYIAVEWQRNGQPES








CAAGCACACCCTCACAATCTCCGCAACGCCCGAGGTCA
EDKYGTTPPQLDADSSYFLYSKLRVDR








CGTGTGTGCTGCTGGACGTGGGCCACCATGACCCCGAG
NSWQEGDTYTCVVMHEALHNHYTQKS








GTGAAGTTCTCCTGGTTCGTGGACGACGTGGAGGTAAA
TSKSAGK*








CACAGCCACGACGAAGCCGAGAGAGGAGCAGTTCAACA
(SEQ ID NO: 68)








GCACCTACCGCGTGGTCAGCGCCCTGCGCATCCACCAC









CAGGACTGGACTGGAGGAAAGGAGTTCAAGTGCAAGGT









CCACAACGAAGGCCTCCCGGCCCCCATCGTGAGGACCA









TCTCCAGGACCAAAGGGCCGGCCCGGGAGCCCCAGGT









GTATGTCCTGGCCCCACCCCAGGAAGAGCTCAGCAAAA









GCACCGTCAGCCTCACCTGCATGGTCACCACCTTCTAC









CCAGACTACATCGCCGTGGACTGGCAGACAAACGGGCA









GCCTGAGTCGGAGGACAAGTACGGCACGACCCCGGGC









CAGCTGGACGCCGACAGCTCCTACTTCCTGTACAGCAA









GCTCAGGGTGGACAGGAACAGCTGGCAGGAAGGAGAC









ACCTACACGTCTGTGGTGATGCACGAGGCCCTCCACAA









TCACTACACGCAGAAGTCCACCTCTAAGTCTGCGGGTA









AATGA









(SEQ ID NO: 69)








IgG1
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGAGTTC
ASTTAPKVYPLSSCCGDKSSSTVTLGC
S82407






variant
TTGCTGCGGGGACAAGTCCAGCTCCACCGTGACCCTGG
LVSSYMPEPVTVTWNSGALKSGVHTFP







3
GCTGCCTGGTCTCCAGCTACATGCCCGAGCCGGTGACC
AVLQSSGLYSLSSMVTVPGSTSGTQTF








GTGACCTGGAACTCGGGTGCCCTGAACAGCGGCGTGCA
TCNVAHPASSTKVDKAVDPRCKTTGD








CACCTTCCCGGCCGTCCTTCAGTCCTCCGGGCTCTACT
CCPPPELPGGPSVFIFPPKPKDTLTISG








CTCTCAGCAGCATGGTGACCGTGCCCGGCAGCACCTCA
TPEVTCVVVDVGHDDPEVKFSWFVDD








GGAACCCAGACCTTCACCTGCAACGTAGCCCACCCGGC
VEVNTATTKPREEQFNSTYRVVSALRI








CAGCAGCACCAAGGTGGACAAGGCTGTTGATCCCAGAT
QHQDWTGGKEFKCKVHNEGLPAPIVRT








GCAAAACAACCTGTGACTGTTCCCCACCGCCTGAGCTC
ISRTKGPAREPQVYVLAPPQEELSKST








CCTGGAGGACCCTCTGTCTTCATCTTCCCACCGAAACC
VSLTCMVTSFYPDYIAVEWQRNGQPES








CAAGGACACGCTCACAATCTCGGGAACGCCCGAGGTCA
EDKYGTTPPQLDADGSYFLYSRLRVDR








CGTGTGTGGTGGTGGACGTGGGCCACGATGACCCCGAG
NSWQEGDTYTCVVMHEALHNHYTQKS








GTGAAGTTCTCCTGGTTCGTGGACGACGTGGAGCTAAA
TSKSAGK*








CACAGCCACGACGAAGCCGAGAGAGGAGCAGTTCAACA
(SEQ ID NO: 70)








GCACCTACCGCGTGGTCAGCGCCCTGCGCATCCAGCAC









CAGGACTGGACTGGAGGAAAGGAGTTCAAGTGCAAGGT









CCACAACGAAGGCCTCCCAGCCCCCATCGTGAGGACCA









TCTCCACGACCAAAGGGCCGGCCCGGGACGCGGAGGT









GTATGTGCTGGCCCCAGCCCAGGAAGAGGTCAGCAAAA









GCACGGTCAGCCTCACGTGCATGGTCACCAGCTTCTAC









CCAGACTACATCGCCGTGGAGTGGCAGAGAAATGCGCA









GCCTGAGTCAGAGGACAAGTACGGCACGACCCCTCCCC









AGCTGGACGCCGACCGCTCCTACTTCCTGTACACCAGG









CTCAGGGTGGACAGGAACAGCTGGCAGGAAGGAGACA









CCTACACGTGTGTGGTGATGGACGAGGCCCTGCACAAT









CACTACACGCAGAAGTCCACCTCTAAGTCTGCGGGTAA









ATGA









(SEQ ID NO: 71)








IgG2
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGGCATC
ASTTAPKVYPLASSCGDTSSSTVTLGC
S82407






variant
CAGCTGCGCAGACACATCCAGCTCCACCGTGACCCTGG
LVSSYMPEPVTVTWNSGALKSGVHTFP







1
GCTGCCTGGTGTCCAGCTACATGCCCGAGCCGGTGACC
AVLQSSGLYSLSSMVTVPASSSGQTFT








GTGACCTGGAACTCGGGTGCCCTGAAGAGCGGCGTGCA
CNVAHPASSTKVDKAVGVSIDCSKCHN








CACCTTCCCGGCTGTCCTTCAGTCCTCCGGGCTCTACT
QPCVREPSVFIFPPKPKDTLMITGTPEV








CTCTCAGCAGCATGGTGACCGTGCCCGCCAGCAGCTCA
TCVVVNVGHDNPEVQFSWFVDDVEVH








GGACAGACCTTCACCTGCAACGTAGCCCACCCGGCCAG
TARSKPREEQFNSTYRVVSALPIQHQD








CAGCACCAAGGTGGACAAGGCTGTTGGGGTCTCCATTG
WTGGKEFKCKVNNKGLSAPIVRIISRSK








ACTGCTCCAAGTGTCATAACCAGCCTTGCGTGAGGGAA
GPAREPQVYVLDPPKEELSKSTLSVTC








CCATCTGTCTTCATCTTCCCACCGAAACCCAAAGACAC
MVTGFYPEDVAVEWQRNRQTESEDKY








CCTGATGATCACAGGAACCCCCCACCTCACGTGTGTCG
RTTPPQLDTDRSYFLYSKLRVDRNSWQ








TGGTGAACGTGGGCCACGATAACCCCGAGGTGCAGTTC
EGDAYTCVVMHEALHNHYMQKSTSKS








TCCTGGTTCGTGGATGACGTGGAGGTGCACACGGCCAG
AGK*








GTCGAAGCCAAGAGAGGAGCAGTTCAACAGCACGTACC
(SEQ ID NO: 72)








GCGTGGTCACCGCCCTGCGCATCCAGCACCAGGACTGG









ACTGGAGGAAAGGAGTTCAAGTGCAAGGTCAACAACAA









AGGCCTCTCGGCCCCCATCGTGAGGATCATCTCCAGGA









GCAAAGGGCCGGCCCGGGAGCCGCAGGTGTATGTCCT









GGACCCACCCAAGGAAGAGCTCAGCAAAAGCACGCTCA









GCGTCACCTGCATGGTCACCCGCTTCTACCCAGAAGAT









GTAGCCGTGGAGTGGCAGAGAAACCGGCAGACTGAGTC









GGAGGACAAGTACCGCACGACCCCGCCCCAGCTGGAC









ACCGACCGCTCCTACTTCCTGTACAGCAAGCTCAGGGT









GGACAGGAACAGCTGCCACGAAGGAGACGCCTACACG









TGTGTGGTGATGCACGAGGCCCTGCACAATCACTACAT









GCAGAAGTCCACCTCTAAGTCTGCGGGTAAATGA









(SEQ ID NO: 73)








IgG2
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGACTTC
ASTTAPKVYPLSSCCGDKSSSTVTLGC
M36946






variant
TTGCTGCGGGGACAAGTCCAGCTCCACCGTGACCCTGG
LVSSYMPEPVTVTWNSGALKSGVHTFP
(X08703)






2
GCTGCCTGGTGTCCAGCTACATGCCCGAGCCGGTGACC
AVLQSSGLYSLSSMVTVPGSTSGQTFT








GTGACCTGGAACTCGGGTGCCCTGAAGAGCGGCGTGCA
CNVAHPASSTKVDKAVGVSSDCSKPN








CACCTTCCCGGCCGTCCTTCAGTCCTCCGGGCTCTACT
NQHCVREPSVFIFPPKPKDTLMITGTPE








CTCTCAGCAGCATGGTGACCGTGCCCGGCAGCACCTCA
VTCVVVNVGHDNPEVQFSWFVDDVEV








GGACAGACCTTCACCTGCAACGTAGCCCACCCGGCCAG
HTARTKPREEQFNSTYRVVSALPIQHQ








CAGCACCAAGGTGGACAAGGCTGTTGGGGTCTCCAGTG
DWTGGKEFKCKVNIKGLSASIVRIISRS








ACTGGTCCAAGCCTAATAACCAGCATTGCGTGACGGAA
KGPAREPQVYVLDPPKEELSKSTVSVTC








CCATCTGTCTTCATCTTCCCACCGAAACCCAAAGACAC
MVIGFYPEDVDVEWQRDRQTESEDKYR








CCTGATGATCACAGGAACCCCCGAGGTCACGTGTGTGG
TTPPQLDADRSYFLYSKLRVDRNSWQR








TGGTGAACGTGGGCCACGATAACCCCGAGGTGCAGTTC
GDTYTCVVMHEALHNHYMQKSTSKSA








TCCTGGTTCGTGGACGACGTGGAGGTGCACACGGCCAG
GK*








GACGAAGCCGAGAGAGGACCAGTTCAACAGCACGTACC
(SEQ ID NO: 74)








GCGTGGTCAGCGCCCTGCCCATCCAGCACCAGGACTGG









ACTGGAGGAAAGGAGTTCAAGTGCAAGGTCAACATCAA









AGGCCTCTCGGCCTCCATCGTGAGGATCATCTCCAGGA









GCAAAGGGCCGGCCCGGGAGCCGCAGGTGTATGTCCT









GCACCCACCCAAGGAACAGCTCAGCAAAAGCACGGTCA









GCGTCACCTGCATGGTCATCGGCTTCTACCCAGAAGAT









GTAGACGTGGAGTGGCAGAGAGACCGGCAGACTGAGTC









GGAGGACAAGTACCGCACGACCCCGCCCCAGCTGGAC









GCCGACCGCTGGTACTTCCTGTACAGCAAGCTCAGGGT









GGACAGGAACAGCTGGCAGAGAGGAGACACCTACACGT









GTGTGGTGATGCACGAGGCCCTGCACAATCACTACATG









CAGAAGTCCACCTCTAAGTCTGCGGGTAAATGA









(SEQ ID NO: 75)








IgG2
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGAGTTC
ASTTAPKVYPLSSCCGDKSSSGVTLGC
X16702






variant
TTGCTGCGGGGACAAGTCCAGCTCGGGGGTGACCCTGG
LVSSYMPFPVTVTWNSGALKSGVHTFP
(M25278)






3
GCTGCCTGGTCTCCAGCTACATGCCCGAGCCGGTGACC
AVLQSSGLYSLSSMVTVPASSSGTQTF








GTGACCTGGAAGTCGGGTGCCCTGAAGAGCGGCGTGCA
TCNVAHPASSTKVDKAVGVSSDCSKP








CACCTTCCCGGCCGTCCTTCAGTCCTCCGGGCTCTACT
NNQHCVREPSVFIFPPKPKDTLMITGTP








CTCTCAGCACCATCGTCACCGTGCCCGCCAGCAGCTCA
EVTCVVVNVGHDNPEVQFSWFVDDVE








GGAACCCAGACCTTCACCTGCAACGTAGCCCACCCGGC
VHTARTKPREEQFNSTYRVVSALPIQH








CAGCAGCACCAAGGTGGACAAGGCTGTTGGGGTCTCCA
QDWTGGKEFKCKVNIKGLSASIVRIISR








GTGACTGCTCCAAGCCTAATAACCAGCATTGCGTGAGG
SKGPAREPQVYVLDPPKEELSKSTVSLT








GAACCATCTGTCTTCATCTTCCCACCGAAACCCAAAGA
CMVIGFYPEDVDVEWQRDRQTESEDKY








CACCCTGATGATCACAGGAACGCCGGAGGTCACGTGTG
RTTPPQLDADRSYFLYSKLRVDRNSWQ








TGCTGCTGAACGTGGGCCACGATAACCCCGAGGTGCAG
RGDTYTCVVMHEALHNHYMQKSTSKS








TTCTCCTGGTTCGTGGACGACGTGGAGGTGCACACGGC
AGK*








CAGGACGAAGCCGAGAGAGGAGCAGTTCAACAGCACGT
(SEQ ID NO: 76)








ACCGCGTGGTCAGCGCCCTGCCCATCCAGCACCAGGAC









TGGACTGGAGGAAAGGAGTTCAAGTGCAAGGTCAACAT









CAAAGGCCTCTCGGCCTCCATCGTGAGGATCATCTCCA









GGAGCAAAGGGCCGGCCCGGGAGCCGCAGGTGTATGT









CCTGGACCCACCCAAGGAAGAGCTCAGCAAAAGCACGG









TCAGCCTCACCTGGATGGTCATCGGCTTCTACCCAGAA









GATGTAGACGTGGAGTGGCAGAGAGACCGGCAGACTGA









GTCGGAGGACAAGTACCGCACGACCCCCCCCCAGCTG









GACGCCGAGGGCTCCTACTTCCTGTACAGCAAGCTGAG









GGTGGACAGGAACAGCTGCCAGAGAGGAGACACCTAC









ACGTGTGTGGTGATGCAGGAGGCCCTGCACAATCACTA









CATGCAGAAGTCCACCTCTAAGTCTGCGGGTAAATGA









(SEQ ID NO: 77)

U63638






IgG3
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGGCATC
AKTTAPKVYPLASSCGDTSSSTVTLGC







variant
CAGCTGCGGAGACACATGCAGCTCCACCGTGACCCTGG
LVSSYMPEPVTVTWNSGALKSGVHTFP







1
GCTGCCTGGTCTCCAGCTACATGCCCGAGCCGGTGACC
AVRQSSGLYSLSSMVTVPASSSETQTF








GTGACCTGGAACTCGGGTGCCCTGAAGAGCGGCGTGCA
TCNVAHPASSTKVKDAVTARRPVPTTP








CACCTTCCCGGCCGTCCGGCAGTGCTCTGGGCTGTACT
KTTIPPGKPTTPKSEVEKTPCQCSKCP








CTCTCAGCAGCATGGTCACTGTGCGGGCCAGCAGCTCA
EPLGGLSVFIFPPKPKDTLTISGTPEVT








GAAACCCAGACCTTCACCTGCAACGTAGCCCACCCGGC
CVVVDVGQDDPEVQFSWFVDDEVHT








CAGCAGCACCAAGGTGGACAAGGCTGTCACTGCAAGGC
ARTKPREEQFNSTYRVVSALRIQHQDW








GTCCAGTCCCGACGACGCCAAAGAGAACTATCCCTCCT
LQGKEKCKVNNKGLPAPIVRTISRTKG








GGAAAACCGACAACCCCAAAGTGTGAAGTTGAAAAGAC
QAREPQVYVLAPPREELSKSTLSLTCLI








ACCCTGCCAGTGTTCCAAATGCCCAGAACCTCTGGGAG
TGFYPEEIDVEWQRNGQPESEDKYHTT








GACTGTCTGTCTTCATCTTCCCACCGAAACCCAAGCAC
APQLDADGSYFLYSKLRVNKSSWQEG








ACCCTCACAATCTCGGGAACGCCCGAGGTCACGTGTGT
DHYTCAVMHEALRNHYKEKSISRSPGK








GGTGGTGGACGTGGGCCAGGATGACCCCGAGGTGCAG
*








TTCTCCTGGTTGGTGGACGACGTGGAGGTGCACACGGC
(SEQ ID NO: 78)








CAGGACGAAGCCGACAGAGGACCAGTTCAACAGCACCT









ACCGCGTGGTCAGCGCCCTGCGCATCCAGCACCAGGA









CTGGCTGCAGGGAAAGGAGTTCAAGTGCAAGGTCAACA









ACAAAGGCCTCCCGGCCCCCATTGTGAGGACCATCTCC









AGGACCAAAGGGCAGGCCCGGGAGCCGCAGGTGTATG









TCCTGGCCCCACCCCGGGAAGAGCTCAGGAAAAGCACG









CTCAGCCTCACCTGCCTGATCACCGGTTTCTACCCAGA









AGAGATAGACGTGGAGTGGCAGAGAAATGGGCAGCCTG









AGTCGGAGGACAAGTACCACACGACCGCACCCCAGCTG









GATGCTGACGGCTCCTACTTCCTGTACAGCAAGCTCAC









GGTGAACAAGAGCAGCTGGCAGGAAGGAGACCACTACA









CGTGTGCAGTGATGCACGAAGCTTTACGGAATCACTAC









AAAGAGAAGTCCATCTCGAGGTCTCCGGGTAAATGA









(SEQ ID NO: 79)








IgG3
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGGCATC
ASTTAPKVYPLASRCGDTSSSTVTLGC
U63639






variant
CCGCTGCGGAGACACATCCAGCTCCACCGTGACCCTGG
LVSSYMPEPVTVTVWNSGALKSGVHTFP







2
GCTGCCTGGTCTCCAGCTACATCCCCGACCCCGTGACC
AVLQSSGLYSLSSMVTVPASTSETQTF








GTGACCTGGAACTCGGGTGCCCTGAAGACTCCCGTGCA
TCNVAHPASSTKVDKAVTARRPVPTTP








CAGCTTCCCGGCCGTCGTTGAGTCCTCCGGGCTGTACT
KTTIPPGKPTTQESEVEKTPCQCSKGP








CTCTCAGCAGGATGGTGACCGTGCCCGCCAGCACCTCA
EPLGGLSVFIFPPKPKDTLTISGTPEVT








GAAACCCAGACCTTCACCTGCAAGGTAGCCCACCCGGC
CVVVDVGQDDPEVQFSWFVDDVEVHT








CAGCAGCACCAAGGTGGACAAGGCTGTCACTGCAAGGC
ARTKPREEQFNSTYRVVSALRIQHQDW








GTCCAGTCCCGACGACGCCAAAGAGAACCATCCCGCCT
LQKKEFKCKVNNKGLPAPIVRTISRTKG








GGAAAACCCACAACCCAGGAGTCTGAAGTTGAAAAGAC
QAREPQVYVLAPPREELSKSTLSLTCLI








ACCCTGCCAGTGTTGCAAATGCCCAGAACCTCTGGGAG
TGFYPEEIDVEWQRNGQPESEDKYHTT








GACTGTCTGTCTTCATCTTCCCACCGAAACCCAAGGAC
APQLDADGSYFLYSRLRVNKSSWQEG








ACCCTCACAATCTCGGGAACGCCCGAGGTCACGTGTGT
DHYTCAVMHEALRNHYKEKSISRSPGK








GGTGGTGGACGTGGGCCAGGATGACCCCGAGGTGCAG
*








TGCTCCTGGTTCGTGGACGACGTGGAGGTGCACACGGC
(SEQ ID NO 80)








CAGGACGAAGCCGAGAGAGGAGCAGTTCAAGAGCAGCT









ACCCCGTGGTCAGGGCCCTGCGCATCCAGCACCAGGA









CTCGCTGCAGGGAAAGGAGTTCAAGTGCAAGGTCAACA









ACAAAGGCCTCCCGGCCCCCATTGTGAGGAGCATCTCC









AGGACCAAAGGGCAGGCCCGGGAGCCGCAGGTGTATG









TCCTGGCCCCACCCCGGGAAGAGCTCAGCAAAAGCACG









CTCAGCCTCACCTGCCTGATCACCGGTTTCTACCCAGA









AGAGATAGACGTGGAGTGGCAGAGAAATGGGCAGCCTC









AGTCGGAGGACAAGTACCACACGACCGCACCCCAGCTG









GATGCTGACGGCTGCTACTTCCTGTACAGCAGGCTCAG









GGTGAACAAGAGCAGCTGGCAGGAAGGAGACCACTACA









CGTGTGCAGTGATGCATGAAGCTTTACGGAATCACTAC









AAAGAGAAGTCCATCTCGAGGTCTCCGGGTAAATGA









(SEQ ID NO: 81)







Bovine
Ig
CAGCCCAAGTCCCCACCCTCGGTCACCCTGTTCCCGCC
QPKSPPSVTLFPPSTEELNGNKATLVC
X62917
Not
Chen L. et



Ig
lambda
CTCCAGGGAGGAGCTCAACGGCAACAAGGCCACCCTG
LISDFYPGSVTVVWKADGSTITRNVETT

registerd
al., Vet.



light

GTGTGTCTCATCAGCGACTTCTACCCGGGTAGCGTCTAC
RASKQSNSKYAASSYLSLTSSDWKSKG


Immunol.



chain

CGTGGTCTCGAAGGCAGACGGCACCACCATCACCCGCA
SYSCEVTHEGSTVTKTVKPSECS*


Immuno-



con-

ACGTGGAGACCACCCGGGCCTCCAAACAGAGCAACAG
(SEQ ID NO: 64)


pathol,



stant

CAAGTAGGCGGCCAGCAGCTACCTGAGGCTGACGAGCA



124, 284-



region

GCGACTGGAAATCGAAAGGCAGTTACAGCTGCGAGGTC



294 (2008)



(CL)

ACGCACGAGGGGAGCACCGTGACGAAGACAGTGAAGC



PMID:





CCTCAGAGTGTTCTTAG



18538861





(SEQ ID NO: 65)









Canine
Canine
IgG-D
GCCTGCACCACGGCCGCCTCGGTTTTCCCACTGGCC
ASTTAPSVFPLAPSCGSTSGSTVALAC
AF354267
http://www.
Tang L.


(Specific
Ig

CCCAGCTGCGGGTCCACTTCCGGCTCCACGGTGGCC
LVSGYFPEPVTVSWNSGSLTSGVHTFP

imgt.org/
et al.,


Name:
heavy

CTGGCCTGCCTGGTGTCAGGCTACTTCCCCGAGCCT
SVLQSSGLYSLSSTVTVPSSRWPSETF

IMGT
Vet Immuno-



Canis

chain

GTAACTGTGTCCTGGAATTCCGGCTCCTTGACCAGC
TCNVVHPASNTKVDKPVPKESTCKCIS

reportoire/
pathol 80



Lupus

con-

GGTGTGCACACCTTCCCGTCCGTCGTGCAGTCCTCA
PCPVPESLGGPSVFIFPPKPKDILRITR

index.
(3-4),



famililaris)
stant

GGGCTCTACTCCCTCAGCAGGACGGTGACAGTGCCC
TPEITCVVLDLGREDPEVQISWFVDGKE

ghp?section
259-270



region

TCCAGCAGGTGGCCCAGCGAGACCTTCACCTGCAAC
VHTAKTQPREQQFNSTYRVVSVLPIEHQ

=locus
(2001)



(CH1

GTGGTCCACCCGGCCAGCAACACTAAAGTAGACAAG
DWLTGKEFKCRVNHIGLPSPIERTISKA

Genes&
PMID:



CH3)

CCAGTGCCCAAAGAGTCCACCTGCAAGTGTATATCC
RGQAHQPSVYVLPPSPKELSSSDTVTL

reportoire=
11457479





CCATGCCCAGTCCCTGAATCACTGGGAGGGGCTTCG
TCLIKDFFPPEIDVEWQSNGQPEPESKY

genetable&






GTCTTCATCTTTCCCCCGAAACCCAAGGACATCCTC
HTTAPQLDEDGSYFLYSKLSVDKSRWQI

species=






AGGATTACCCGAACACCCGAGATCACCTGTGTGGTG
QGDTFTCAVMHEALGNHYTDLSLSHS


dog







TTAGATGTGGGCGGTGAGGAGCCTGAGGTGCAGATC
PGK*

&group=IGHC






AGCTGGTTCGTGGATGGTAAGGAGGTGCACACAGCC
(SEQ ID NO 84)








AAGACGCAGCCTCGTGAGCAGCAGTTCAACAGCACC









TACCGTGTGGTCAGCGTCCTCCCCATTGAGCACCAG









GACTGGCTCACCGGAAAGGAGTTCAAGTGCAGAGTC









AACCACATAGGCCTCCCGTCCCCCATCGAGAGGACT









ATCTCCAAAGCCAGAGGGCAAGCCCATCAGCCCAGT









GTGTATGTCCTGCCACCATCCCCAAAGGAGTTGTCA









TCCAGTGACACGGTCACCCTGACCTGCCTGATCAAA









GACTTCTTCCCACCTGACATTGATGTGGAGTGGCAG









AGCAATGGACAGCCGGAGCCCGAGAGCAAGTACCAC









ACGACTGCGCCCCAGCTGGACGAGGACGGGTCCTAC









TTCCTGTACAGCAATTCTCTCTGTGGACAAGAGCCGC









TGGCAGCAGGGAGACACCTTCACATGTGCGGTGATG









CATGAAGCTCTACAGAACCACTACACAGATCTATCCC









TCTCCCATTCTCCGGGTAAATGA









(SEQ ID NO: 85)







Canine
Ig
CAGCCCAAGGCGTCCCCCTCGGTCACACTCTTCCCG
QPKASPSVTLFPPSSEELGANKATLVC
E02824
not
None



Ig
lambda
CCCTCCTCTGACGAGCTCGGCCCCAACAAGGCCACC
LISDFYPSGVTVAWKASGSPVTQGVET

registered




light
(CL)
CTGGTGTGCCTCATCAGCGACTTCTACCCCAGCGGC
TKPSKQSNNKYAASSYLSLTPDKWKSHI






chain

GTGACGGTGGCCGGAAGGCAAGCGGCAGCCCCGT
SSFSCLVTHEGSTVEKKVAPAECS*






con-

CACCCAGGGCGTGGAGACGACCAAGCCCTCCAAGCA
(SEQ ID NO: 82)






stant

GAGCAACAACAAGTACGCGGCCAGCAGCTACCTGAG







region

CCTGACGCCTGACAAGTGGAAATCTCACAGCAGCTT









CAGCTGCCTGGTCACGCACGAGGGGAGCACCGTGG









AGAAGAAGGTGGCCCCCGCAGAGTGCTCTTAG









(SEQ ID NO: 83)









Ovian
Ovine
IgG1
GCCTCAACAACACCCCCGAAAGTGTACCCTCTGACT
ASTTPPKVYPLTSCCGDTSSSIVTLGC
X69797
http://www.
Dufour V.


(Scientific
Ig

TCTTGCTGCGGGGACACGTCCAGCTCCATCGTGACC
LVSSYMPEPVTVTWNSGALTSGVHTF

imgt.org/
et al. J.


Name:
chain

CTGGGCTGCCTGGTCTGCAGCTATATGCCCGAGCCG
PAILQSSGLYSLSSVVTVPASTSGAQT

IMGT
Immunol,



Ovis

light

GTGACCGTGACCTGGAACTCTGGTGCCCTGACCAGG
FICNVAHPASSTKVDKRVEPGCPDPCK

reportoire/
156, 2163-



aries)
con-

GGCGTGCACACCTTCCCGGCCATCCTGCAGTCCTCC
HCRCPPPELPGGPSVFIFPPKPKDTLTI

index.
2170 (1996)



stant

GGGCTCTACTCTCTCAGCAGCGTGGTGACCGTGCCG
SGTPEVTCVVVDVGQDDPEVQFSWFV

ghp?section
PMID:



region

GCCAGCACCTCAGGAGCCCAGACCTTCATCTGCAAC
DNVEVRTARTKPREEQFNSTFRVVSAL

=locus
8690905



CH1

GTAGCCCACCCGGCCAGCAGCACCAAGGTGGACAAG
PIQHQDWTGGKEFKCKVHNEALPAPIV

Genes&




CH3)

CGTGTTGAGCCCGGATGCCCGGACCCATGCAAACAT
RTISRTKGQAREPQVYVLAPPQEELSK

reportoire=






TGCCGATGCCCACCCCCTGAGCTCCCCGGAGGACC
STLSVTCLVTGFYPDYIAVEWQKNGQP

genetable&






GTCTGTCTTCATCTTCCCACCGAAACCCAAGGACAC
ESEDKYGTTTSQLDADGSYFLYSRLRV

species=






CCTTACAATCTCTGGAACGCCCGAGGTCACGTGTGT
DKNSWQEGDTYACVVMHEALHNHYTQ


sheep







GGTGGTGGACGTGGGCCAGGATGACCCCGAGGTGC
KSISKPPGK*

&group=IGHC






ACTTCTCCTGGTTCGTGGACAACGTGGACGTGCCCA
(SEQ ID NO: 90)








CGGCCAGGACAAAGCCGAGAGAGGAGCAGTTCAACA









GCACCTTCCGCGTGGTCAGCGCCGTGCCCATCCAGC









ACCAAGACTGGACTGGAGGAAAGGAGTTCAAGTGCA









AGGTCCACAACGAAGCCCTCCCGGCCCCCATCGTGA









GGACCATCTCCAGGACCAAAGGGCAGGCCCGGGAG









CCGGAGGTGTACGTCCTGGCCCCACCCCAGGAAGAG









CTCAGCAAAAGCACGCTCAGCGTCACCTGCCTGGTC









ACCGGCTTCTACCCAGACTACATCGCCGTGGAGTGG









CAGAAAAATGGGCAGCCTGAGTCGGAGGACAAGTAC









GGCACGACCACATCCCAGCTGGACGCCGACGGCTCC









TACTTGCTGTACAGCAGGCTCAGGGTGGAGAAGAAC









AGCTGGCAAGAAGGAGACACCTACGCGTGTGTGGTG









ATGCACGAGGCTCTGCACAACCACTACACACAGAAG









TCGATCTCTAAGCCTCCGGGTAAATGA









(SEQ ID NO: 91)








IgG2
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTCACT
ASTTAPKVYPLTSCCGDTSSSSSIVTL
X70983

Clarkson





TCTTGCTGCGGGGACACGTCCAGCTCCAGCTCCATC
GCLVSSYMPEPVTVTWNSGALTSGVH


C.A. et





GTGACCCTGGGCTGCCTGGTCTCCAGCTATATGCCC
TFPAILQSSGLYSLSSVVTVPASTSGA


al, Mol.





GAGCCGGTGACCGTGACCTGGAACTCTGGTGCCCTG
QTFICNVAHPASSAKVDKRVGISSDYS


Immunol,





ACCAGCGGCGTGCACACCTTCCCGGCCATCCTGCAG
KCSKPPCVSRPSVFIFPPKPKDSLMITG


20 1195-





TCCTCCGGGCTCTACTCTCTCAGCAGCGTGGTGACC
TPEVTCVVVDVGQGDPEVGFSWFVDN


1204 (1993)





GTGCCGGCCAGCAGCTCAGGAGCCCAGACCTTCATC
VEVRTARTKPREEQFNSTFRVVSALPI


PMID:





TGCAACGTACCCCACCCCCCCAGCACCGCGAACGTG
QHDHWTGGKEFKCKVHSKGLPAIVRT


8413324





GACAAGCGTGTTGGGATCTCCAGTGACTACTCCAAG
ISRAKGQAREPQVYVLAPPQEELSKST








TGTTCTAAACCGCCTTGCGTGAGCCGACCGTCTGTC
LSVTCLVTGFYPDYIAVEWQRARQPES








TTCATCTTCCCCCCGAAACCCAAGGACAGCCTCATG
EDKYGTTTSQLDADGSYFLYSRLRVGK








ATCACAGGAACGCCCGAGGTCACGTGTGTCGTGGTG
SSWQRGDTYACVVMHEALHNHYTGKS








GACGTGGGCCAGGGTGACCCCGAGGTGCAGTTCTCC
ISKPPGK*








TGGTTCGTGGACAACGTGGAGGTGCGCACGGCCAGG
(SEQ ID NO: 92)








ACAAAGCCGAGAGAGGAGCAGTTCAACAGCACCTTC









CGCGTGGTCAGCGCCCTGCCCATCCAGCACGACCAC









TGGACTCGAGGAAAGGAGTTCAAGTGCAAGGTCCAC









AGCAAAGCCCTCCCGGCCCCCATCGTGAGGACCATC









TCCAGGGCCAAAGGGCAGGCCCGGGAGCCGCAGGT









GTAGGTCCTGGCCCCACCCCAGGAAGAGCTCAGCAA









AAGCACGCTCAGCGTCACCTGCCTGGTCACCGGCTT









CTACCCAGACTACATCGCCGTGGAGTGGCAGAGAGC









GCGGCAGCCTCAGTCCGAGGAGAAGTACGCCACGAC









CACATCCCAGCTGGACGCCGACGGCTCCTACTTCCT









GTACAGCAGGCTCAGGGTGGACAAGAGCAGCTGGCA









AAGAGGAGACACCTAGGCGTGTGTGGTGATGCACGA









GGCTCTGCACAACCACTACACACAGAAGTCGATCTC









TAAGCCTCCGGGTAAATGA









(SEQ ID NO: 93)







Ovine
Ig
CCATCCGTCTTCCTCTTCAAACCATCTGAGGAACAG
PSVFLFKPSEEQLRTGTVSVVCLVNDF
X54110
Not
Jenne C.N.



Ig
kappa
CTGAGGACCGGAACTGTCTCTGTCGTCTGCTTCGTG
YPKDINVKVKVDGVTQNSNFQNSFTDQ

registered
et al. Dev



light
(CL)
AATGATTTCTACCCCAAAGATATCAATGTCAAGGTGA
DSKKSTYSLSSTLTLSSSEYQSHNAYA


Comp.



chain

AAGTGGATGGGGTTACCCAGAACAGCAACTTCCAGA
CEVSHKSLPTALVKSFNKNEC*


Immunol.



con-

ACAGCTTCACAGACCAGGACAGRAAGAAAAGCACCT
(SEQ ID NO: 86)


30 (1-2),



stant

ACAGCCTCAGCAGCACCCTGAGACTGTCCAGCTCAG



165-174



region

AGTACCAGAGCCATAACGCCTATGCGTGTGAGGTCA



(2006)





GCCACAAGAGCCTGCCCACCGCCCTCGTCAAGAGCT



PMID:





TCAATAAGAATGAATGTTAG



16083958





(SEQ ID NO: 87)








Ig
GGTCAGCCCAACTCCGCACCCTCGGTCACCCTGTTC
GQPKSAPSVTLFPPSTEELSTNKATVV
AY734681






lambda
CCGCCTTCCACGGAGGAGCTCAGTAGCAAGAAGGCC
CLINDFYPGSVNVVWKADGSTINQNVK







(CL)
ACCGTGGTGTGTCTCATCAACGACTTCTACCCGGGT
TTQASKQSNSKYAASSYLTLTGSEWKS








AGCGTGAACGTGGTCTGGAAGGCAGATGGCAGCACC
KSSYTCEVTHEGSTVTKTVKPSECS*








ATCAATCAGAACGTGAAGACCACCCAGGCCTCCAAA
(SEQ ID NO: 88)








CAGAGCAACAGCAAGTACGCGGCCAGCAGCTACCTG









ACCCTGACGGGCAGCGAGTGGAAGTCTAAGAGCAGT









TAGACCTGCGAGGTCACGCACGAGGGGAGCACCGTG









ACGAAGACAGTGAAGCCCTCAGAGTGTTCTTAG









(SEQ ID NO: 89)









Porcine
Por-
IgG3
GCCCCCAAGACGGCCCCATCGGTCTACCCTCTGGCCCCCTGCGGCAC
APKTAPSVYPLAPCGRDTSGPNVALG
U03781
http://www.
Butler J.E.


(Scientific
cine

CGACACGTCTC
CLASSYFPEPVTMTWNSGALTSGVHT

imgt.org/
et al.


Name: Sus
Ig

GCCCTAACGTGGCCTTGGGGTGCCTGGCCTCAAGCTACTTCCCCGAG
FPSVLQPSGLYSLSSMVTVPASSLSS

IMGT
Immuno-



serpa)
heavy

CCAGTGACCATG
KSYTCNVNHPATTTKVDKRVGTKTKP

reportoire/
genetics



chain

ACCTGGAACTGGGGCGCCCTGACCAGTGGCGTGCATACCTTCCCATC
PCPICPGCEVAGPSVFIFPPKPKDTLMI

index.
61(3)



con-

CGTCCTCCAGCC
SQTPEVTCVVVDVSKEHAEVQFSWYV

ghp?section
209-230



stant

CTCAGGGCTCTACTCCCTCAGCAGCATGGTCACCGTGCCCGCCAGCA
DGVEVHTAETRPKEEQFNSTYRVVSV

=locus
PMID:



region

GCCTGTCGAGCA
LPIQHQDWLKGKEFKCKVNNVDLPAP

Genes&
19028748



(CH1

AGAGCTACACCTGCAATGTCACCACCCGGCCACCACCACCAAGGTGG
TRTISKAIGQSREPQVYTLPPPAEELS

reportoire=
Kaeskoves



CH3)

ACAAGCGTGTT
RSKVTVTCLVIGIFYPPDIHVEWKSNGQ

genetable&
I et al.





GGAACAAAGACCAAACCACCATGTCCCATATGCCCAGGCTGTGAAGT
PEPEGNYRTTPPQDDVDGTFFLYSKL

species=
J. Immunol





GCCCGGGCCCTC
AVDKARWDHGETFECAVMHEALHNHY


sheep

153(8)





GGTCTTCATCTTCCCTCCAAAACCCAAGGACACCCTCATGATCTCCC
TQKSISKTGGK*

&group=IGHC
3585-3573





AGACCCCCGAGG
(SEQ ID NO: 94)


(1994)





TCACGTGCGTGGTGGTGGACGTCAGCAAGGAGCACGCCGAGCTCCAG



PMID:





TTCTCCTGGTAC



7930579





GTGGACGGCGTAGAGGTGCACACGCCCGACACGAGACCAAAGGAGGA









GCAGTTCAACAG









CACCTACCGTGTCCTCAGCGTCCTGCCCATCCAGCACCACGACTGGC









TGAAGGGGAAGG









AGTTCAAGTGCAAGGTCAACAACGTAGACCTCCCAGCCCCCATCACG









AGGACCATCTCC









AAGGCTATAGGGCAGAGCCGGGAGCGGCAGGTGTACACCCTGCCCCC









ACCCGCCGAGG









ACCTGTCCAGGAGCAAAGTCACCGTAACCTGCCTGGTCATTGGCTTC









TACCCACCTGAC









ATCCATGTTGAGTGGAAGAGCAACGGACAGCCGGAGCCAGAGGGCAA









TTACCGCACCAC









CCCGCCCCAGCAGGACGTGGACGGGACCTTCTTCCTGTACAGCAAGC









TCGCGGTGGACA









AGGCAAGATGGGACCATGGAGAAACATTTGAGTGTGCCGTGATGCAC









GAGGCTCTGGAC









AACCACTACAGCCAGAAGTCCATCTCCAAGACTCAGGGTAAATGA









(SEQ ID NO: 95)








IgG3
GCCCCCAAGACGGCCCCATCGGTCTACCCTCTGGCCCCCTGCCGCAG
APKTAPSVYPLAPCGRDVSGPNVALG
U003718







GGACGTCTCTG
CLASSYFPEPVTVTWNSGALTSGVHT








GCCCTAACGTGGCCTTGGGCTGCCTGGCCTCAAGCTACTTCCCCGAG
FPSVLQPSGLYSLSSMVTVPASSLSS








CCAGTGACCGTG
KSYTCNVNHPATTTKVDKRVGIHQPQ








ACCTGGAACTCGGGCGCCCTGACCACTGGCGTGCACACCTTCCCATC
TCPICPGCEVAGPSVFIFPPKPKDTLMI








CGTCCTGCAGCC
SQTPEVTCVVVDVSKEHAEVQFSWYV








GTCAGGGCTCTACTCCCTCACCAGCATGCTCACCGTGCCGGCCAGCA
DGVEVHTAETRPKEEQFNSTYRVVSV








GCCTGTCCAGCA
LPIQHQDWLKGKEFKCKVNNVKLPAPI








AGAGCTACACCTGCAATGTCAACCACCCGGCCAGCACCACCAAGGTG
TRTISKAIGQSREPQVYTLPPPAEELS








GACAAGCGTGTT
RSKVTLTCLVIGFYPPDIHVEWKSNGQ








GGAATACACCAGCCGCAAACATGTCCCATATGCCCAGGCTGTGAAGT
PEPENTYRTTPPQQDVDGTFLYSKL








GGCCGGGCCCTC
AVDKARWDHGDKFECAVMHEALHNH








GGTCTTCATCTTCCCTCCAAAACCCAACGACACCCTCATGATCTCCC
YTQKSISKTQGK*








AGACCCCCGAGG
(SEQ ID NO: 96)








TCACGTGCGTGGTGGTGGACGTCAGCAAGGAGCACGCCGAGGTCCAG









TTCTCCTGGTAC









GTGGACGGCGTAGAGGTGCACACGGCCGAGACGAGACCAAAGGAGGA









GCAGTTCAACAG









CACCTACCGTGTGGTCAGCGTCGTGCCCATCCAGCACGAGGACTGGC









TGAAGGGGAACG









AGTTCAAGTGCAAGGTCAACAACGTAGACCTCCCACCCCCCATCACC









AGGACCATCTCC









AAGGCTATAGGGCAGAGCCGGGAGCCGCAGGTGTACACCCTGCCCCC









ACCCGCCGAGG









AGCTGTCCAGGAGCAAAGTCACGCTAAGCGCCTCCCCATTGCCTTCT









ACCCACCTGAC









ATCCATGTTGAGTGGAAGAGCAACGGACAGCCGGAGCCAGAGAACAC









ATACCGCACCAC









CCCGCCCCAGCAGGACGTGGACGGGACCTTCTTCCTGTACAGCAAAC









TCGCGGTGGACA









AGGCAACATCGGAOCATGGAGACAAATTTGAGTGTCCGCGGAGGGAC









CACGCGCTGCAC









AACCACTACACCCAGAAGACCATCTCCAAGACTCAGGGTAAATGA









(SEQ ID NO: 97)








IgG2
GCCCCCCAAGACGCCCCCATCGGTCTACCCTCTGGCCCCCTGCAGCA
APKTAPSVYPLAPCSRDTSGPNVALG
U03779







GGGACACGTCTG
CLASSYFPEPVTVTWNSGALSSGVHT








GCCCTAACGTGGCGTTGGGCTGCCTGGCCTCAAGCTACTTCCCCGAG
FPSVLQPSGLYSLSSMVTVPASSLSS








CCAGTGACCGTG
KSYTCNVNHPATTTKVDKRVGTKTKP








ACCTGGAACTCGGGCGCCCTGTCCAGTGGCGTGCATACCTTCCCATC
PCPICPACESPGPSVFIFPPKPKDTLMI








CGTCCTGCAGCC
SRTPQVTCVVVDVSQENPEVQFSWYV








GTCAGGGCTCTACTCCCTCAGCAGCATGGTGACCGTGCCGGCCAGCA
GDVEVHTAQTRPKEEQFNSTYRVVSV








GCCTGTCCAGCA
LIIQHQDWLNGKEFKCKVNNKDLPAPI








AGAGCTACACCTGCAATGTCAACCACCCGGCCACCACCACCAAGGTG
TRISKAKGQTREPQVYTLPPHAEELS








GACAAGCGTGTT
RSKVSITCLVIGFYPPDIDVEWQRNGQ








TGGAACAAAGACCAAACCACCATGTCCCATATGCCCAGCCTGTGAAT
PEPGNYRTTPPQQDVDGTYFLYSKF








CACCAGGGCCCTC
SVDKASWQGGGIFQCAVMHEALHNHY








TGGTCTTCATCTTCCCTCCAAAACCCAAGGACACCCTCATGATCTCC
TQKSISKTPGK*








CCGACACCCCAGG
(SEQ ID NO: 98)








TCACGTGCGTGGTGGTTGATGTGAGCCAGGAGAACCGGCAGGTCCAG









TTCTGCTGGTAC









GTGGACGGCGTAGAGGTGCACACGGCCCAGACGAGGCCAAAGGAGGA









GCAGTTCAACAG









CACCTACCGCGTGGTCAGCGTCCTACCCATCCAGCACCAGGACTCGC









TGAACGGGAAGG









AGTTCAAGTCCAAGGTCAACAACAAAGACCTCCCAGCCCCCATCACA









AGGATCATCTCC









AAGGCCAAAGGGCAGACCCGGGAGCCGCAGGTGTACACCCTGCCCCC









ACACGCCGAGG









TACCTCTCCACGAGCAAAGTCACCATAACCTGCCTGGTCATTCGCTT









GTACCCACCTCAC









ATCGATGTCGAGTGCCAAAGAAACGGACAGCCGGAGCCAGAGGGCAA









TTACCGCACCAC









CCCGCCCCAGCAGGACGTGGACGGGACCTACTTCCTGTACAGCAAGT









TCTCGGTGGACA









AGCCCAGCTGGGAGGGTGGAGGCATATTCCAGTGTGCGGTGATCGAC









GAGGGTCTGCAC









AACCACTACACCCAGAAGTCTATCTCCAAGACTCCGGGTAAATGA









(SEQ ID NO: 99)








IgG2
GCCCCCAAGACCGCCCCATTGCTCTACCCTCTCCCCCGCTGCCCCAG
APKTAPLVYPLAPCGRDTSGPNVALG
U03780







GGAACGTCTG
CLASSYFPEPVTVTWNSGALTSGVHT








GCCCTAACGTGGCCTTGGGCTGCCTGGCCTCAAGCTACTTCCCCGAG
FPSVLQPSGLYSLSSMVTVPASSLSS








CCAGTGACCGTG
KSYTCNVNHPATTTKVDKRVGTKTKP








ACCTGGAACTCGGGCGCCCTGACCACTGGGGTCCATACCTTCCCATC
PCPICPACESPGPSVFIFPPKPKDTLMI








CGTCCTCCACCG
SRTPQVTCVVVDVSQENPEVQFSWYV








GTCAGGGCTCTACTCCCTCAGCAGCATGGTGACCGTGCCGGCCAGCA
DGVEVHTAQTRPKEEQFNSTYRVVSV








GCCTCTCCACCA
LIIQHQDWLNGKEFKCKVNNKDLPAPI








AGAGCTACACCTGCAATGTCAACCACCCGGCCAGCACCACCAAGGTG
TRISKAKGQTREPQVYTLPPHEELS








GACAAGCCTCTT
RSKVSITCLVIGFYPPDIDVEWQRNGQ








GGAACAAAGACCAAAGCACCATGTCCCATATGCCCAGCCTGTCAATCG
PEPEGNYRTTPPQQDVDGTYFLYSKF








CCAGGGCCCTC
SVDKASWQGGGIFQCAVMHEALHNHY








GGTCTTCATCTTCCCTCCAAAACCCAACGACACCCTCATGATCTCCC
TQKSISTPGK*








CCACACCCCAGG
(SEQ ID NO: 100)








TTCAGGTGCGTGGTAGTTGATGTGAGCCAGGAGAAGGCGGAGGTCCA









GTTCTCCTGGTAC









GTGGACGGCCTAGAGGTGCACACCGCCCAGACGAGGCCAAAGGAGGA









GCAGTTCAACAC









CAGCTACCGCCTGGTCAGCGTCCTGCCCATCCAGCACGAGGACTGGCT









GAACGGGAAGG









AGTTCAAGTGCAAGGTCAACAACAAAGACCTCCCAGCCCCCATCACAA









GGATCATCTCC









AAGGCCAAAGGGCAGACCCGGGAGCCGCACGTGTACACCCTGCCCCCA









CACCCCGAGG









AGCTCTCCAGGACCAAAGTCACCATAACCTGCCTGCTCATTGCCTTCT









ACCCACCTGAC









ATCGATGTCGAGTGGCAAAGAAACGGACAGCCGGAGCCAGAGGGCAAT









TACCGCACCAC









CCCCCCCCAGCAGCACCTGGACGTGACCTACAACCTGTACAGCAAGT









TCTCGGCGACA









TAGGCCACCTGGCACGGTGGACGCATATTGGAGTGTTCCGGTGATGC









ACGAGGCTCTGCAC









AACCACTACACCCAGAAGTCTATCTCCAAGACTCCGGGTAAATGA









(SEQ ID NO: 101)








IgG3
GCCTACAACACACCTCCATCCGTCTACCCTCTGGCCCCCTGTGGCAGC
AYNTAPSVYPLAPCGRDVSDHNVALG
EU372858







CGGCGTCTCTCA
CLVSSYFPEPVTVTWNSGALSRVVHT








TCATAACGTGGCCTTGGGCTGCCTTGTCTCAAGCTACTTCCCCGAGC
FPSVLQPSGLYSLSSMVIVAASSLSTL








CAGTGACCGTGA
SYTCNVYHPATNTKVDKRVDIEPPTPI








CCTGGAACTCGGGTGCCCTGTCCAGAGTCGTGCATACCTTCCCATCC
CPEICSCPAAEVLGAPSVFLFPPKPKD








GTCCTGCAGCCG
ILMISRTPKVTCVVVDVSQEEAEVQFS








TCAGGCCTCTACTCCCTGAGCAGCATCGTGATCGTCCCGCCCACCAGC
WYVDGVQLYTAQTRPMEEQFNSTYRV








CTGTCCACCCT
VSVLPIQHQDWLKGKEFKCKVNNKDLL








GAGCTACACGTGCAACGTCTACCACCCGGCCACCAACACCAAGGTGGA
SPITRTISKATGPSRVPQVYTLPPAWE








CAAGCGTCTTG
ELSKSKVSITCLVTGFYPPDIDVEQWS








ACATCGAACCGCCCACACCCATCTGTCCCGAAATTTGCTCATGCCCAG
NGQQEPEGNYRTTPPQQDVDGTYFLY








CTGCAGAGGTC
SKLAVDKVRWQRGDLFQCAVMHEALH








CTCGGAGCACCGTCGGTCTTCCTCTTCCCTCCAAAACCCAAGGACATC
NHYTQKSISKTQGK








CTCATGATCTC
(SEQ ID NO: 102)








CCGGACACCCAAGGTCACGTGCGTCGTCGTGGACGTGAGCCAGGAGGA









GGCTGAAGTCC









AGTTCTCCTGGTACGTGGACGGCGTACAGTTGTACACGGCCCAGACG









AGGCCAATGGAG









GAGCAGTTGAACAGCACCTACCGCGTGGTCAGCGTCCTGCCCATCCAG









CACCAGGACTG









GCTGAAGGGGAACGAGTTCAAGTCCAAGGTCAACAACAAAGACCTCCT









TTCCCCCATCA









CGAGGACCATCTCCAAGGCTACAGGGCCGAGCCGGGTGCCGCAGGTGT









ACACCCTGCC









CCCAGCCTCCGAACACCTGTCCAACAGCAAAGTCACCATAACCTGCCT









GGTCACTGGGT









TCTACCCACCTGACATCGATGTCGAGTGGCAGAGCAACCGACAACAAG









AGCCAGAGGGC









AATTACCGCACCACCCCGCCCCAGCAGGAGGTGGATGGGACGTACTTC









CTGTACAGCAA









GCTCGCGGTGGACAAGGTCAGGTGGCAGCGFGGAGACCTATTCCAGTG









TGCGGTGACGC









ACGAGGCTCTGCACAACCACTACACCCAGAAGTCCATCTCCAAGACT









CAGGGTAAATGA









(SEQ ID NO: 103)








IgG4
ACCTTCCCATCCGTCGTGCAGCCGTCAGGCCTCTACTCCCTCAGCAGC
TFPSVLQPSGLYSLSSMVTVPASSLS
U03782







ATGGTGACCGT
SKSYTCNVNHPATTTKVDKRVGTKTK








GCCGGCCAGCAGCCTGTCCAGCAAGAGCTACACCTGCAATGTCAACC
PPCPICPACEGPGPSAFIFPPKPKDTL








ACCCGGCCACCA
MISTRPKVTCVVVDVSQENPEVQFSW








CCACCAAGGTGGACAAGCGTGTTGGAACAAAGACCAAACCACCATGTC
YVDGVEVHTAQTRPKEEQFNSTYRVV








CCATATGCCCA
SVLPIQHQDWLNGKEFKCKVNNKDLP








GCCTGTGAAGGGCCCGGGCCCTCGGCCTTCATCTTCCCTCCAAAACCC
APITRISKAKGQTREPQVYTLPPPTEE








AAGGACACCCT
LSRSKVTLTCLVTGFYPPDIDVEWQRN








CATGATCTCCCGGACCCCCAAGGTCACGTGCGTGGTGGTAGATGTGAG
GQPEPEGNYRTTPPQQDVDGTYFLYS








CCAGGAGAACC
KLAVDKASWQRGDTFQCAVMHEALH








CGGAGGTCCAGTTCTCCTGGTACGTGGACGGCGTAGAGGTGCACACG
NHYTQKSIFKTPGK*








GCCCAGACGAGG
(SEQ ID NO: 104)








CCAAAGGACGAGCACTTCAACAGCACCTACCCCGTGGTCAGCGTCCTC









CCCATCCACCA









CCAGGACTGGCTGAACGGGAAGGAGTTCAAGTGCAAGGTCAACAACA









AAGACCTCCCAG









CCCCCATCACAAGGATCATCTCCAAGGCCAAAGGGCAGACCCGGGAGC









CGCAGGTGTAC









ACCCTGCCCCGACCCACCGAGGAGCTCTCCAGGTCCAAAGTCACGCTA









ACCTGCCTGGT









CACTGGCTTCTACCCACCTGACATCGATGTCGAGTGGCAAAGAAACGG









ACAGCCGGAGC









CAGAGGGCAATTACCGCACCACCCCGCCCCAGCAGGACGTGGACGGGA









CCTACTTCCTG









TACAGCAAGCTCGCCGTCCACAAGGCCACCTGCCAGCCTGGACACACA









TTCCAGTGTCC









GGTGATGCACGAGGCTCTGCACAACCACTACACCCAGAAGTCCATCTT









CAAGACTCCGG









GTAAATGA









(SEQ ID NO: 105)








IgG4
GCCCCCAAGACGGCCCCATCGGTCTACCCTCTGGCCCCCTGCGGCAGG
APKTAPSVYPLAPCGRDVSGPNVALG
EU372654







GACGTGTCTG
CLASSYFPEPVTVTWNSGALTSGVHT








GCCCTAACGTGGCCTTGGGGTGCCTGGCCTCAAGCTACTTCCCCGAGC
FPSVLQPSGLYSLSSMVTVPASSLSS








CAGTGACCGTG
KSYTCNVNHPATTTKVDKRVGIHQPQ








ACCTGGAACTCGGGCGCCCTGACCAGTGGCGTGCACACCTTCCCATCC
TCPICPACEGPGPSAFIFPPKPKDTLMI








GTCCTGCAGCC
SRTPKVTCVVVDVSQENPEVQFSWYV








GTCAGGGCTCTACTCCCTCAGCAGCATGGTGACCGTGCCGGCCAGCAG
GHVEVHTAQTRPKEEQFNSTYRVVSV








CCTGTCCAGCA
LLIQHQDWLNGKEFKCKVNNKDLPAPI








AGAGCTACACCTGCAATGTCTAACCAGCCGGCCACCACCACCAAGGTG
TRISKAKGQTREPQVYTLPPPTEELSF








GACAAGCGTGTT
SKVTLTCLVTGFYPPDIDVEWQRNGQ








GGAATACACCAGCCGCAAACATGTCCCATATGCCGAGCCTGTGAAGGG
PEPEGNYRTTPPQQDVDGTYFLYSKL








CCCCGGCCCTC
AVDKASWQRGDTFQCAVMHEALHNH








GGCCTTCATCTTCCCTCCAAAACCCAAGGACACCCTCATGATCTCCCG
YT








GACCCCCAAGG
(SEQ ID NO: 106)








TCACGTGCGTGGTGGTTGATGTGAGGCAGGAGAACCCGGAGGTCCAGT









TGTCCTGGTAC









GTGGACGGCGTAGAGGTGCACACGGCCCAGACGAGGCCAAAGGAGGAG









CAGTTCAACAG









CACCTACCGCGTGGTCAGCGTCCTGCTCATCCAGCACCAGGACTGGCT









GAAGGGGAAGG









AGTTCAAGTGCAAGCTCAAGAACAAAGACCTCCCAGCCCCCATCACAA









GGATCATCTCC









AAGGCCAAAGGGCAGACCCGGGAGCCGCAGGTGTACACCCTGCCCCCA









CCCACCGAGG









AGCTGTCCAGGAGCAAAGTCACGCTAACCTGCCTGGTCACTGGCTTCT









ACCCACCTGAC









ATCGATGTCGAGTGGCAAAGAAACGGACAGCCGGACCCAGAGGGCAAT









TACCCCACCAC









CCCGCCCCAGCAGGACGTGGACGGGACCTACTTCCTGTACAGCAAGCT









CGCGGTGGACA









AGGCCAGCTGGCAGCGTGGAGACACATTCCAGTGTGCGGTGATGCACG









AGGCTCTGCAC









AACCACTACACCC









(SEQ ID NO: 107)








IgG5
GCCCCCAAGACGGCCCCATCGGTCTACCCTCTGGCCCCCTGCAGCAG
APKTAPSVYPLAPCSRDTSGPNVALG
EU372657







GGACACGTCTG
CLVSSYFPEPVTVTWNSGALTSGHVT








GCCCTAACGTGGCCTCGGCTGCCTGGTCTCAAGCTACTTCCCCGAGC
FPSVLQPSGLYSLSSMVTVPAHSLSS








CAGTGACCGTG
KRYTCNVNHPATKTKVDLCVGRPCPI








ACCTGGAACTCGGGCGCCCTGACCAGTGGCGTGCACACCTTCCCATCC
CPGCEVAGPSVFIFPPKPKDILMISRTP








GTCCTGCAGCC
EVTCVVVDVSKEHAEVQFSWYVDGEE








CTCAGGGCTCTACTCCCTCAGCAGCATGGTGACCGGCCGGCCCACAGC
VHTAETRPKEEQFNSTYRVVSVLPIQH








TTGTCCAGCA
EDWLKGKEFECKVNNEDLPGPITRTIS








AGCGCTATACGTGCAATGTCAACCACCCAGCCACCAAAACCAAGCTGG
KAKGVVRSPEVYTLPPPAEELSKSIVT








ACCTGTGTGTT
LTCLVKSIFPIFIHVEWEINGKPEPENA








GGACGACCATGTCCCATATGCCCAGGCTGTGAAGTGCCCGGGCCCTCG
YRTTPPQEDEDRTYFLYSKLAVDKAR








CTCTTCATCTT
WDHGETFECAVMHEALNHNYTQKSIS








CCCTCCAAAACCCAAGGACATCCTCATGATCTCCCGGACCCCCGAGGT
KTQGK*








CACGTGCGTGG
(SEQ ID NO: 108)








TGGTGGACGTCAGCAAGGAGCACGCCGAGGTCCAGTTCTCCTGGTACG









TGGACGGCGAA









GAGCTGCACACCGCCGAGACCAGGCCAAAGGACGAGCAGTTCAACACC









ACCTACCGCGT









GGTCAGCGTCCTGCCCATCCAGCACGAGGACTGGCTGAAGGGGAAGG









AGTTCGAGTGCA









AGGTCAACAACGAAGACCTCCCAGGCCCCATCACGAGGACCATCTCCA









AGCCCAAACCC









GTGGTACGGAGCCGGGAGGTGTACACCCTGCCGCCACCCGCCGAGGA









GCTGTCCAAGA









GCATAGTCACGCTAACCTGCCTGGTCAAAAGCATCTTCCCGTCTTTCA









TCCATGTTGAGT









GGAAAATCAACGGAAAAGGAGAGCCAGAGAACGCATATCGCACCACC









GCGGCTCAGGAC









CACCAGGACAGGACCTACTCCCTGTACAGCAAGCTCGCCGTGCACAA









CGCAAGATGGGA









CCATGGAGAAACATTTGAGTGTGCGGTGATGCACGAGGCTCTGCACA









ACCACTACACCC









AGAAGTCCATCTCGAAGACTCAGGGTAAATGA









(SEQ ID NO: 109)








IgG5
GCCTACAACACAGCTCGATCGGTCTACCCTCTGGCCCCCTGTGGCAGG
AYNTAPSVYPLAPCGRDVSDHNVALG
EU372686







GACGTGTCTGA
CLVSSYFPEPVTVTWNWGAQTSGVHT








TCATAACGTGGCCTTGGGCTGCCTGGTCTCAAGCTACTTCCCCGAGCC
FPSVLQPSGLYSLSSTVTVPAHSLSSK








AGTGACCGTGA
CFTCNVNHPATTTKVDLCVGKKTKPR








CCTGGAACTGGGGCGCCCAGACCAGTGGCGTGCACACCTTCCCATCCG
CPICPGCEVAGPSVFIFPPKPKDILMIS








TCCTGCAGCCG
RTPEVTCVVVDVSKEHAEVQFSWYVD








TCAGGGCTCTACTGCCTCAGCAGCAGGGTGAGCGTGGCGGCCCACAG
GDDVHTAETRPKEEQFNSTYRVVSVL








CTTGTCCAGCAA
PIQHEDWLKGKEFECKVNNEDLPGPIT








CTGCTTCACGTGCAATGTCAACCACCCCGCCACCACCACCAAGGTCGA
RTISKAKGVVRSPEVYTLPPPAEELSK








CCTCTGTGTTG
SIVTLTCLVKSFFPPFIHVEWKINGKPE








GAAAAAAGACCAAGCCTCGATGTCCCATATGCCCAGGCTGTGAAGTG
PENAYRTTPPQEDEDGTYFLYSKFSVE








GCCGGGCCCTCG
KFRWHSGGIHCAVMHEALHNHYT








GTCTTCATCTTCCCTCCAAAACCCAAGGACATCCTCATGATCTCCCG
(SEQ ID NO: 110)








GACCCCCGAGGT









CACGTGCGTGGTCGTGCACGTCAGCAAGGAGCACGCCGAGGTCCAGTT









CTCCTGCTACC









TGGACGGCGAAGAGGTGCACACGGCCGAGACGAGACCAAAGGAGGAG









CAGTTCAACAGC









ACTTACCGCGTGGTCAGCCTCCTGCCCATCCAGCACGAGGACTGGCTG









AAGGGGAAGGA









CTTCCAGTGCAACGTCAACAACGAACACGTCCCACGCCCCACGACGA









GCACCATCTCCA









AGCCCAAAGGGGTGGTACGGAGCCCGGAGGTGTACACCCTGCCCCCA









CCCGCCGAGGA









GCTGTCCAAGAGCATAGTCACGCTAACCTGCCTGGTCAAAAGCTTCTT









CCCGCCTTTCAT









CGATGTTGAGTGGAAAATCAACGCAAAACCAGAGGCAGAGAACCCATA









CCCCACCACCC









CGCCCCAGGAGGACGAGGACGGGACCTACTTCCTGTACAGCAAGTTCT









CGGTGGAAAAG









TTCAGGTGGCACAGTGGAGGCATCCACTGTGCGGTGATGCACGAGGCT









CTGCACAACCA









CTAGACCC









(SEQ ID NO: 111)








IgG6
CCCCCCAAGACGCCCCCATTAGTCTACCCTCTGGCCCCCTGCGGCACG
APKTAPSVYPLAPCGRDTSGPNVALG
EU372655







GACACGTCTG
CLASSYFPEPVTLTWNSGALTSGVHT








GCCCTAACGTGGCCTTGGGCTGCCTGGCCTCAAGCTACTTCCCCGAGC
FPSVLQPSGLYSLSSMVTVPASSLSS








CAGTGACCCTG
KSYTCNVNHPATTTKVDLCVGRPCPI








ACCTGGAACTCGGGCGCCCTGACCAGTGGCGTGCATACCTTCCCATCC
CPACEGPGPSVFIFPPKPKDTLMISRT








GTCCTGCAGCC
PQVTCVVVDVSQENPEVQFSWYVDG








GTCAGCCCTGTACTCCCTCAGCAGCATGGTGACCGGCCGGCCAGCAGC
VEVHTAQTRPKEQFNSTYRVVSVLPI








CTGTCCAGCA
QHEDWLKGKEFECKVNNKDLPAPITRII








AGAGCTACACCTGCAATGTCAACCACCCGGCCACCACCACCAAGGTGG
SKSKGPSREPQVYTLSPSAEELSRSKV








ACCTGTGTGTT
SITCLVTGFYPPDIDVEWKSNGQPEPE








GGACGACCATCTCCCATATGCCCAGCCTGTGAAGGGCCCGGGCCCTCG
GNYRTTPPQQDVDGTYFLYSKLAVDK








GTCTTCATCTT
ASWQRGDPFQCAVMHEALHNHT








CCCTCCAAAACCCAAGGACACCCTCATGATCTCCCGGACACGCCAGGT
(SEQ ID NO: 112)








CACGTGCGTGG









TGGTAGATGTGAGCCAGGAAAACCCGGAGGTCCAGTTCTCCTGGTAT









GTGGACGGTGTA









GAGGTGCACACGGCCCAGACGAGGCCAAAGGAGGCGCAGTTCAACAGC









ACCTACCGTGT









GGTCAGCGTCCTGCCCATCCAGCACGAGGACTGGCTGAAGGGGAAGGA









GTTCGAGTGCA









AGGTCAACAACAAAGACCTCCCAGCCCGCATGACAAGGATCATCTGC









AAGACCAAAGGG









CCGAGCCGGGAGCCACAGGTGTACACCCTGTCCGCATCCGCCGAGGAG









CTGTCCAGGA









GCAAAGTCAGCATAACCTGCCTGGTCACTGGCTTCTACCCACCTGACA









TCGATGTCGAG









TGGAACAGCAACGCACAGCCGGAGCCAGAGGGCAATTACCCCACCACC









CCGCCCCAGC









AGGACGTGGACGGGACCTACTTCCTGTACAGCAAGCTCGCGGTGGAC









AAGGCCAGCTGG









CAGCGTGTGAGACCCATTCCAGTGTGCGGTGATGCACGAGGCTCTGCA









CAACCACTACACCC









(SEQ ID NO: 113)








IgG6
CCCCCCAAGACGCCCCCATCGGTCTACCCTCTCGCCCCCTGCCCCAC
APKTAPSVYPLAPCGRDTSGPNVALG
EU372653







CCACACCTCTC
CLASSYFPEPVTVTWNSGALTSGVHT








GCCCTAACGTGCCCTTGGGCTGCCTGGCCTCAAGCTACTTCCCCGAGC
FPSVLQPSGLYSLSSTVTVPARSSSRK








CAGTGACCGTG
CFTCNVNHPATTTKVDLCVGRPCPIC








ACCTGGAACTCGGGCGCCCTGACCAGTGGCGTGCACACCTTCCCATGC
PACEGNGPSVFIFPPKPKTLMISRTP








GTCGTGCAGCC
EVTCVVVDVSQENEPEVQFSWYVDGEE








GTCAGCCCTCTACTCCCTCAGCAGCACGGTGACCGTGCCGCCCAGGAG
VHTAETRPKEEQFNSTRYVVSVLPIQH








CTCGTCCAGAA
QDWLKGKEFECKVNNDLPAPITRIISK








ACTGCTTCACGTGCAATGTCAACCACCCGGCCACCACCACCAAGGTGG
AKGPSREPQVYTLSPSAEELSRSKVSI








ACCTGTGTGTT
TLLVTGFYPPDIDVEWKSNGQPEPEG








GGACGACCATGTCCCATATGCCCAGCCTGTGAAGGGAACGGGCCCTCG
NYRSTPPQEDEDGTYFLYSKLAVDKA








GTCTTCATGTT
RLQSGGIHCAVMHEALHNHYTQKSISK








CCCTCGAAAACCCAAGGACACCCTCATCATCTCCCGGACCCCCGAGCT
T








CACGTGGCTCC
(SEQ ID NO: 112)








TGGTAGATGTGAGCCAGGAAAACCCGGAGGTCCAGTTCTCCTGGTACG









TGGACGGCGAA









GAGGTGCACACGGCCGAGACGAGGCCAAAGGAGGAGCAGTTCAACAG









CACCTACCGTGT









GGTCAGCCTCCTGCCCATCCAGCACCAGGACTGGCTGAAGGGAAAGG









AGTTCGAGTGCA









AGCTCAACAACAAAGACCTCCCAGCCCCCATCACAAGGATCATCTCC









AAGGCCAAAGGG









CCGAGGCGGGAGCCGCAGGTGTACACCCTGTCCCCATCCGCCGAGGAG









CTGTCCAGGA









GCAAAGTCAGCATAACCTGCCTGGTCACTGGCTTCTACCCACCTGAC









ATCGATGTCGAG









TGCAAGAGCAACGGAGACCCGGAGCCAGAGGGCAATTACCGCTCCAC









CCCGCCCCAGGA









GGACGAGGACGGGACCTACTTCCTGTACAGCAAACTCGCGGTGGACA









AGGCGAGGTTGC









AGAGTGCAGGCATCCACTGTGCGGTGATGCACGAGGCTCTGCACAACC









ACTACACCCAG









AAGTCCATCCCAAGACT









(SEQ ID NO: 115)







Por-
Ig


FP312892
http://www.
Schwartz



cine
kappa



imgt.org/
J.C.



Ig
(CK)



IMGT
et al



light
variant



reportoire/
Immuno-



chain
1



index.
genetics



con-
Ig


CU604948
ghp?section
84, 303-



stant
kappa



=locus
313 (2012)



region
(CK)



Genes&
PMID:




variant



reportoire=
22108543




2



genetable&









species=










Pig










&group=IGLC





Ig


CU407669
http://www.





lambda



imgt.org/





(CL)



IMGT





variant



reportoire/





1



index.





Ig


CU467599
ghp?section





lambda



=locus





(CL)



Genes&





variant



reportoire=





2



genetable&









species=










Pig










&group=IGKC






Water
Water
IgG1?
GAGCGGCGTGCACACCTTCCCGGCCGTCCTTCAGTCC
SGVHTFPAVLQSSGLYSLSSTVTAPAS
NW_
Not
None


buffalo
bu-

TCCGGGCTCTACTCTCTGAGCAGCACGGTGACCGCGC
ATKSQTFTCNVAHPASSTKVDKAVVP
005690903
registered



(Scientific
ffalo

CCCCCAGCGCCACAAAAAGCCAGACCTTCACCTGCAA
PCRPKPCDCCPPPELPGGPSVFIFPPK





Name:
Ig

CGTAGCCCACCCGGCCAGCAGCACCAAGGTGGACAAG
PKDTLTISGTPEVTCVVVDVGHDPEV






Bubalus

havy

GCTGTTGTTGCCCCATGCAGACCGAAACCCTGTGATTG
KFSWFVDDVEVNTARTKPREEQFNSTY






bubalis)
chain

CTGCCCACCCCCTGAGCTCCCCGGAGGACCCTCTGTC
RVVSALPIQHNDWTGGKEFKCKVYNEG






con-

TTCATCTTCCCACCAAAACCCAAGGACACCCTCACAAT
LPAPIVRTISRTKGQAREPQVYVLAPP






stant

CTCTGGAACTCCTGAGGTCACGTGTGTGGTGGTGGAC
QDELSKSTVSITCMVTGFYPDYIAVEW






(CJ1

GTGGGCCAGGATGACCCCGAGGTGAAGTTCTCCTGGT
QKDGQPESEDKYGTTPPQLDSDGSYF






CH3)

TCGTCGACGATGTGGAGGTAAACACAGCCAGGACGAA
LYSRLRVNKNSWQEGAYICVVMHE








GCCAAGAGAGGAGCAGTTCAACAGCACCTACTCGCGTG
(SEQ ID NO: 118)








GTCAGCGCCCTGCCCATCCAGCACAACGACTGGACTG









GAGGAAAGGAGTTCAAGTGCAAGGTCTACAATGAAGGC









CTCCCAGCCCCCATCGTGAGGACCATCTCCAGGACCA









AAGGGCAGGCCCGGGAGCCGCAGGTGTACGTCCTGGC









CCGACCCCAGGACGAGCTCACCAAAAGCACGGTCAGC









ATCACTTGCATGGTCACTGGCTTCTACCCAGACTACAT









CGCCGTAGAGTGGCAGAAAGATGGGCAGCCTGAGTCA









GAGGACAAATATGGCACGACCCCGCCCCAGCTGGACA









GCGATGGCTCCTACTTCCTGTACAGCAGGCTCAGGGT









GAACAAGAACAGCTGGCAAGAAGGAGGCGCCTACACG









TGTGTAGTGATGCATGAGGC









(SEQ ID NO: 119)








IgG2?
GCCTCCATCACAGCCCCGAAAGTCTACCCTCTGACTTC
ASITAPKVYPLTSCRGETSSSTVTLGC
NW_







TTGCCGCGCGGAAACGTCCAGCTCCACCGTGACCCTG
LVSSYMPEPVTVTWNSGALKSGVHTF
005766143







GGCTGCCTGGTGTCCAGCTACATGCCCGAGCCGGTGA
PAVLQSSGLYSLSSTVTAPASATKSQT








CGGTGACCTGGAACTCGGGTGCCGTGAAGAGCGGCGT
FTCNVAHPASSTKVDTAVGFSSDCCK








GCACACCTTCCCGGCCGTCCTTCAGTCCTCTGGGCTC
FPKPCVRPGSVFIFPPKPKDTLMITGNP








TACTCTCTCAGCAGCACGGTGACCGCGCCCGCCAGCG
EVTCVVDVGRDNPEVQFSWFVGDVE








CCACAAAAAGCCAGACCTTCACCTGCAACGTAGCCCAC
VHTGRSKPREEQFNSTRYVVSTLPIQH








CCGGCCAGCAGCACCAAGGTGGACACGGCTGTTGGGT
NDWTGGKEFKCKVNKGLPAPIVRTIS








TCTCGAGTGACTGCTGCAAGTTTCCTAAGCCTTGTGTG
RIIKGQAREPQVYLAPPQEELLSKSTVS








AGGGGACCATCTGTCTTCATCTTCCCGCCGAAACCCAA
VTCMVTGFYPDYIAVEWHRDRQAESED








AGACACCCTGATGATCACAGGAAATCCCGAGGTCACAT
KYRTTPPQLDSDGSYFLYSRLKVNKNS








GTGTGGTGGTGGACGTGGGCCGGGATAACCCCGAGGT
WQEGGAYTCVYMHE








GCAGTTCTCCTGGTTCGTGGGTGATGTGGAGGTGCAC
(SEQ ID NO: 120)








ACGGGCAGGTCGAAGCCGAGAGAGGAGCAGTTCAACA









GCACCTAGCGCGTGGTCAGCACCCTGCCCATCCAGCA









CAATGACTGGACTGGAGGAAAGGAGTTCAAGTGCAAG









GTCAACAACAAAGGCCTCCCAGCCCCCATCGTGAGGA









CCATCTCCAGGACCAAAGGGCAGGCCCGGGAGCCGCA









GGTGTACGTCCTGGCCCCACCCCAGGAAGAGCTCAGC









AAAAGCACGGTCAGCGTCACTTCCATGGTCACTGGCTT









CTACCCAGACTACATCGCCGTAGAGTCGCATAGAGACC









GGCAGGCTGAGTCGGAGGACAAGTACCGCACGACCCC









GCCCCAGCTGGACAGCGATGGCTCCTACTTCCTGTAC









AGCAGGCTCAAGGTGAACAAGAACAGCTGGCAAGAAG









GAGGCGCCTACACGTGTGTAGTGATGCATGAGGC









(SEQ ID NO: 121)








IgG3?
GCCTCCACCACAGCCCCGAAAGTCTACCCTCTGGCAT
ASTTAPKVYPLASSCGDTSSSTVTLGC
NW_







CCAGCTGCGGGGACACGTCCAGGTCCACCGTGACCCT
LVSSYMPEPVTVTWNSGALKNGVHTF
005784206







GGGCTGCCTGGTCTCCAGCTACATGCCCGAGCCGGTG
PAVRQSSGLYSLSSMVTMPTSTAGTQ








ACCGTGACCTGGAACTCGGGTGCCCTCAAGAACGGCG
TFTCNVAHPASSTKVDTAVTARHPVP








TGCACACCTTCCCGGCCGTCGGGCAGTCCTCCGGGCT
KTPETPIHPVKPPTQEPRDEKTPCQCP








CTACTCTCTCAGCAGCATGGTGACCATGCCCACCAGCA
KCPEPLGGLSVFIFPPKPKDTLTISGTP








CCGCAGGAACCCAGACCTTCACCTGCAACGTAGCCCA
EVTCVVVDVGQDDPEVQFSWFVDDVE








CCCGGCCAGCAGCACCAAGGTGGACACGGCTGTCACT
VHTARMKPREEQFNSTYRVVSALPIQH








GCAAGGCATCCGGTCCCGAAGACACCAGAGACACCTA
QDWLREKEFKCKVNNKGLPAPIVRTISR








TCCATCCTGTAAAACCCCCAACCCAGGAGCCCAGAGAT
TKGQAREPQVYVLAPPREELSKSTLSL








GAAAAGACACCCTGCCAGTGTCCCAAATGCCCAGAACC
TCLITGFYPEEVDVEWQRNGQPESEDK








TCTGGGAGGACTGTCTCTCTTCATCTTCCCACCGAAAC
YHTTPPQLDADGSYFLYSRLRVKRSSW








CCAAGGACACCCTCACAATCTCTGGAACGCCCGAGGT
QEGDHYTCAVMHEALRNHYKEKPISRS








CACGTGTGTGGTGGTGGACGTGGGCCAGGATGACCCC
PGK*








GAAGTGCAGTTCTCCTGGTTCGTGGATGACGTGGAGG
(SEQ ID NO: 122)








TGCACACAGCCAGGATGAAGCCAAGAGAGGAGCAGTT









CAACAGCACCTACCGCGTGGTCAGCGCCCTGCCCATC









CAGCACCAGGACTGGCTGCGGGAAAAGGAGTTCAAGT









GCAAGGTCAACAACAAAGGCCTCCCGGCCCCCATCGT









GAGGACCATCTCCAGGACCAAAGGGCAGGCCCGGGAG









CCACAGGTGTATGTCCTGGCCCCACCCCGGGAAGAGC









TCAGCAAAAGCACGCTCAGCCTCACCTGCCTAATCACC









GGCTTCTACCCAGAAGAGGTAGACGTGGAGTGGCAGA









GAAATGGGCAGCCTGAGTCAGAGGACAAGTACCACAC









GACCCCACCCCAGCTGGACGCTGACGGCTCCTACTTC









CTGTACAGCAGGCTCAGGGTGAACAGGAGCAGCTGGC









AGCAAGGAGACCACTACACGTGTGCAGTGATGCATGAA









GCTTTACGGAATCACTACAAAGAGAAGCCCATCTCGAG









GTCTCCGGCTAAATCA









(SEQ ID NO: 123)







Water
Ig
CAGCCCAAGTCCGCACCCTCAGTCACCCTGTTCCCAC
QPKSAPSVTLFPPSTEELSANKATLVG
NW_
Not
None



bu-
lambda?
CCTCCACGGAGGAGCTCAGCGCCAACAAGGCCACCCT
LISDFYPGSMTVARKADGSTITRNVETT
005690786
registered




ffalo

GGTGTGTCTCATCAGCGACTTCTACCCGGGTAGCATGA
RASKQSNSKYAASSYLSLTGSEWKSKG






Ig

CCGTGGCCAGGAAGGCAGACGGCAGCACCATCACCCG
SYSCEVTHEGSTVTKTVKPSECS*






light

GAACGTGGAGACCACCCGGGCCTCCAAACAGAGCAAC
(SEQ ID NO: 116)






chain

AGCAAGTACGCGGCCACCAGCTACCTCAGCCTGACGG







con-

GCAGCGAGTGGAAATCGAAAGGCAGTTACAGCTGCGA







stant

GGTCACGCACGAGGGGAGCACCGTGACAAAGACAGTG







region

AAGCGCTCAGAGTGTTCTTAG







(CL)

(SEQ ID NO: 117)









The amino acid sequences as shown in SEQ ID NOS: 8 to 13, 28, 30, 32, 34, 36, 38, 40, 42, 44, 46, 48, 50, 52, 54, 56, 58, 60, 62, 64, 66, 68, 70, 72, 74, 76, 78, 80, 82, 84, 86, 88, 90, 92, 94, 96, 98, 100, 102, 104, 106, 108, 110, 112, 114, 116, 118, 120 and 122 may have deletion(s), substitution(s) or addition(s) of one or several (e.g., up to five, about 10 at the 3 most) amino acids. Even when such mutations have been introduced, the resulting amino acid sequences are capable of having the function as the constant region of Ig heavy chain or light chain.


The anti-PD-L1 antibody of the present invention may have a four-chain structure comprising two light chains and two heavy chains.


The anti-PD-L1 antibody of the present invention may be prepared as described below. Briefly, an artificial gene is synthesized which comprises the light chain sequence (variable region sequence and constant region sequence) and the heavy chain sequence (variable region sequence and constant region sequence) of the anti-PD-L1 antibody of the present invention. The resultant gene is inserted into a vector (e.g., plasmid), which is then introduced into a host cell (e.g., mammal cell such as CHO cell). The host cell is cultured, and the antibody of interest is collected from the resultant culture. In the synthesis of the artificial gene, codons of the nucleotide sequence may be optimized.


The present invention provides a DNA encoding an anti-PD-L1 antibody comprising (a) a light chain comprising CDR1 having the amino acid sequence of KSISKY (SEQ ID NO: 1), CDR2 having the amino acid sequence of SGS and CDR3 having the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2) and (b) a heavy chain comprising CDR1 having the amino acid sequence of GYTFTDYI (SEQ ID NO: 3). CDR2 having the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and CDR3 having the amino acid sequence of ARGITMMVVISHWKFDF (SEQ ID NO: 5). The present invention also provides a DNA encoding a light chain of an anti-PD-L1 antibody comprising CDR1 having the amino acid sequence of KSISKY (SEQ ID NO: 1), CDR2 having the amino acid sequence of SGS and CDR3 having the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2) (the DNA of (a′)). Further, the present invention provides a DNA encoding a heavy chain of an anti-PD-L1 antibody comprising CDR1 having the amino acid sequence of GYTFTDYI (SEQ ID NO: 3), CDR2 having the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and CDR3 having the amino acid sequence of ARGITMMVVISHWKFDF (SEQ ID NO: 5) (the DNA of (b′)).


For (a) a light chain comprising CDR1 having the amino acid sequence of KSISKY (SEQ ID NO: 1), CDR2 having the amino acid sequence of SGS and CDR3 having the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2) and (b) a heavy chain comprising CDR1 having the amino acid sequence of GYTFTDYI (SEQ ID NO: 3), CDR2 having the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and CDR3 having the amino acid sequence of ARGITMMVVISHWKFDF (SEQ ID NO: 5), reference should be had to the foregoing description. A DNA comprising the DNA of (a′) and the DNA of (‘b) may be synthesized on commercial synthesizer. Restriction enzyme recognition sites, KOZAK sequences, poly-A addition signal sequences, promoter sequences, intron sequences or the like may be added to this DNA.


The present invention also provides a vector comprising the above-mentioned DNA encoding an anti-PD-L1 antibody.


As the vector, Escherichia coli-derived plasmids (e.g., pBR322, pBR325, pUC12 or pUC13); Bacillus subtilis-derived plasmids (e.g., pUB110, pTP5 or pC194), yeast-derived plasmids (e.g., pSH19 or pSH15); bacteriophages such as λ phage; animal viruses such as retrovirus or vaccinia virus; or insect pathogen viruses such as baculovirus may be used. In the Examples described later, pDC6 (Japanese Patent No. 5704753, U.S. Pat. No. 9,096,878, EU Patent 2385115, Hong Kong (China) patent HK1163739 and Australia Patent 2009331326) is used.


The vector may also comprise promoters, enhancers, splicing signals, poly-A addition signals, intron sequences, selection markers, SV40 replication origins, and so forth.


The present invention also provides a host cell transformed by the above vector. It is possible to prepare the anti-PD-L1 antibody of the invention by culturing the host cell and collecting the antibody of interest from the resultant culture. Therefore, the present invention also provides a method of preparing an antibody, comprising culturing the above-described host cell and collecting the anti-PD-L1 antibody of the invention from the culture. In the method of the present invention for preparing an antibody, a vector incorporating a DNA comprising a DNA encoding the light chain and a DNA encoding the heavy chain may be transfected into a host cell. Alternatively, a vector incorporating a DNA encoding the light chain and a vector incorporating a DNA encoding the heavy chain may be co-transfected into a host cell.


Examples of the host cell include, but are not limited to, bacterial cells (such as Escherichia bacteria, Bacillus bacteria or Bacillus subtilis), fungal cells (such as yeast or Aspergillus), insect cells (such as S2 cells or Sf cells), animal cells (such as CHO cells, COS cells. HeLa cells. C127 cells, 3T3 cells. BHK cells or HEK 293 cells) and plant cells. Among these, CHO-DG44 cell (CHO-DG44(dfhr−/−)) which is a dihydrofolate reductase deficient cell is preferable.


Introduction of a recombinant vector into a host cell may be performed by the methods disclosed in Molecular Cloning 2nd Edition, J. Sambrook et al., Cold Spring Harbor Lab. Press, 1989 (e.g., the calcium phosphate method, the DEAE-dextran method, transfection, microinjection, lipofection, electroporation, transduction, scrape loading, the shotgun method, etc.) or by infection.


The resultant transformant may be cultured in a medium, followed by collection of the anti-PD-L1 antibody of the present invention from the culture. When the antibody is secreted into the medium, the medium may be recovered, followed by isolation and purification of the antibody from the medium. When the antibody is produced within the transformed cells, the cells may be lysed, followed by isolation and purification of the antibody from the cell lysate.


Examples of the medium include, but are not limited to, OptiCHO medium, Dynamis medium, CD CHO medium, ActiCHO medium. FortiCHO medium, Ex-Cell CD CHO medium. BalanCD CHO medium, ProCHO 5 medium and Cellvento CHO-100 medium.


The pH of the medium varies depending on the cell to be cultured. Generally, a pH range from 6.8 to 7.6 is used; mostly, a pH range from 7.0 to 7.4 is appropriate.


When the cell to be cultured is CHO cells, culture may be performed by methods known to those skilled in the art. For example, it is usually possible to perform culturing in a gas-phase atmosphere having a CO2 concentration of 0-40%, preferably 2-10%, at 30-39° C., preferably around 37° C.


The appropriate period of culture is usually from one day to three months, preferably from one day to three weeks.


Isolation and purification of the antibody may be performed by known methods. Known isolation/purification methods which may be used in the present invention include, but are not limited to, methods using difference in solubility (such as salting-out or solvent precipitation); methods using difference in molecular weight (such as dialysis, ultrafiltration, gel filtration or SDS-polyacrylamide gel electrophoresis); methods using difference in electric charge (such as ion exchange chromatography); methods using specific affinity (such as affinity chromatography); methods using difference in hydrophobicity (such as reversed phase high performance liquid chromatography): and methods using difference in isoelectric point (such as isoelectnc focusing).


It is also possible to prepare the anti-PD-L1 antibody of the present invention by culturing a hybridoma which may be prepared by the method disclosed in the literature (Ikebuchi R, Konnai S, Okagawa T, Yokoyama K, Nakajima C, Suzuki Y. Murata S, Ohashi K, Immunology. 2014 August; 142(4):551-61). A hybridoma producing anti-PD-L1 antibody 6C11-3A11 is stored at the laboratory of the present inventors (Laboratory of Infectious Diseases, Department of Disease Control, Faculty of Veterinary Medicine, Hokkaido University).


The PD-L1 antibody of the present invention may be used for detecting PD-L. Therefore, the present invention provides a composition for detecting PD-L1, comprising the PD-L1 antibody as an active ingredient.


Detection of PD-L1 may be performed by such methods including, but are not limited to, immunohistochemical staining, immunocytochemical staining, flow cytometry, enzyme linked immunosorbent assay (ELISA) and Western blotting.


Analytes for detection may be exemplified by samples such as tissues or body fluids taken from organisms (e.g., blood (whole blood, plasma, serum, or specific cell such as erythrocyte, leukocyte or lymphocyte), urine, saliva, etc.); cell culture; and cultured cells (established cell lines, primary cultured cells, subcultured cells, etc.). The source of such analytes is not particularly limited. Examples include rat, canine, ovine, goat, porcine, feline, human, equine, bovine, water buffalo, yak, rabbit, mouse, hamster, and guinea pig.


The PD-L1 antibody of the present invention may be labeled with radioisotopes, enzymes, luminescent substances, fluorescent substances, biotin, or the like. If reaction with a primary antibody (the anti-PD-L1 antibody of the present invention) which specifically binds to a target molecule (PD-L1) is followed by reaction with a secondary antibody which binds to the primary antibody so as to detect the target molecule, it is suitable to label the secondary antibody.


Since PD-L1 is strongly expressed in cancer cells and virus-infected cells, the composition of the present invention may be used for diagnosis of cancers and/or infections. Usually, the amount (concentration) of PD-L in an analyte is determined based on the amount (concentration) of the complex of PD-L1 and anti-PD-L1 antibody. When the amount (concentration) of PD-L1 in the analyte is high compared to negative control (e.g., healthy surrounding tissue (connecting tissue, blood vessels, etc.)), the analyte may be diagnosed as suffering cancer and/or infection. Alternatively, if PD-L1 is detected in the analyte, the analyte may be diagnosed as suffering cancer and/or infection.


Examples of cancers and/or infections include, but are not limited to, neoplastic diseases (e.g., malignant melanoma, lung cancer, gastric cancer, renal cancer, breast cancer, bladder cancer, esophageal cancer, ovarian cancer and the like), leukemia, Johne's disease, anaplasmosis, bacterial mastitis, mycotic mastitis, mycoplasma infections (such as inycoplasma mastitis, mycoplasma pneumonia or the like), tuberculosis, Theileria orientalis infection, cryptosporidiosis, coccidiosis, trypanosomiasis and leishmaniasis.


The composition of the present invention can be used to select subject animals suitable for therapy using an anti-PD-L1 antibody. For example, animals satisfying the following two points may be considered as candidate animals.


1. A case diagnosed as suffering cancer (such as melanoma) or infection in pathological examination


2. A case found positive for anti-PD-L1 antibody


Negative control may be healthy surrounding tissue (connecting tissue, blood vessels, etc.), and positive control may be a case of cancer (such as melanoma) or infection. Basically, animals with a tumor which is positive in immunohistochemical staining of almost all regions may be subjected to clinical trial.


Subject animals are not particularly limited and may include rat, canine, ovine, goat, porcine, feline, human, equine, bovine, water buffalo, yak, rabbit, mouse, hamster, and guinea pig.


The composition of the present invention may further comprise reagents for detecting labels, diluents, lavage fluids, written instructions describing criteria for diagnosis/selection, and so on.


EXAMPLES

Hereinbelow, the present invention will be described in more detail with reference to the following Examples. However, the present invention is not limited to these Examples.


Example 1

1. Introduction


Programmed cell death 1 (PD-1), an immunoinhibitory receptor, and its ligand programmed cell death ligand 1 (PD-L1) are molecules identified by Prof. Tasuku Honjo et al., Kyoto University, as factors which inhibit excessive immune response and are deeply involved in immunotolerance. Recently, it has been elucidated that these molecules are also involved in immunosuppression in infections and tumors in various animals. In the subject Example, an anti-bovine PD-L1 monoclonal antibody was prepared by immunizing rats, and then a clone (6C11-3A11) capable of detecting canine PD-L1 was selected. Further, the present inventors performed immunohistochemical staining to examine whether or not this anti-bovine PD-L1 antibody 6C11-3A11 would be useful for detecting PD-L1 in canine malignant tumors (such as melanoma) and porcine/ovine infections.


2. Materials and Methods


2.1 Rat Anti-Bovine PD-L1 Monoclonal Antibody Producing Cells


The nucleotide sequence of bovine PD-L1 was identified (Ikebuchi R, Konnai S, Shirai T. Sunden Y, Murata S. Onuma M, Ohashi K. Vet Res. 2011 Sep. 26:42:103). Based on the sequence information, a recombinant bovine PD-L1 was prepared. Rat was immunized in the footpad with this recombinant protein, and hybridomas were established by the iliac lymph node method. As a result, a plurality of hybridomas producing rat anti-bovine PD-L1 monoclonal antibodies were obtained (Ikebuchi R, Konnai S, Okagawa T, Yokoyama K, Nakajima C, Suzuki Y, Murata S, Ohashi K. Immunology 2014 August; 142(4):551-561). Rat anti-bovine PD-L1 antibody 6C11-3A11 is one of the monoclonal antibodies established from the above-described immunized rat.


2.2 Identification of Full-Length Canine PD-L1 Gene


To determine the full length of canine PD-L1 cDNA, PCR primers were first designed based on the putative nucleotide sequence of canine PD-L1 already registered at The National Center for Biotechnology Information (NCBI) (GenBank accession number; XM_541302). Briefly, primers to amplify the inner sequence of the open reading frame (ORF) of this gene were designed (cPD-1 inner F and R), and PCR was performed. For the amplified products, nucleotide sequences were determined with a capillary sequencer according to conventional methods. Further, to determine the nucleotide sequence of full-length PD-L1 cDNA, primers (cPD-L1 5′ GSP and 3′GSP) were designed based on the canine PD-L1 cDNA sequences determined above. 5′-RACE and 3-RACE were then performed using, respectively, the 5′-RACE system for rapid amplification of cDNA ends and 3′-RACE system for rapid amplification of cDNA ends (Invitrogen). The resultant gene fragments of interest were sequenced as described above (Maekawa N, Konnai S, Ikebuchi R, Okagawa T, Adachi M, Takagi S, Kagawa Y. Nakajima C, Suzuki Y. Murata S, Ohashi K. PLoS One. 2014 Jun. 10; 9(6):e98415).











Primer (cPD-L1 inner F): 



(SEQ ID NO: 22)



ATGAGAATGTTTAGTGTCTT







Primer (cPD-L1 inner R): 



(SEQ ID NO: 23)



TTATGTCTCTTCAAATTGTATATC







Primer (cPD-L1 5′GSP):



(SEQ ID NO: 24)



TTTTAGACAGAAAGTGA







Primer (cPD-L1 3′GSP):



(SEQ ID NO: 25)



GACCAGCTCTTCTTGGGGAA







2.3 Preparation of Canine PD-L1 Expressing COS-7 Cells


For preparing a canine PD-L1-EGFP expression plasmid, PCR was performed using a synthesized beagle PBMC-derived cDNA as a template and primers designed by adding BglII and EcoRI recognition sites on the 5′ side (cPD-L1-EGFP F and R). The resultant PCR products were digested with BglII (New England Biolabs) and EcoRI (Takara), and then purified with FastGene Gel/PCR Extraction Kit (NIPPON Genetics), followed by cloning into pEGFP-N2 vector (Clontech) similarly treated with restriction enzymes. The resultant expression plasmid of interest was extracted with QIAGEN Plasmid Midi kit (Qiagen) and stored at −30° C. until use in experiments. Hereinafter, the thus prepared expression plasmid is designated as pEGFP-N2-cPD-L1.











Primer (cPD-L1-EGFP F):



(SEQ ID NO: 26)



GAAGATCTATGAGAATGTTTAGTGTC







Primer (cPD-L1-EGFP R):



(SEQ ID NO: 27)



GGAATTCTGTCTCTTCAAATTGTATATC






COS-7 cells were subcultured at a density of 5×104 cells/cm in 6-well plates, and then cultured overnight in RPMI 1640 medium containing 10% inactivated fetal bovine serum and 0.01% L-glutamine at 37° C. in the presence of 5% CO2. The pEGFP-N2-cPD-L1 or pEGFP-N2 (negative control) was introduced into COS-7 cells at 0.4 μg/cm2 using Lipofectamine 2000 (Invitrogen). The cells were cultured for 48 hours (canine cPD-L-EGFP expressing cell and EGFP expressing cell). In order to confirm the expression of PD-L1 in the thus prepared expressing cells, intracellular localization of enhanced green fluorescent protein (EGFP) was visualized with an inverted confocal laser microscope LSM700 (ZEISS) (Maekawa N, Konnai S, Ikebuchi R, Okagawa T, Adachi M. Takagi S, Kagawa Y, Nakajima C, Suzuki Y, Murata S, Ohashi K. PLoS One. 2014 Jun. 10; 9(6):e98415).


2.4 Cross-Reactivity of Rat Anti-Bovine PD-L1 Antibody 6C11-3A11 with Canine PD-L1


In order to confirm that rat anti-bovine PD-L1 antibody 6C1-3A11 specifically binds to canine PD-L1, flow cytometry was performed using the canine cPD-L1-EGFP expressing cell or the EGFP expressing cell prepared in 2.3 above. To 2×105-1×106 cells, 10 μg/ml of anti-bovine PD-L1 antibody 6C11-3A11 was added and reacted for 30 min at room temperature. After washing, the antibody binding to cell surfaces was detected with Allophycocyanine-labeled goat anti-rat Ig antibody (Beckman Coulter). For the analysis, FACS Verse (Becton. Dickinson and Company) was used. As a negative control antibody, rat IgG2a (κ) isotype control (BD Bioscience) was used. For every washing operation and dilution of antibodies, 10% inactivated goat serum-supplemented PBS was used. The results are shown in FIG. 1.


2.5 CDR Analysis of Rat Anti-Bovine PD-L1 Antibody 6C1-3A11


The heavy chain and the light chain genes of rat anti-bovine PD-L1 antibody 6C11-3A11 were identified from a hybridoma producing the antibody by RACE method. The complementarity-determining regions (CDRs) of rat anti-bovine PD-L1 antibody 6C11-3A11 were determined using NCBI IGBLAST (http://www.ncbi.nlm.nih.gov/igblast/). The results are shown in FIG. 2.


2.6 Immunohistochemical Staining of Canine Tumor Tissues and Ovine/Porcine Infected Tissues


In order to confirm that rat anti-bovine PD-L1 antibody 6C11-3A1 is applicable to PD-L1 immunohistochemical staining of canine tumors, formalin-fixed and paraffin-embedded canine tumor samples were immunohistochemically stained. According to conventional methods, the resultant samples were deparaffinized and then subjected to microwave treatment (5 min, twice) in citrate buffer. Subsequently, the samples were reacted with PD-L1 antibody 6C11-3A11 (400-fold dilution) for 30 min and then with Simple Stain Mouse MAX-PO (Rat) (Nichirei Bioscience) for 30 mm. For coloring, diaminobenzidine (DAB) was reacted for 10 min.


The results are shown in FIGS. 3, 4, 5-1, 5-2, 6 and 7.


Anti-MelanA antibody, the only commercially available antibody specific to melanoma, stained tumor cells very weakly (FIG. 3, left). On the other hand, the PD-L1 antibody (6C11-3A11) established by the present inventors stained tumor cells very strongly (FIG. 3. Right). The PD-L1 antibody (6C11-3A11) was capable of staining almost all cases of melanoma.


In canine melanoma, tumor cells were found diffusely positive for the PD-L1 antibody (6C1-3A11). (Positive number/tested number=12/12: positive rate 100%)


In canine lymphoma, tumor cells were found diffusely positive for the PD-L1 antibody (6C11-3A11). In canine osteosarcoma, some tumor cells were stained intracellularly. In canine renal cell carcinoma, tumor cells were found diffusely positive in various tissue types.


In a case of ovine listeriosis, a PD-L1 staining image of a brain lesion of ovine listeriosis showing neurologic symptoms is shown in FIG. 6, left panel. In an enlarged photograph of this image, expression of PD-L1 was observed in macrophages infiltrating into brain lesions (FIG. 6, Right).


In a case of porcine circovirus type 2 infection, PD-L1 was stained with lymphoid follicles, and virus was stained in these cells (FIG. 7, Left).


In a case of porcine mycoplasma pneumonia, a great number of macrophages infiltrated pulmonary lesions, and PD-L1 was stained in these infiltrating cells (FIG. 7, Right).


As described so far, anti-bovine PD-L1 antibody 6C11-3A11 may be used for detecting PD-L1 in various canine tumors (such as malignant melanoma) and ovine/porcine infections by immunohistochemical staining. This suggests the possibility of using anti-bovine PD-L1 antibody 6C11-3A11 for diagnosis in a multiple-animal and a multiple-disease manner.


Example 2J

1. Introduction


Monoclonal antibodies may be produced by culturing hybridomas and purifying antibodies from the resultant culture supernatants. Alternatively, when the nucleotide sequence of an antibody of interest has been identified, a cell expressing the antibody may be prepared by transfecting cultured cells with a vector for expressing the nucleotide sequence; the thus prepared antibody expressing cell may be used as a substitute for hybridoma. In the subject Example, a method will be illustrated below in which an antibody is produced by a protein expression system using an expression vector and a mammalian cell.


2. Materials and Methods


2.1 Preparation of Rat Anti-Bovine PD-L1 Antibody 6C11-3A1 Expression Vector


Based on the nucleotide sequence of rat anti-bovine PD-L1 antibody 6C1-3A11 identified in 2.5 of Example 1 above, gene synthesis is performed so that NotI restriction enzyme recognition site, KOZAK sequence, antibody's light chain sequence, poly-A addition signal sequence (PABGH), promoter sequence (PCMV), SacI restriction enzyme recognition site, intron sequence (INRBG), KOZAK sequence, antibody's heavy chain sequence and XbaI restriction enzyme recognition site will be located in this order. In this case, codons of the antibody gene may have been optimized in advance depending on the type of the cell that is to express the gene. The synthesized gene strand is incorporated into an expression vector pDC6 (kindly provided by Prof. S. Suzuki, Research Center for Zoonosis Control, Hokkaido University) at the cloning site (NotI and XbaI restriction enzyme recognition sequences located downstream of PCMV and between INRBG and PABGH) using restriction enzyme recognition sequences so that the above-listed sequences will be located in the above-mentioned order to thereby construct a rat anti-bovine PD-L1 antibody expressing vector pDC6.


2.2 Expression of Rat Anti-Bovine PD-L1 Antibody 6C11-3A11


The rat anti-bovine PD-L1 antibody expressing vector pDC6 as prepared in 2.1 above is transfected into CHO-DG44 cells (CHO-DG44(dfhr−/−)) which are dihydrofolate reductase deficient cells, and high expression clones are selected by dot blotting. For increased expression, gene amplification treatment may be performed by adding load on cells in a medium containing 60 nM, 250 nM or 1000 nM methotrexate (Mtx). The thus prepared cells stably expressing rat anti-bovine PD-L1 antibody 6C11-3A11 are transferred to Mtx-free Opti-CHO medium. By culturing those cells under shaking for 14 days (125 rpm, 37° C., 5% CO2), a culture supernatant containing the antibody of interest can be obtained. The antibody in the culture supernatant may be purified by known methods such as affinity chromatography or ion exchange chromatography for use in various experiments.


Example 3

1. Introduction


For the purpose of establishing a novel diagnosis method for tumor diseases, a rat-human chimeric anti-PD-L1 antibody is obtained in the subject Example by culturing Chinese hamster ovary cells (CHO cells) that will express a chimeric antibody gene in which the variable region gene of rat anti-bovine PD-L antibody 6C11-3A11 is combined with the constant region gene of human immunoglobulin (IgG4).


2. Materials and Methods


2.1 Preparation of Rat-Human Chimeric Anti-PD-L1 Expression Vector (FIG. 10)


Hereinbelow, a rat-human chimeric anti-PD-L1 antibody is established using rat anti-bovine PD-L1 monoclonal antibody 6C1-3A11 as its variable region.


Briefly, heavy chain and light chain variable region genes were identified from a hybridoma producing the rat anti-bovine PD-L1 antibody 6C11-3A11. Further, a nucleotide sequence was prepared by linking the heavy chain and light chain variable region genes of the above rat antibody to the constant region of heavy chain IgG4 and the constant region of light chain Kappa of a known human antibody, respectively. After codon optimization, gene synthesis is performed so that NotI restriction enzyme recognition site, KOZAK sequence, chimeric antibody's light chain sequence, poly-A addition signal sequence (PABGH), promoter sequence (PCMV), SacI restriction enzyme recognition site, intron sequence (INRBG), KOZAK sequence, chimeric antibody's heavy chain sequence and XbaI restriction enzyme recognition site will be located in this order. The synthesized gene strand is incorporated into the expression vector pDC6 (kindly provided by Prof. S. Suzuki, Research Center for Zoonosis Control, Hokkaido University) at the cloning site (NotI and XbaI restriction enzyme recognition sequences located downstream of PCMV and between INRBG and PABGH) using restriction enzyme recognition sequences so that the above-listed sequences will be located in the above-mentioned order (FIG. 10). Thus, a rat-human chimeric anti-PD-L1 antibody expressing vector is constructed. This expression vector is transfected into CHO-DG44 cells (CHO-DG44(dfhr−/−)) which are dihydrofolate reductase deficient cells, and high expression clones are selected by dot blotting. For increased expression, gene amplification treatment may be performed by adding load on cells in a medium containing 60 nM, 250 nM or 1000 nM methotrexate (Mtx). The thus prepared cells stably expressing rat-human chimeric anti-PD-L1 antibody 6C11-3A11 are transferred to Mtx-free Opti-CHO medium. By culturing those cells under shaking for 14 days (123 rpm, 37° C., 5% CO2), a culture supernatant containing the antibody of interest can be obtained. The antibody in the culture supernatant may be purified by known methods such as affinity chromatography or ion exchange chromatography for use in various experiments.


Example 41

1. Introduction


With respect to PD-L1 in canine tumors, a detection method by immunohistochemical staining with rat anti-bovine PD-L1 antibody 6G7-E1 was previously established, and the expression profiles in various tumors have been reported (Maekawa N, Konnai S, Okagawa T, Ikebuchi R, Izumi Y, Takagi S, Kagawa Y, Nakajima C, Suzuki Y, Kato Y, Murata S. Ohashi K. PLoS One. 2016 Jun. 11(6): e0157176). In the subject Example, in order to examine whether rat anti-bovine PD-L1 antibody 6C11-3A11 is more useful than existing anti-PD-L1 antibody 6G7-E1 in expression analysis of PD-L1 in canine tumors, immunohistochemical staining of various canine tumors was performed to thereby directly compare the PD-L1 detection sensitivities of 6G7-E1 and 6C11-3A11.


2. Materials and Methods


2.1 Comparison by Flow Cytometry Using Canine PD-L-EGFP Stably Expressing CHO-DG44 Cells (FIG. 11)


First, in order to prepare canine PD-L1 membrane expressing cells, 2.5 μg of canine PD-L1-EGFP expression plasmid (pEGFP-N2-cPD-L1) prepared in 2.3 of Example 1 or pEGFP-N2 (negative control) was introduced into 4×106 CHO-DG44 cells using Lipofectamine LTX (Invitrogen). Forty-eight hours later, the medium was exchanged with CD DG44 medium (Life Technologies) containing G418 (Enzo Life Science) 800 μg/ml, GlutaMAX supplement (Life Technologies) 20 ml-L, and 10% Pluronic F-68 (Life Technologies) 18 ml/L, followed by selection of stably expressing cells and cloning by limiting dilution. The thus prepared canine PD-L1 membrane expressing cell or EGFP expressing cell was reacted with rat anti-bovine PD-L1 antibody 6C11-3A11 or 6G7-E1 at room temperature for 30 min. After washing, antibodies binding to cell surfaces were detected with Allophycocyanine-labeled goat anti-rat Ig antibody (Beckman Coulter). For analysis, FACS Verse (Becton. Dickinson and Company) was used. As a negative control, rat IgG2a (κ) or IgM (κ) isotype control (BD Bioscience) was used. For every washing operation and dilution of antibodies, 10% inactivated goat serum-supplemented PBS was used.


The results are shown in FIG. 11. Rat anti-bovine PD-L1 antibodies 6C11-3A11 and 6G7-E1 bound specifically to canine PD-L1 membrane expressing cells. The resultant fluorescence intensity was higher with 6C11-3A11 than with 6G7-E1, suggesting that 6C11-3A11 is an antibody with higher affinity.


2.2 Comparison of the Detection Sensitivities of Both Antibodies in PD-L1 Expression Analysis of Various Canine Tumors (Immunohistochemical Staining)


Using samples of canine skin squamous cell carcinoma (n=5), nasal adenocarcinoma (n=5), transitional cell carcinoma (n=5), anal sac gland carcinoma (n=5), soft tissue sarcoma (n=5) and osteosarcoma (n=5), immunohistochemical staining with rat anti-bovine PD-L1 antibody 6C11-3A11 was performed according to the method described in 2.6 of Example 1. With rat anti-bovine PD-L1 antibody 6G7-E1, immunohistochemical staining was performed in the same manner using sections derived from the same analytes. The final concentration of 6G7-E1 used on this occasion was 10 μg/ml, and biotin-labeled goat anti-rat IgM antibody (Jackson ImmunoResearch Laboratories) was used as a secondary antibody.


The results are shown in FIGS. 12 and 13. While specific signals were not observed in squamous cell carcinoma, nasal adenocarcinoma, transitional cell carcinoma, anal sac gland carcinoma and soft tissue sarcoma upon staining with 6G7-E1, satisfactory positive reactions were obtained upon staining with 6C11-3A11. On the other hand, specific signals were also obtained with 6G7-E1 in osteosarcoma but staining with 6C11-3A11 provided higher signal intensities. The PD-L1 positive rate of these tumors obtained by 6C11-3A11 staining was 100% (5 out of 5 cases) in all of the above-listed tumor species excepting soft tissue sarcoma which turned out to be PD-L1 positive at a rate of 80% (4 out of 5 cases).


Subsequently, samples of oral malignant melanoma (n=17), mammary adenocarcinoma (n=10), histiocytic sarcoma (n=10), diffuse large B-cell lymphoma (n=10) and transmissible venereal tumor (n=4) were immunohistochemically stained with 6C11-3A11 to analyze PD-L1 expression therein.


The results are shown in FIG. 14. The PD-L1 positive rate was 100% in oral malignant melanoma (17 out of 17 cases), 100% in mammary adenocarcinoma (10 out of 10 cases), 20% in histiocytic sarcoma (2 out of 10 cases), 20% in diffuse large B-cell lymphoma (2 out of 10 cases) and 0% in transmissible venereal tumor (0 out of 4 cases).


The above-described results revealed that 6C11-3A1 is superior to the existing anti-PD-L1 antibody 6G7-E1 in the detection of canine PD-L1.


Example 5

1. Introduction


Johne's disease is a bovine chronic infection caused by Mycobacterium avium subsp. paratuberculosis. In cattle affected with Johne's disease. PD-L1 expression has been confirmed in M. avium subsp. paratuberculosis-infected cells in ileal lesions which are a localized site of infection with this bacterium (Okagawa T, Konnai S, Nishimori A, Ikebuchi R, Mizorogi S. Nagata R, Kawaji S. Tanaka S, Kagawa Y. Murata S, Mori Y and Ohashi K. Infect Immun, 84:77-89, 2016). In the subject Example, immunohistochemical staining of ileai lesions of cattle with Johne's disease was performed in order to examine whether rat anti-bovine PD-L1 antibody 6C11-3A11 could be used for detecting bovine PD-L1 or not.


2. Materials and Methods


2.1. Construction of Bovine PD-L1 Expressing Cells


The nucleotide sequence of the full-length cDNA of bovine PD-L1 gene (GenBank accession number ABS10902; Ikebuchi R. Konnai S. Shirai T, Sunden Y, Murata S, Onuma M, Ohashi K Vet. Res. 2011 Sep. 26: 42:103) was determined. Based on the resultant nucleotide sequence, bovine PD-L1 membrane expressing cells were prepared. First, for preparing a bovine PD-L1 expressing plasmid, PCR was performed using a synthesized bovine PBMC-derived cDNA as a template and primers having NheI and XhoI recognition sites added on the 5′ side (boPD-L1-EGFP F and R). The PCR products were digested with NheI (Takara) and XhoI (Takara), purified with FastGene Gel/PCR Extraction Kit (NIPPON Genetics) and cloned into pEGFP-N2 vector (Clontech) that had been subjected to similar restriction enzyme treatments. The resultant expression plasmid of interest was extracted with QIAGEN Plasmid Midi kit (Qiagen) and stored at −30° C. until use in experiments. Hereinafter, the thus prepared expression plasmid is designated as pEGFP-N2-boPD-L1.











Primer (boPD-L1-EGFP F):



(SEQ ID NO: 124)



CTAGCTAGCACCATGAGGATATATAGTGTCTTAAC







Primer (boPD-L1-EGFP R)



(SEQ ID NO: 125)



CAATCTCGAGTTACAGACAGAAGATGACTGC






Bovine PD-L1 membrane expressing cells were prepared by the procedures described below. First, 2.5 μg of pEGFP-N2-boPD-L1 or pEGFP-N2 (negative control) was introduced into 4×106 CHO-DG44 cells using Lipofectamine LTX (Invitrogen). Forty-eight hours later, the medium was exchanged with CD DG44 medium (Life Technologies) containing G418 (Enzo Life Science) 800 μg/ml, GlutaMAX supplement (Life Technologies) 20 ml/L, and 10% Pluronic F-68 (Life Technologies) 18 ml/L; thereafter, selection was performed simultaneously with cloning by limiting dilution (bovine PD-L1 expressing cell and EGFP expressing cell). In order to confirm the expression of bovine PD-L1 in the thus prepared bovine PD-L1 expressing cell, intracellular localization of EGFP was visualized with an inverted confocal laser microscope LSM700 (ZEISS).


2.2. Binding Specificity of Rat Anti-Bovine PD-L1 Antibody 6C11-3A11 to Bovine PD-L1


It was confirmed by flow cytometry that rat anti-bovine PD-L1 antibody 6C11-3A11 specifically binds to the bovine PD-L1 expressing cell (described above). First, rat anti-bovine PD-L1 antibody 6C11-3A11 or rat IgG2a (κ) isotype control (BD Biosciences) as a negative control was reacted with the bovine PD-L1 expressing cell or the EGFP expressing cell (negative control) at room temperature for 30 min. After washing, APC-labeled anti-rat 1 g goat antibody (Southern Biotech) was reacted at room temperature for 30 min. After washing, antibodies bound to cell surfaces were detected by FACS Verse (BD Biosciences). For every washing operation and dilution of antibody. PBS supplemented with 1% bovine serum albumin (Sigma-Aldrich) was used.


The results are shown in FIG. 15. It was revealed that rat anti-bovine PD-L1 antibody 6C11-3A11 binds specifically to the bovine PD-L1 expressing cell.


2.3. Immunohistochemical Staining Using Tissue Samples from Infected Cattle


In order to confirm that rat anti-bovine PD-L1 antibody 6C11-3A11 is applicable to PD-L1 immunohistochemical staining of bovine tissues, immunohistociemical staining was performed with formalin-fixed, paraffin-embedded bovine tissue samples. Briefly, ilium tissue blocks from cattle which naturally developed Johne's disease (#1, presenting clinical symptoms of Johne's disease such as diarrhea and severe emaciation), cattle experimentally infected with M. avium subsp. paratuberculosis (#65, clinical symptoms such as shedding of M. avium subsp. paratuberculosis and diarrhea were observed; Okagawa T. Konnai S, Nishimori A, Ikebuchi R, Mizorogi S, Nagata R, Kawaji S. Tanaka S, Kagawa Y, Murata S, Mori Y and Ohashi K. Infect Immun, 84:77-89, 2016) and uninfected control cattle (C #6) (the blocks kindly provided by Dr. Yasuyuki Mori, National Institute of Animal Health, National Agriculture and Food Research Organization) were used for staining. According to conventional methods, the stained samples were deparaffinized and then subjected to microwave treatment (5 min, twice) in citrate buffer. Subsequently, the samples were reacted with rat anti-bovine PD-L1 antibody 6C11-3A11 (400-fold dilution) for 30 min and then with Simple Stain Mouse MAX-PO (Rat) (Nichirei Bioscience) for 30 min. Finally, the samples were reacted with diarninobenzidine (DAB) for 10 min for coloring, followed by observation with an optical microscope.


The results are shown in FIG. 16. Rat anti-bovine PD-L1 antibody 6C11-3A11 detected expression of PD-L in M. avium subsp. paratuberculosis-infected cells (confirmed by Ziehl-Neelsen staining) in ileal lesions of cattle #1 that naturally developed Johne's disease and experimentally infected cattle #65 (FIG. 16a, b). On the other hand, PD-L1 was not expressed in the ileum of uninfected cattle (C #6), so reaction of rat anti-bovine PD-L1 antibody 6C11-3A11 (non-specific reaction) was not recognized (FIG. 16a).


As described above, it was shown that rat anti-bovine PD-L1 antibody 6C11-3A11 can be used for detecting PD-L1 in bovine tissues by immunohistochemical staining.


All publications, patents and patent applications cited herein are incorporated herein by reference in their entirety.


INDUSTRIAL APPLICABILITY

The anti-PD-L1 antibody of the present invention is applicable to diagnosis of cancers and/or infections. Further, the anti-PD-L1 antibody of the present invention is also applicable to selection of subject animals suitable for therapy with anti-PD-L1 antibodies.














SEQUENCE LISTING FREE TEXT


<SEQ ID NO: 1>


SEQ ID NO: 1 shows the amino acid sequence of CDR1 of the light 





chain variable region (VL) of anti-PD-L1 antibody 6C11-3A11 





(IgG2a).






KSISKY






<SEQ ID NO: 2>




embedded image







<SEQ ID NO: 3>


SEQ ID NO: 3 shows the amino acid sequence of CDR1 of the heavy





chain variable region (VH) of anti-PD-L1 antibody 6C11-3A11 





(IgG2a).






GYTFTDYI






<SEQ ID NO: 4>


SEQ ID NO: 4 shows the amino acid sequence of CDR2 of the VH of





anti-PD-L1 antibody 6C11-3A11 (IgG2a).






INPDSGGN






<SEQ ID NO: 5>




embedded image







<SEQ ID NO: 6>




embedded image







<SEQ ID NO: 7>




embedded image







<SEQ ID NO: 8>


SEQ ID NO: 8 shows the amino acid sequence of the light chain 





(kappa chain) constant region of anti-PD-L1 antibody 6C11-3A11 





(IgG2a).





RADAAPTVSIFPPSTEQLATGGASVVCLMNNFYPRDISVKWKIDGTERRDGVLDSVTDQDSKDST





YSMSSTLSLTKADYESHNLYTCEVVHKTSSSPVVKSFNRNEC*





<SEQ ID NO: 9>


SEQ ID NO: 9 shows the amino acid sequence of the heavy chain 





constant region (CH) of anti-PD-L1 antibody 6C11-3A11 (IgG2a).





AETTAPSVYPLAPGTALKSNSMVTLGCLVKGYFPEPVTVTWNSGALSSGVHTFPAVLQSGLYTLT





SSVTVPSSTWSSQAVTCNVAHPASSTKVDKKIVPRECNPCGCTGSEVSSVFIFPPKTKDVLTITL





TPKVTCVVVDISQNDPEVRFSWFIDDVEVHTAQTHAPEKQSNSTLRSVSELPIVHRDWLNGKTFK





CKVNSGAFPAPIEKSISKPEGTPRGPQVYTMAPPKEEMTQSQVSITCMVKGFYPPDIYTEWKMNG





QPQENYKNTPPTMDTDGSYFLYSKLNVKKETWQQGNTFTCSVLHEGLHNHHTEKSLSHSPGK*





<SEQ ID NO: 10>


SEQ ID NO: 10 shows the amino acid sequence (GenBank: #V01241.1) 





of the light chain (kappa chain) constant region of a rat  





antibody (IgG2a).





ADAAPTVSIFPPSTEQLATGGASVVCLMNNFYPRDISVKWKIDGTERRDGVLDSVTDQDSKDSTY





SMSSTLSLTKADYESHNLYTCEVVHKTSSSPVVKSFNRNEC*





<SEQ ID NO: 11>


SEQ ID NO: 11 shows the amino acid sequence (GenBank: #X16129.1) 





of the light chain (kappa chain) constant region of a rat  





antibody (IgG2a).





RADAAPTVSIFPPSTEQLATGGASVVCLMNNFYPRDISVKWKIDGTERRDGVLDSVTDQDSKDST





YSMSSTLSLSKADYESHNLYTCEVVHKTSSSPVVKSFNRNEC





<SEQ ID NO: 12>


SEQ ID NO: 12 shows the amino acid sequence (GenBank:  





#DQ402471.1) of the light chain (kappa chain) constant region of  





a rat antibody (IgG2a).





AAPTVSIFPPSMEQLTSGGATVVCFVNNFYPRDISVKWKIDGSEQRDGVLDSVTDQDSKDSTYSM





SSTLSLTKVEYERHNLYTCEVVHKTSSSPVVKSFNRNEC*





<SEQ ID NO: 13>


SEQ ID NO: 13 shows the amino acid sequence (GenBank: #DQ402472.1) 





of the CH of a rat antibody (IgG2a).





APSVYPLAPGTALKSNSMVTLGCLVKGYFPEPVTVTWNSGALSSGVHTFPAVLQSGLYTLTSSVT





VPSSTWSSQAVTCNVAHPASSTKVDKKIVPRECNPCGCTGSEVSSVFIFPPKTKDVLTITLTPKV





TCVVVDISQNDPEVRFSWFIDDVEVHTAQTHAPEKQSNSTLRSVSELPIVHRDWLNGKTFKCKVN





SGAFPAPIEKSISKPEGTPRGPQVYTMAPPKEEMTQSQVSITCMVKGFYPPDIYTEWKMNGQPQE





NYKNTPPTMDTDGSYFLYSKLNVKKETWQQGNTFTCSVLHEGLHNHHTEKSLSHSPGK*





<SEQ ID NO: 14>


SEQ ID NO: 14 shows the nucleotide sequence of the VL of 





anti-PD-L1 antibody 6C11-3A11 (IgG2a).





ATGAGGGTCCAGATTCAGTTTTGGGGGCTTCTTCTGCTCTGGACATCAGGTATACAGTGTGATGT





CCAGATGACCCAGTCTCCATCTAATCTTGCTGCCTCTCCTGGAGAAAGTGTTTCCATCAATTGCA





AGGCAAGTAAGAGCATTAGCAAGTATTTAGCCTGGTATCAACAGAAACCTGGGAAAGCAAATAAG





CTTCTTATCTACTCTGGGTCAACTTTGCAATCTGGAACTCCATCGAGGTTCAGTGGCAGTGGATC





TGGTACAGATTTCACTCTCACCATCAGAAACCTGGAGCCTGAAGATTTTGGACTCTATTACTGTC





AACAGCATAATGAATACCCGCTCACGTTCGGTTCTGGGACCAAGCTGGAGATCAAA





<SEQ ID NO: 15>


SEQ ID NO: 15 shows the nucleotide sequence of the VH of 





anti-PD-L1 antibody 6C11-3A11 (IgG2a).





ATGGGATGGATCTGTATCATCTTTCTTGTGGCAATAGCTACAGGTGCCCACTCCCAGGTCAAGCT





GCTGCAGTCTGGGGCTGCACTGGTGAAGCCTGGGGACTCTGTGAAGATGTCTTGCAAAGCTTCTG





GTTATACATTCACTGACTACATTATACACTGGGTGAAGCAGAGTCATGGAAAAAGCCTTGAGTGG





ATTGGTTATATTAATCCTGACAGTGGTGGTAATAACTACAATGAAAAGTTCAAGAGCAAGGCCAC





ATTGACTGTAGACAAATCCAGCAGCACAGCCTATATGGAGTTTAGCAGATTGACATCTGAGGATT





CTGCAATCTACTACTGTGCAAGAGGGATTACCATGATGGTAGTTATTAGCCACTGGAAGTTTGAC





TTCTGGGGCCCAGGAACCATGGTCACCGTGTCCTCA





<SEQ ID NO: 16>


SEQ ID NO: 16 shows the nucleotide sequence of the light chain 





(kappa chain) constant region of anti-PD-L1 antibody 6C11-3A11 





(IgG2a).





CGGGCTGATGCTGCACCAACTGTATCTATCTTCCCACCATCCACGGAACAGTTAGCAACTGGAGG





TGCCTCAGTCGTGTGCCTCATGAACAACTTCTATCCCAGAGACATCAGTGTCAAGTGGAAGATTG





ATGGCACTGAACGACGAGATGGTGTCCTGGACAGTGTTACTGATCAGGACAGCAAAGACAGCACG





TACAGCATGAGCAGCACCCTCTCGTTGACCAAGGCTGACTATGAAAGTCATAACCTCTATACCTG





TGAGGTTGTTCATAAGACATCATCCTCACCCGTCGTCAAGAGCTTCAACAGGAATGAGTGTTAG





<SEQ ID NO: 17>


SEQ ID NO: 17 shows the nucleotide sequence of the CH of 





anti-PD-L1 antibody 6C11-3A11 (IgG2a).





GCTGAAACAACAGCCCCATCTGTCTATCCACTGGCTCCTGGAACTGCTCTCAAAAGTAACTCCAT





GGTGACCCTGGGATGCCTGGTCAAGGGCTATTTCCCTGAGCCAGTCACCGTGACCTGGAACTCTG





GAGCCCTGTCCAGCGGTGTGCACACCTTCCCAGCTGTCCTGCAGTCTGGACTCTACACTCTCACC





AGCTCAGTGACTGTACCCTCCAGCACCTGGTCCAGCCAGGCCGTCACCTGCAACGTAGCCCACCC





GGCCAGCAGCACCAAGGTGGACAAGAAAATTGTGCCAAGGGAATGCAATCCTTGTGGATGTACAG





GCTCAGAAGTATCATCTGTCTTCATCTTCCCCCCAAAGACCAAAGATGTGCTCACCATCACTCTG





ACTCCTAAGGTCACGTGTGTTGTGGTAGACATTAGCCAGAATGATCCCGAGGTCCGGTTCAGCTG





GTTTATAGATGACGTGGAAGTCCACACAGCTCAGACTCATGCCCCGGAGAAGCAGTCCAACAGCA





CTTTACGCTCAGTCAGTGAACTCCCCATCGTGCACCGGGACTGGCTCAATGGCAAGACGTTCAAA





TGCAAAGTCAACAGTGGAGCATTCCCTGCCCCCATCGAGAAAAGCATCTCCAAACCCGAAGGCAC





ACCACGAGGTCCACAGGTATACACCATGGCGCCTCCCAAGGAAGAGATGACCCAGAGTCAAGTCA





GTATCACCTGCATGGTAAAAGGCTTCTATCCCCCAGACATTTATACGGAGTGGAAGATGAACGGG





CAGCCACAGGAAAACTACAAGAACACTCCACCTACGATGGACACAGATGGGAGTTACTTCCTCTA





CAGCAAGCTCAATGTAAAGAAAGAAACATGGCAGCAGGGAAACACTTTCACGTGTTCTGTGCTGC





ATGAGGGCCTGCACAACCACCATACTGAGAAGAGTCTCTCCCACTCTCCTGGTAAATGA





<SEQ ID NO: 18>


SEQ ID NO: 18 shows the nucleotide sequence (GenBank: #V01241.1) 





of the light chain (kappa chain) constant region of a rat





antibody (IgG2a).





GGGCTGATGCTGCACCAACTGTATCTATCTTCCCACCATCCACGGAACAGTTAGCAACTGGAGGT





GCCTCAGTCGTGTGCCTCATGAACAACTTCTATCCCAGAGACATCAGTGTCAAGTGGAAGATTGA





TGGCACTGAACGACGAGATGGTGTCCTGGACAGTGTTACTGATCAGGACAGCAAAGACAGCACGT





ACAGCATGAGCAGCACCCTCTCGTTGACCAAGGCTGACTATGAAAGTCATAACCTCTATACCTGT





GAGGTTGTTCATAAGACATCATCCTCACCCGTCGTCAAGAGCTTCAACAGGAATGAGTGTTAG





<SEQ ID NO: 19>


SEQ ID NO: 19 shows the nucleotide sequence (GenBank: #X16129.1) 





of the light chain (kappa chain) constant region of a rat  





antibody (IgG2a).





CGGGCTGATGCTGCACCAACTGTATCTATCTTCCCACCATCCACGGAACAGTTAGCAACTGGAGG





TGCCTCAGTCGTGTGCCTCATGAACAACTTCTATCCCAGAGACATCAGTGTCAAGTGGAAGATTG





ATGGCACTGAACGACGAGATGGTGTCCTGGACAGTGTTACTGATCAGGACAGCAAAGACAGCACG





TACAGCATGAGCAGCACCCTCTCGTTGTCCAAGGCTGACTATGAAAGTCATAACCTCTATACCTG





TGAGGTTGTTCATAAGACATCATCCTCACCCGTCGTCAAGAGCTTCAACAGGAATGAGTGTTAG





<SEQ ID NO: 20>


SEQ ID NO: 20 shows the nucleotide sequence (GenBank: #DQ402471.1) 





of the light chain (kappa chain) constant region of a rat





antibody (IgG2a).





GCCGCACCAACTGTATCCATCTTCCCACCATCCATGGAACAGTTAACATCTGGAGGTGCCACAGT





CGTGTGCTTCGTGAACAACTTCTATCCCAGAGACATCAGTGTCAAGTGGAAGATTGATGGCAGTG





AACAACGAGATGGTGTCCTGGACAGTGTTACTGATCAGGACAGCAAAGACAGCACGTACAGCATG





AGCAGCACCCTCTCGTTGACCAAGGTTGAATATGAAAGGCATAACCTCTATACCTGTGAGGTTGT





TCATAAGACATCATCCTCACCCGTCGTCAAGAGCTTCAACAGGAATGAGTGTTAG





<SEQ ID NO: 21>


SEQ ID NO: 21 shows the nucleotide sequence (GenBank: #DQ402472.1) 





of the CH of a rat antibody (IgG2a).





CAGCCCCCTCTGTCTATCCACTGGCTCCTGGAACTGCTCTCAAAAGTAACTCCATGGTGACCCTG





GGATGCCTGGTCAAGGGCTATTTCCCTGAGCCAGTCACCGTGACCTGGAACTCTGGAGCCCTGTC





CAGCGGTGTGCACACCTTCCCAGCTGTCCTGCAGTCTGGACTCTACACTCTCACCAGCTCAGTGA





CTGTACCCTCCAGCACCTGGTCCAGCCAGGCCGTCACCTGCAACGTAGCCCACCCGGCCAGCAGC





ACCAAGGTGGACAAGAAAATTGTGCCAAGGGAATGCAATCCTTGTGGATGTACAGGCTCAGAAGT





ATCATCTGTCTTCATCTTCCCCCCAAAGACCAAAGATGTGCTCACCATCACTCTGACTCCTAAGG





TCACGTGTGTTGTGGTAGACATTAGCCAGAATGATCCCGAGGTCCGGTTCAGCTGGTTTATAGAT





GACGTGGAAGTCCACACAGCTCAGACTCATGCCCCGGAGAAGCAGTCCAACAGCACTTTACGCTC





AGTCAGTGAACTCCCCATCGTGCACCGGGACTGGCTCAATGGCAAGACGTTCAAATGCAAAGTCA





ACAGTGGAGCATTCCCTGCCCCCATCGAGAAAAGCATCTCCAAACCCGAAGGCACACCACGAGGT





CCACAGGTATACACCATGGCGCCTCCCAAGGAAGAGATGACCCAGAGTCAAGTCAGTATCACCTG





CATGGTAAAAGGCTTCTATCCCCCAGACATTTATACGGAGTGGAAGATGAACGGGCAGCCACAGG





AAAACTACAAGAACACTCCACCTACGATGGACACAGATGGGAGTTACTTCCTCTACAGCAAGCTC





AATGTAAAGAAAGAAACATGGCAGCAGGGAAACACTTTCACGTGTTCTGTGCTGCATGAGGGCCT





GCACAACCACCATACTGAGAAGAGTCTCTCCCACTCTCCTGGTAAATGA










<SEQ ID NOS: 22 to 27>


SEQ ID NOS: 22 to 27 show the nucleotide sequences of primers cPD-L1 inner F, cPD-L1 inner R, cPD-L1 5′GSP, cPD-L1 3′GSP, cPD-L1-EGFP F and cPD-L1-EGFP R in this order.


<SEQ ID NO: 28>


SEQ ID NO: 28 shows the amino acid sequence of the light chain (kappa chain) constant region of a human antibody.


<SEQ ID NO: 29>


SEQ ID NO: 29 shows the nucleotide sequence of the light chain (kappa chain) constant region of a human antibody.


<SEQ ID NO: 30>


SEQ ID NO: 30 shows the amino acid sequence of the CH (CH1-CH3) of a human antibody (IgG4 variant 1).


<SEQ ID NO: 31>


SEQ ID NO: 31 shows the nucleotide sequence of the CH (CH1-CH3) of a human antibody (IgG4 variant 1).


<SEQ ID NO: 32>


SEQ ID NO: 32 shows the amino acid sequence of the CH (CH1-CH3) of a human antibody (IgG4 variant 2).


<SEQ ID NO: 33>


SEQ ID NO: 33 shows the nucleotide sequence of the CH (CH1-CH3) of a human antibody (IgG4 variant 2).


<SEQ ID NO: 34>


SEQ ID NO: 34 shows the amino acid sequence of the CH (CH1-CH3) of a human antibody (IgG4 variant 3).


<SEQ ID NO: 35>


SEQ ID NO: 35 shows the nucleotide sequence of the CH (CH1-CH3) of a human antibody (IgG4 variant 3).


<SEQ ID NO: 36>


SEQ ID NO: 36 shows the amino acid sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 37>


SEQ ID NO: 37 shows the nucleotide sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 38>


SEQ ID NO: 38 shows the amino acid sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 39>


SEQ ID NO: 39 shows the nucleotide sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 40>


SEQ ID NO: 40 shows the amino acid sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 41>


SEQ ID NO: 41 shows the nucleotide sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 42>


SEQ ID NO: 42 shows the amino acid sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 43>


SEQ ID NO: 43 shows the nucleotide sequence of the light chain (kappa chain) constant region of a mouse antibody.


<SEQ ID NO: 44>


SEQ ID NO: 44 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG1 variant 1).


<SEQ ID NO: 45>


SEQ ID NO: 45 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG1 variant 1).


<SEQ ID NO: 46>


SEQ ID NO: 46 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG1 variant 2).


<SEQ ID NO: 47>


SEQ ID NO: 47 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG1 variant 2).


<SEQ ID NO: 48>


SEQ ID NO: 48 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG2a variant 1).


<SEQ ID NO: 49>


SEQ ID NO: 49 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG2a variant 1).


<SEQ ID NO: 50>


SEQ ID NO: 50 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG2a variant 2).


<SEQ ID NO: 51>


SEQ ID NO: 51 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG2a variant 2).


<SEQ ID NO: 52>


SEQ ID NO: 52 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG2b variant 1).


<SEQ ID NO: 53>


SEQ ID NO: 53 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG2b variant 1).


<SEQ ID NO: 54>


SEQ ID NO: 54 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG2b variant 2).


<SEQ ID NO: 55>


SEQ ID NO: 55 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG2b variant 2).


<SEQ ID NO: 56>


SEQ ID NO: 56 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG2c variant 1).


<SEQ ID NO: 57>


SEQ ID NO: 57 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG2c variant 1).


<SEQ ID NO: 58>


SEQ ID NO: 58 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG2c variant 2).


<SEQ ID NO: 59>


SEQ ID NO: 59 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG2c variant 2).


<SEQ ID NO: 60>


SEQ ID NO: 60 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG2c % variant 3).


<SEQ ID NO: 61>


SEQ ID NO: 61 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG2c variant 3).


<SEQ ID NO: 62>


SEQ ID NO: 62 shows the amino acid sequence of the CH (CH1-CH3) of a mouse antibody (IgG3).


<SEQ ID NO: 63>


SEQ ID NO: 63 shows the nucleotide sequence of the CH (CH1-CH3) of a mouse antibody (IgG3).


<SEQ ID NO: 64>


SEQ ID NO: 64 shows the amino acid sequence of the light chain (lambda chain) constant region of a bovine antibody.


<SEQ ID NO: 65>


SEQ ID NO: 65 shows the nucleotide sequence of the light chain (lambda chain) constant region of a bovine antibody.


<SEQ ID NO: 66>


SEQ ID NO: 66 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG1 variant 1).


<SEQ ID NO: 67>


SEQ ID NO: 67 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG1 variant 1).


<SEQ ID NO: 68>


SEQ ID NO: 68 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG1 variant 2).


<SEQ ID NO: 69>


SEQ ID NO: 69 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG1 variant 2).


<SEQ ID NO: 70>


SEQ ID NO: 70 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG1 variant 3).


<SEQ ID NO: 71>


SEQ ID NO: 71 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG1 variant 3).


<SEQ ID NO: 72>


SEQ ID NO: 72 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG2 variant 1).


<SEQ ID NO: 73>


SEQ ID NO: 73 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG2 variant 1).


<SEQ ID NO: 74>


SEQ ID NO: 74 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG2 variant 2).


<SEQ ID NO: 75>


SEQ ID NO: 75 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG2 variant 2).


<SEQ ID NO: 76>


SEQ ID NO: 76 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG2 variant 3).


<SEQ ID NO: 77>


SEQ ID NO: 77 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG2 variant 3).


<SEQ ID NO: 78>


SEQ ID NO: 78 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG3 variant 1).


<SEQ ID NO: 79>


SEQ ID NO: 79 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG3 variant 1).


<SEQ ID NO: 80>


SEQ ID NO: 80 shows the amino acid sequence of the CH (CH1-CH3) of a bovine antibody (IgG3 variant 2).


<SEQ ID NO: 81>


SEQ ID NO: 81 shows the nucleotide sequence of the CH (CH1-CH3) of a bovine antibody (IgG3 variant 2).


<SEQ ID NO: 82>


SEQ ID NO: 82 shows the amino acid sequence of the light chain (lambda chain) constant region of a canine antibody.


<SEQ ID NO: 83>


SEQ ID NO: 83 shows the nucleotide sequence of the light chain (lambda chain) constant region of a canine antibody.


<SEQ ID NO: 84>


SEQ ID NO: 84 shows the amino acid sequence of the CH (CH1-CH3) of a canine antibody (IgG-D).


<SEQ ID NO: 85>


SEQ ID NO: 85 shows the nucleotide sequence of the CH (CH1-CH3) of a canine antibody (IgG-D).


<SEQ ID NO: 86>


SEQ ID NO: 86 shows the amino acid sequence of the light chain (kappa chain) constant region of an ovine antibody.


<SEQ ID NO: 87>


SEQ ID NO: 87 shows the nucleotide sequence of the light chain (kappa chain) constant region of an ovine antibody.


<SEQ ID NO: 88>


SEQ ID NO: 88 shows the amino acid sequence of the light chain (lambda chain) constant region of an ovine antibody.


<SEQ ID NO: 89>


SEQ ID NO: 89 shows the nucleotide sequence of the light chain (lambda chain) constant region of an ovine antibody.


<SEQ ID NO: 90>


SEQ ID NO: 90 shows the amino acid sequence of the CH (CH1-CH3) of an ovine antibody (IgG1).


<SEQ ID NO: 91>


SEQ ID NO: 91 shows the nucleotide sequence of the CH (CH1-CH3) of an ovine antibody (IgG1).


<SEQ ID NO: 92>


SEQ ID NO: 92 shows the amino acid sequence of the CH (CH1-CH3) of an ovine antibody (IgG2).


<SEQ ID NO: 93>


SEQ ID NO: 93 shows the nucleotide sequence of the CH (CH1-CH3) of an ovine antibody (IgG2).


<SEQ ID NO: 94>


SEQ ID NO: 94 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG1a).


<SEQ ID NO: 95>


SEQ ID NO: 95 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG1a).


<SEQ ID NO: 96>


SEQ ID NO: 96 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG1b).


<SEQ ID NO: 97>


SEQ ID NO: 97 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG1b).


<SEQ ID NO: 98>


SEQ ID NO: 98 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG2a).


<SEQ ID NO: 99>


SEQ ID NO: 99 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG2a).


<SEQ ID NO: 100>


SEQ ID NO: 100 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG2b).


<SEQ ID NO: 101>


SEQ ID NO: 101 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG2b).


<SEQ ID NO: 102>


SEQ ID NO: 102 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG3).


<SEQ ID NO: 103>


SEQ ID NO: 103 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG3).


<SEQ ID NO: 104>


SEQ ID NO: 104 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG4a).


<SEQ ID NO: 105>


SEQ ID NO: 105 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG4a).


<SEQ ID NO: 106>


SEQ ID NO: 106 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG4b).


<SEQ ID NO: 107>


SEQ ID NO: 107 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG4b).


<SEQ ID NO: 108>


SEQ ID NO: 108 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG5a).


<SEQ ID NO: 109>


SEQ ID NO: 109 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG5a).


<SEQ ID NO: 110>


SEQ ID NO: 110 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG5b).


<SEQ ID NO: 111>


SEQ ID NO: 111 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG5b).


<SEQ ID NO: 112>


SEQ ID NO: 112 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG6a).


<SEQ ID NO: 113>


SEQ ID NO: 113 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG6a).


<SEQ ID NO: 114>


SEQ ID NO: 114 shows the amino acid sequence of the CH (CH1-CH3) of a porcine antibody (IgG6b).


<SEQ ID NO: 115>


SEQ ID NO: 115 shows the nucleotide sequence of the CH (CH1-CH3) of a porcine antibody (IgG6b).


<SEQ ID NO: 116>


SEQ ID NO: 116 shows the amino acid sequence of the light chain (estimated to be Ig lambda) constant region (CL) of a water buffalo antibody.


<SEQ ID NO: 117>


SEQ ID NO: 117 shows the nucleotide sequence of the light chain (estimated to be Ig lambda) constant region (CL) of a water buffalo antibody.


<SEQ ID NO: 118>


SEQ ID NO: 118 shows the amino acid sequence of the CH (CH1-CH3) of a water buffalo antibody (estimated to be IgG1).


<SEQ ID NO: 119>


SEQ ID NO: 119 shows the nucleotide sequence of the CH (CH1-CH3) of a water buffalo antibody (estimated to be IgG1).


<SEQ ID NO: 120>


SEQ ID NO: 120 shows the amino acid sequence of the CH (CH1-CH3) of a water buffalo antibody (estimated to be IgG2).


<SEQ ID NO: 121>


SEQ ID NO: 121 shows the nucleotide sequence of the CH (CH1-CH3) of a water buffalo antibody (estimated to be IgG2).


<SEQ ID NO: 122>


SEQ ID NO: 122 shows the amino acid sequence of the CH (CH1-CH3) of a water buffalo antibody (estimated to be IgG3).


<SEQ ID NO: 123>


SEQ ID NO: 123 shows the nucleotide sequence of the CH (CH1-CH3) of a water buffalo antibody (estimated to be IgG3).


<SEQ ID NO: 124>


SEQ ID NO: 124 shows the nucleotide sequence of primer boPD-L1-EGFP F.


<SEQ ID NO: 125>


SEQ ID NO: 125 shows the nucleotide sequence of primer boPD-L1-EGFP R.

Claims
  • 1. An anti-PD-L1 antibody comprising (a) a light chain comprising CDR1 having the amino acid sequence of KSISKY (SEQ ID NO: 1), CDR2 having the amino acid sequence of SGS and CDR3 having the amino acid sequence of QQHNEYPLT (SEQ ID NO: 2) and (b) a heavy chain comprising CDR1 having the amino acid sequence of GYTFTDYI (SEQ ID NO: 3), CDR2 having the amino acid sequence of INPDSGGN (SEQ ID NO: 4) and CDR3 having the amino acid sequence of ARGITMMVVISHWKFDF (SEQ ID NO: 5).
  • 2. The antibody of claim 1, which is from rat.
  • 3. The antibody of claim 2, which is a rat anti-bovine PD-L1 antibody.
  • 4. The antibody of claim 3, wherein the light chain variable region has the amino acid sequence as shown in SEQ ID NO. 6 and the heavy chain variable region has the amino acid sequence as shown in SEQ ID NO: 7.
  • 5. The antibody of claim 1, wherein the light chain constant region has the amino acid sequence of the constant region of kappa chain.
  • 6. The antibody of claim 1, wherein the heavy chain constant region has the amino acid sequence of the constant region of IgG2a.
  • 7. The antibody of claim 5, wherein the light chain constant region has the amino acid sequence as shown in any one of SEQ ID NOS: 8, 10 to 12 and the heavy chain constant region has the amino acid sequence as shown in SEQ ID NO: 9 or 13.
  • 8. The antibody of claim 1 which has a four-chain structure comprising two light chains and two heavy chains.
  • 9. A composition comprising the antibody of claim 1 as an active ingredient and a carrier.
  • 10. A method to diagnose malignant melanoma cancer comprising contacting in vitro one or more cells from a subject with the composition of claim 9; determining if said antibodies in said composition binds to said one or more cells, wherein increased binding to cancer cell as compared to a control is indicative of malignant melanoma cancer.
Priority Claims (1)
Number Date Country Kind
2017-061389 Mar 2017 JP national
PCT Information
Filing Document Filing Date Country Kind
PCT/JP2018/011895 3/23/2018 WO 00
Publishing Document Publishing Date Country Kind
WO2018/181064 10/4/2018 WO A
Foreign Referenced Citations (2)
Number Date Country
WO-2016006241 Jan 2016 WO
WO-2016050721 Apr 2016 WO
Non-Patent Literature Citations (12)
Entry
“International Application Serial No. PCT/JP2018/011895, International Search Report dated Jun. 19, 2018”, w/ English Translation, (Jun. 19, 2018), 6 pgs.
“International Application Serial No. PCT/JP2018/011895, Written Opinion dated Jun. 19, 2018”, (Jun. 19, 2018), 6 pgs.
Ikebuchi, Ryoyo, et al., “Influence of PD-L 1 cross-linking on cell death in PD-L 1-expressing cell lines and bovine lymphocytes”, Immunology 142.4, (2014), 551-561.
Maekawa, Naoya, et al., “Expression of PD-L1 on canine tumor cells and enhancement of IFN-? production from tumor-infiltrating cells by PD-L1 blockade”, PLoS One 9.6, (2014), e98415.
Okagawa, Tomohiro, et al., “Bovine immunoinhibitory receptors contribute to suppression of Mycobacterium avium subsp. paratuberculosis-specific T-cell responses”, Infection and immunity 84.1, (2016), 77-89.
“International Application Serial No. PCT JP2018 011895 International Preliminary Report on Patentability dated Oct. 3, 2019”, 7 pgs.
Koenig, A., “Expression of S100a, vimentin, NSE, and Melan A MART-1 in seven canine melanoma cell lines and twenty-nine retrospective cases of canine melanoma”, Veterinary pathology 38.4, (2001), 427-435.
Ramos-Vara, J.A., “Retrospective study of 338 canine oral melanomas with clinical, histologic, and immunohistochemical review of 129 cases”, Veterinary Pathology 37.6, (2000), 597-608.
Todoroff, R. J., “Oral and pharyngeal neoplasia in the dog: a retrospective survey of 361 cases”, Journal of the American Veterinary Medical Association 175.6, (1979), 567-571.
Koenig, A., et al., “Expression of S100a, vimentin, NSE, and Melan A/MART-1 in seven canine melanoma cell lines and twenty-nine retrospective cases of canine melanoma”, Veterinary pathology 38.4, (2001), 427-435.
Ramos-Vara, J.A., et al., “Retrospective study of 338 canine oral melanomas with clinical, histologic, and immunohistochemical review of 129 cases”, Veterinary Pathology 37.6, (2000), 597-608.
Todoroff, R. J., et al., “Oral and pharyngeal neoplasia in the dog: a retrospective survey of 361 cases”, Journal of the American Veterinary Medical Association 175.6, (1979), 567-571.
Related Publications (1)
Number Date Country
20200031932 A1 Jan 2020 US