Epitope Mapping Using the X-Ray Crystallographic Structure of Complement Receptor Type 2 (CR2)/CD21: Identification of a Highly Inhibitory Monoclonal Antibody That Directly Recognizes the CR2-C3d Interface
Complement receptor type 2 (CR2)/CD21 is a B lymphocyte cell membrane C3d/iC3b receptor that plays a central role in the immune response. Human CR2 is also the receptor for the EBV viral membrane glycoprotein gp350/220. Both C3d and gp350/220 bind CR2 within the first two of 15-16 repetitive domains...
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| creator | Guthridge, Joel M Young, Kendra Gipson, Matthew G Sarrias, Maria-Rossa Szakonyi, Gerda Chen, Xiaojiang S Malaspina, Angela Donoghue, Eileen James, Judith A Lambris, John D Moir, Susan A Perkins, Stephen J Holers, V. Michael |
| description | Complement receptor type 2 (CR2)/CD21 is a B lymphocyte cell membrane C3d/iC3b receptor that plays a central role in the immune response. Human CR2 is also the receptor for the EBV viral membrane glycoprotein gp350/220. Both C3d and gp350/220 bind CR2 within the first two of 15-16 repetitive domains that have been designated short consensus/complement repeats. Many mAbs react with human CR2; however, only one currently available mAb is known to block both C3d/iC3b and gp350/220 binding. We have used a recombinant form of human CR2 containing the short consensus/complement repeat 1-2 ligand-binding fragment to immunize Cr2(-/-) mice. Following fusion, we identified and further characterized four new anti-CR2 mAbs that recognize this fragment. Three of these inhibited binding of CR2 to C3d and gp350/220 in different forms. We have determined the relative inhibitory ability of the four mAbs to block ligand binding, and we have used overlapping peptide-based approaches to identify linear epitopes recognized by the inhibitory mAbs. Placement of these epitopes on the recently solved crystal structure of the CR2-C3d complex reveals that each inhibitory mAb recognizes a site either within or adjacent to the CR2-C3d contact site. One new mAb, designated 171, blocks CR2 receptor-ligand interactions with the greatest efficiency and recognizes a portion of the C3d contact site on CR2. Thus, we have created an anti-human CR2 mAb that blocks the C3d ligand by direct contact with its interaction site, and we have provided confirmatory evidence that the C3d binding site seen in its crystal structure exists in solution. |
| doi_str_mv | 10.4049/jimmunol.167.10.5758 |
| format | Article |
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Michael</creator><creatorcontrib>Guthridge, Joel M ; Young, Kendra ; Gipson, Matthew G ; Sarrias, Maria-Rossa ; Szakonyi, Gerda ; Chen, Xiaojiang S ; Malaspina, Angela ; Donoghue, Eileen ; James, Judith A ; Lambris, John D ; Moir, Susan A ; Perkins, Stephen J ; Holers, V. Michael</creatorcontrib><description>Complement receptor type 2 (CR2)/CD21 is a B lymphocyte cell membrane C3d/iC3b receptor that plays a central role in the immune response. Human CR2 is also the receptor for the EBV viral membrane glycoprotein gp350/220. Both C3d and gp350/220 bind CR2 within the first two of 15-16 repetitive domains that have been designated short consensus/complement repeats. Many mAbs react with human CR2; however, only one currently available mAb is known to block both C3d/iC3b and gp350/220 binding. We have used a recombinant form of human CR2 containing the short consensus/complement repeat 1-2 ligand-binding fragment to immunize Cr2(-/-) mice. Following fusion, we identified and further characterized four new anti-CR2 mAbs that recognize this fragment. Three of these inhibited binding of CR2 to C3d and gp350/220 in different forms. We have determined the relative inhibitory ability of the four mAbs to block ligand binding, and we have used overlapping peptide-based approaches to identify linear epitopes recognized by the inhibitory mAbs. Placement of these epitopes on the recently solved crystal structure of the CR2-C3d complex reveals that each inhibitory mAb recognizes a site either within or adjacent to the CR2-C3d contact site. One new mAb, designated 171, blocks CR2 receptor-ligand interactions with the greatest efficiency and recognizes a portion of the C3d contact site on CR2. Thus, we have created an anti-human CR2 mAb that blocks the C3d ligand by direct contact with its interaction site, and we have provided confirmatory evidence that the C3d binding site seen in its crystal structure exists in solution.</description><identifier>ISSN: 0022-1767</identifier><identifier>EISSN: 1550-6606</identifier><identifier>DOI: 10.4049/jimmunol.167.10.5758</identifier><identifier>PMID: 11698449</identifier><language>eng</language><publisher>United States: Am Assoc Immnol</publisher><subject>Animals ; Antibodies, Monoclonal - immunology ; Antigen-Antibody Complex - immunology ; Binding Sites ; Binding, Competitive ; CD21 antigen ; Complement C3b - metabolism ; Complement C3d - immunology ; Complement C3d - metabolism ; complement component C3d ; complement receptor 2 ; Crystallography, X-Ray ; Epitope Mapping ; HIV-1 - immunology ; Humans ; Mice ; Mice, Knockout ; Models, Molecular ; Peptide Fragments - metabolism ; Receptors, Complement 3d - chemistry ; Receptors, Complement 3d - immunology ; Receptors, Complement 3d - metabolism ; T-Lymphocytes - virology ; Viral Matrix Proteins - metabolism</subject><ispartof>The Journal of immunology (1950), 2001-11, Vol.167 (10), p.5758-5766</ispartof><lds50>peer_reviewed</lds50><oa>free_for_read</oa><woscitedreferencessubscribed>false</woscitedreferencessubscribed><citedby>FETCH-LOGICAL-c413t-f3aebc59b1f725d6317ab95197b8d0354ff41e3e4c1edde6139b79f28a8901113</citedby><cites>FETCH-LOGICAL-c413t-f3aebc59b1f725d6317ab95197b8d0354ff41e3e4c1edde6139b79f28a8901113</cites></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,776,780,27901,27902</link.rule.ids><backlink>$$Uhttps://www.ncbi.nlm.nih.gov/pubmed/11698449$$D View this record in MEDLINE/PubMed$$Hfree_for_read</backlink></links><search><creatorcontrib>Guthridge, Joel M</creatorcontrib><creatorcontrib>Young, Kendra</creatorcontrib><creatorcontrib>Gipson, Matthew G</creatorcontrib><creatorcontrib>Sarrias, Maria-Rossa</creatorcontrib><creatorcontrib>Szakonyi, Gerda</creatorcontrib><creatorcontrib>Chen, Xiaojiang S</creatorcontrib><creatorcontrib>Malaspina, Angela</creatorcontrib><creatorcontrib>Donoghue, Eileen</creatorcontrib><creatorcontrib>James, Judith A</creatorcontrib><creatorcontrib>Lambris, John D</creatorcontrib><creatorcontrib>Moir, Susan A</creatorcontrib><creatorcontrib>Perkins, Stephen J</creatorcontrib><creatorcontrib>Holers, V. Michael</creatorcontrib><title>Epitope Mapping Using the X-Ray Crystallographic Structure of Complement Receptor Type 2 (CR2)/CD21: Identification of a Highly Inhibitory Monoclonal Antibody That Directly Recognizes the CR2-C3d Interface</title><title>The Journal of immunology (1950)</title><addtitle>J Immunol</addtitle><description>Complement receptor type 2 (CR2)/CD21 is a B lymphocyte cell membrane C3d/iC3b receptor that plays a central role in the immune response. Human CR2 is also the receptor for the EBV viral membrane glycoprotein gp350/220. Both C3d and gp350/220 bind CR2 within the first two of 15-16 repetitive domains that have been designated short consensus/complement repeats. Many mAbs react with human CR2; however, only one currently available mAb is known to block both C3d/iC3b and gp350/220 binding. We have used a recombinant form of human CR2 containing the short consensus/complement repeat 1-2 ligand-binding fragment to immunize Cr2(-/-) mice. Following fusion, we identified and further characterized four new anti-CR2 mAbs that recognize this fragment. Three of these inhibited binding of CR2 to C3d and gp350/220 in different forms. We have determined the relative inhibitory ability of the four mAbs to block ligand binding, and we have used overlapping peptide-based approaches to identify linear epitopes recognized by the inhibitory mAbs. Placement of these epitopes on the recently solved crystal structure of the CR2-C3d complex reveals that each inhibitory mAb recognizes a site either within or adjacent to the CR2-C3d contact site. One new mAb, designated 171, blocks CR2 receptor-ligand interactions with the greatest efficiency and recognizes a portion of the C3d contact site on CR2. Thus, we have created an anti-human CR2 mAb that blocks the C3d ligand by direct contact with its interaction site, and we have provided confirmatory evidence that the C3d binding site seen in its crystal structure exists in solution.</description><subject>Animals</subject><subject>Antibodies, Monoclonal - immunology</subject><subject>Antigen-Antibody Complex - immunology</subject><subject>Binding Sites</subject><subject>Binding, Competitive</subject><subject>CD21 antigen</subject><subject>Complement C3b - metabolism</subject><subject>Complement C3d - immunology</subject><subject>Complement C3d - metabolism</subject><subject>complement component C3d</subject><subject>complement receptor 2</subject><subject>Crystallography, X-Ray</subject><subject>Epitope Mapping</subject><subject>HIV-1 - immunology</subject><subject>Humans</subject><subject>Mice</subject><subject>Mice, Knockout</subject><subject>Models, Molecular</subject><subject>Peptide Fragments - metabolism</subject><subject>Receptors, Complement 3d - chemistry</subject><subject>Receptors, Complement 3d - immunology</subject><subject>Receptors, Complement 3d - metabolism</subject><subject>T-Lymphocytes - virology</subject><subject>Viral Matrix Proteins - metabolism</subject><issn>0022-1767</issn><issn>1550-6606</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2001</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNqFkcFu1DAURSMEokPhDxDyCpVFprbj2Am7Ki10pFZIw1RiFznOy8RVEgfb0Sj8Y_-pDjMIdmxs6enc-57ujaL3BK8ZZvnlo-77aTDdmnCxDsNUpNmLaEXSFMecY_4yWmFMaUwEF2fRG-ceMcYcU_Y6OiOE5xlj-Sp6uhm1NyOgezmOetijB7e8vgX0I97KGRV2dl52ndlbObZaoe_eTspPFpBpUGH6sYMeBo-2oGD0xqLdHOwouii29NNlcU3JZ7SpA6EbraTXZliEEt3qfdvNaDO0ugon2Bndm8GozgyyQ1cBr0w9o10rPbrWFpQPcNhh9oP-Be73hWFDXCR18PBgG6ngbfSqkZ2Dd6f_PHr4crMrbuO7b183xdVdrBhJfNwkEiqV5hVpBE1rnhAhqzwluaiyGicpaxpGIAGmCNQ1cJLklcgbmsksx4SQ5Dz6ePQdrfk5gfNlr52CrpMDmMmVgtKQtGD_BUlGqOA8DSA7gsoa5yw05Wh1L-1cElwufZd_-i5D38tw6TvIPpz8p6qH-q_oVHAALo5AG-I-hBxL14c2A07Kw-Hwr9czKsO4jQ</recordid><startdate>20011115</startdate><enddate>20011115</enddate><creator>Guthridge, Joel M</creator><creator>Young, Kendra</creator><creator>Gipson, Matthew G</creator><creator>Sarrias, Maria-Rossa</creator><creator>Szakonyi, Gerda</creator><creator>Chen, Xiaojiang S</creator><creator>Malaspina, Angela</creator><creator>Donoghue, Eileen</creator><creator>James, Judith A</creator><creator>Lambris, John D</creator><creator>Moir, Susan A</creator><creator>Perkins, Stephen J</creator><creator>Holers, V. Michael</creator><general>Am Assoc Immnol</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7T5</scope><scope>H94</scope><scope>7X8</scope></search><sort><creationdate>20011115</creationdate><title>Epitope Mapping Using the X-Ray Crystallographic Structure of Complement Receptor Type 2 (CR2)/CD21: Identification of a Highly Inhibitory Monoclonal Antibody That Directly Recognizes the CR2-C3d Interface</title><author>Guthridge, Joel M ; Young, Kendra ; Gipson, Matthew G ; Sarrias, Maria-Rossa ; Szakonyi, Gerda ; Chen, Xiaojiang S ; Malaspina, Angela ; Donoghue, Eileen ; James, Judith A ; Lambris, John D ; Moir, Susan A ; Perkins, Stephen J ; Holers, V. 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Michael</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Epitope Mapping Using the X-Ray Crystallographic Structure of Complement Receptor Type 2 (CR2)/CD21: Identification of a Highly Inhibitory Monoclonal Antibody That Directly Recognizes the CR2-C3d Interface</atitle><jtitle>The Journal of immunology (1950)</jtitle><addtitle>J Immunol</addtitle><date>2001-11-15</date><risdate>2001</risdate><volume>167</volume><issue>10</issue><spage>5758</spage><epage>5766</epage><pages>5758-5766</pages><issn>0022-1767</issn><eissn>1550-6606</eissn><abstract>Complement receptor type 2 (CR2)/CD21 is a B lymphocyte cell membrane C3d/iC3b receptor that plays a central role in the immune response. Human CR2 is also the receptor for the EBV viral membrane glycoprotein gp350/220. Both C3d and gp350/220 bind CR2 within the first two of 15-16 repetitive domains that have been designated short consensus/complement repeats. Many mAbs react with human CR2; however, only one currently available mAb is known to block both C3d/iC3b and gp350/220 binding. We have used a recombinant form of human CR2 containing the short consensus/complement repeat 1-2 ligand-binding fragment to immunize Cr2(-/-) mice. Following fusion, we identified and further characterized four new anti-CR2 mAbs that recognize this fragment. Three of these inhibited binding of CR2 to C3d and gp350/220 in different forms. We have determined the relative inhibitory ability of the four mAbs to block ligand binding, and we have used overlapping peptide-based approaches to identify linear epitopes recognized by the inhibitory mAbs. Placement of these epitopes on the recently solved crystal structure of the CR2-C3d complex reveals that each inhibitory mAb recognizes a site either within or adjacent to the CR2-C3d contact site. One new mAb, designated 171, blocks CR2 receptor-ligand interactions with the greatest efficiency and recognizes a portion of the C3d contact site on CR2. Thus, we have created an anti-human CR2 mAb that blocks the C3d ligand by direct contact with its interaction site, and we have provided confirmatory evidence that the C3d binding site seen in its crystal structure exists in solution.</abstract><cop>United States</cop><pub>Am Assoc Immnol</pub><pmid>11698449</pmid><doi>10.4049/jimmunol.167.10.5758</doi><tpages>9</tpages><oa>free_for_read</oa></addata></record> |
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| identifier | ISSN: 0022-1767 |
| ispartof | The Journal of immunology (1950), 2001-11, Vol.167 (10), p.5758-5766 |
| issn | 0022-1767 1550-6606 |
| language | eng |
| recordid | cdi_proquest_miscellaneous_72260274 |
| source | MEDLINE; EZB-FREE-00999 freely available EZB journals; Alma/SFX Local Collection |
| subjects | Animals Antibodies, Monoclonal - immunology Antigen-Antibody Complex - immunology Binding Sites Binding, Competitive CD21 antigen Complement C3b - metabolism Complement C3d - immunology Complement C3d - metabolism complement component C3d complement receptor 2 Crystallography, X-Ray Epitope Mapping HIV-1 - immunology Humans Mice Mice, Knockout Models, Molecular Peptide Fragments - metabolism Receptors, Complement 3d - chemistry Receptors, Complement 3d - immunology Receptors, Complement 3d - metabolism T-Lymphocytes - virology Viral Matrix Proteins - metabolism |
| title | Epitope Mapping Using the X-Ray Crystallographic Structure of Complement Receptor Type 2 (CR2)/CD21: Identification of a Highly Inhibitory Monoclonal Antibody That Directly Recognizes the CR2-C3d Interface |
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