Comparison of HLA-DR1-restricted T cell response induced in HLA-DR1 transgenic mice deficient for murine MHC class II and HLA-DR1 transgenic mice expressing endogenous murine MHC class II molecules

Transgenic mice expressing human HLA class II molecules provide a useful model for identifying HLA-restricted CD4+ epitopes. However, the influence of endogenous murine H-2-restricted T cell responses on HLA-restricted responses is not known. In the present study, we show that HLA-DR1 transgenic mic...

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Veröffentlicht in:	International immunology 2004-09, Vol.16 (9), p.1275-1282
Hauptverfasser:	Pajot, Anthony, Pancré, Véronique, Fazilleau, Nicolas, Michel, Marie-Louise, Angyalosi, Gerhild, Ojcius, David M., Auriault, Claude, Lemonnier, François A., Lone, Yu-Chun
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Schlagworte:	Animals antigen BC β constant BJ β junction BV β variable CD4-Positive T-Lymphocytes - immunology CDR complementarity determining region CTL cytotoxic T lymphocyte Cytokines - biosynthesis Epitope Mapping Genes, T-Cell Receptor beta H-2 Antigens - physiology HBc hepatitis B virus capsid protein HBs hepatitis B virus surface protein Hepatitis B Core Antigens - immunology Hepatitis B Surface Antigens - immunology Hepatitis B virus HLA-DR1 Antigen - physiology Humans major histocompatibility complex Mice Mice, Transgenic TH helper T lymphocyte transgenic mice vaccine
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container_title	International immunology
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creator	Pajot, Anthony Pancré, Véronique Fazilleau, Nicolas Michel, Marie-Louise Angyalosi, Gerhild Ojcius, David M. Auriault, Claude Lemonnier, François A. Lone, Yu-Chun
description	Transgenic mice expressing human HLA class II molecules provide a useful model for identifying HLA-restricted CD4+ epitopes. However, the influence of endogenous murine H-2-restricted T cell responses on HLA-restricted responses is not known. In the present study, we show that HLA-DR1 transgenic mice deficient for H-2 class II expression (HLA-DR1+/+/IAβ0/0) exhibit an equivalent expression level of the transgene HLA-DR1 and a similar diversity in the TCR repertoire, but a slightly different number of CD4+ peripheral T cells, when compared to HLA-DR1 transgenic mice in which H-2 class II molecules were retained (HLA-DR1+/+/IAβ+/+). More importantly, a strong antigen-specific HLA-DR1-restricted response was observed in nearly all HLA-DR1+/+/IAβ0/0 mice immunized with HBV envelope protein (HBs) or capsid protein (HBc), whereas weak HBs- or HBc-specific HLA-DR1-restricted responses were detected in half of the immunized HLA-DR1+/+/IAβ+/+ mice. Conversely, strong HBs- or HBc-specific H-2-restricted T cell responses were detected in HLA-DR1+/+/IAβ+/+ mice but not in HLA-DR1+/+/IAβ0/0 mice. Our results indicate that the coexpression of endogenous H-2 class II molecules reduces the intensity of HLA-DR1-restricted antigen-specific responses in transgenic mice, by favoring murine over human MHC recognition and education. Thus, HLA-DR1+/+/IAβ0/0 mice represent a better model for identifying and characterizing HLA-DR1-restricted epitopes relevant for human disease.
doi_str_mv	10.1093/intimm/dxh129
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However, the influence of endogenous murine H-2-restricted T cell responses on HLA-restricted responses is not known. In the present study, we show that HLA-DR1 transgenic mice deficient for H-2 class II expression (HLA-DR1+/+/IAβ0/0) exhibit an equivalent expression level of the transgene HLA-DR1 and a similar diversity in the TCR repertoire, but a slightly different number of CD4+ peripheral T cells, when compared to HLA-DR1 transgenic mice in which H-2 class II molecules were retained (HLA-DR1+/+/IAβ+/+). More importantly, a strong antigen-specific HLA-DR1-restricted response was observed in nearly all HLA-DR1+/+/IAβ0/0 mice immunized with HBV envelope protein (HBs) or capsid protein (HBc), whereas weak HBs- or HBc-specific HLA-DR1-restricted responses were detected in half of the immunized HLA-DR1+/+/IAβ+/+ mice. Conversely, strong HBs- or HBc-specific H-2-restricted T cell responses were detected in HLA-DR1+/+/IAβ+/+ mice but not in HLA-DR1+/+/IAβ0/0 mice. Our results indicate that the coexpression of endogenous H-2 class II molecules reduces the intensity of HLA-DR1-restricted antigen-specific responses in transgenic mice, by favoring murine over human MHC recognition and education. 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Immunol</addtitle><description>Transgenic mice expressing human HLA class II molecules provide a useful model for identifying HLA-restricted CD4+ epitopes. However, the influence of endogenous murine H-2-restricted T cell responses on HLA-restricted responses is not known. In the present study, we show that HLA-DR1 transgenic mice deficient for H-2 class II expression (HLA-DR1+/+/IAβ0/0) exhibit an equivalent expression level of the transgene HLA-DR1 and a similar diversity in the TCR repertoire, but a slightly different number of CD4+ peripheral T cells, when compared to HLA-DR1 transgenic mice in which H-2 class II molecules were retained (HLA-DR1+/+/IAβ+/+). More importantly, a strong antigen-specific HLA-DR1-restricted response was observed in nearly all HLA-DR1+/+/IAβ0/0 mice immunized with HBV envelope protein (HBs) or capsid protein (HBc), whereas weak HBs- or HBc-specific HLA-DR1-restricted responses were detected in half of the immunized HLA-DR1+/+/IAβ+/+ mice. Conversely, strong HBs- or HBc-specific H-2-restricted T cell responses were detected in HLA-DR1+/+/IAβ+/+ mice but not in HLA-DR1+/+/IAβ0/0 mice. Our results indicate that the coexpression of endogenous H-2 class II molecules reduces the intensity of HLA-DR1-restricted antigen-specific responses in transgenic mice, by favoring murine over human MHC recognition and education. Thus, HLA-DR1+/+/IAβ0/0 mice represent a better model for identifying and characterizing HLA-DR1-restricted epitopes relevant for human disease.</description><subject>Animals</subject><subject>antigen</subject><subject>BC β constant</subject><subject>BJ β junction</subject><subject>BV β variable</subject><subject>CD4-Positive T-Lymphocytes - immunology</subject><subject>CDR complementarity determining region</subject><subject>CTL cytotoxic T lymphocyte</subject><subject>Cytokines - biosynthesis</subject><subject>Epitope Mapping</subject><subject>Genes, T-Cell Receptor beta</subject><subject>H-2 Antigens - physiology</subject><subject>HBc hepatitis B virus capsid protein</subject><subject>HBs hepatitis B virus surface protein</subject><subject>Hepatitis B Core Antigens - immunology</subject><subject>Hepatitis B Surface Antigens - immunology</subject><subject>Hepatitis B virus</subject><subject>HLA-DR1 Antigen - physiology</subject><subject>Humans</subject><subject>major histocompatibility complex</subject><subject>Mice</subject><subject>Mice, Transgenic</subject><subject>TH helper T lymphocyte</subject><subject>transgenic mice</subject><subject>vaccine</subject><issn>0953-8178</issn><issn>1460-2377</issn><issn>1460-2377</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2004</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNqFkk1v1DAQhi0EokvhyBVZHLiltePEH8dqC91VtwXRFUJcrKwzLi6JHexEWn4g_wuvdqFSBeI00swz74zHL0IvKTmhRLFT50fX96ft9ist1SM0oxUnRcmEeIxmRNWskFTII_QspTtCCCsVe4qOaF1Wqq7oDP2ch35ookvB42DxYnVWnH-kRYQ0RmdGaPEaG-g6nDND8Amw8-1kct753zQeY-PTLXhncO8M4BasMw78iG2IuJ-i84CvFnNsuiYlvFzixrf_7IbtkIcl528x-DbkSpjSX1X60IGZOkjP0RPbdAleHOIxWr97u54vitX7i-X8bFWYqmZjUQpOBdgWSmEqyomEVgkqbWNsxZWlZCPlhnK7kVwJLggllbTKcGnKWlaKHaM3e9khhu9TPpHuXdpdp_GQd9ScCykYZf8FqcjiipQZfP0AvAtT9PkNmqqaUFbXu7HFHjIxpBTB6iG6vok_NCV6ZwK9N4HemyDzrw6i06aH9p4-_Pq9oEsjbP_Um_hNc8FErRefv-ibq4vq8ub6k_7AfgGGgb5v</recordid><startdate>20040901</startdate><enddate>20040901</enddate><creator>Pajot, Anthony</creator><creator>Pancré, Véronique</creator><creator>Fazilleau, Nicolas</creator><creator>Michel, Marie-Louise</creator><creator>Angyalosi, Gerhild</creator><creator>Ojcius, David M.</creator><creator>Auriault, Claude</creator><creator>Lemonnier, François A.</creator><creator>Lone, Yu-Chun</creator><general>Oxford University Press</general><general>Oxford Publishing Limited (England)</general><scope>BSCLL</scope><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>7QL</scope><scope>7QP</scope><scope>7QR</scope><scope>7T5</scope><scope>7T7</scope><scope>7TK</scope><scope>7U9</scope><scope>8FD</scope><scope>C1K</scope><scope>FR3</scope><scope>H94</scope><scope>K9.</scope><scope>M7N</scope><scope>P64</scope><scope>7X8</scope></search><sort><creationdate>20040901</creationdate><title>Comparison of HLA-DR1-restricted T cell response induced in HLA-DR1 transgenic mice deficient for murine MHC class II and HLA-DR1 transgenic mice expressing endogenous murine MHC class II molecules</title><author>Pajot, Anthony ; 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Immunol</addtitle><date>2004-09-01</date><risdate>2004</risdate><volume>16</volume><issue>9</issue><spage>1275</spage><epage>1282</epage><pages>1275-1282</pages><issn>0953-8178</issn><issn>1460-2377</issn><eissn>1460-2377</eissn><abstract>Transgenic mice expressing human HLA class II molecules provide a useful model for identifying HLA-restricted CD4+ epitopes. However, the influence of endogenous murine H-2-restricted T cell responses on HLA-restricted responses is not known. In the present study, we show that HLA-DR1 transgenic mice deficient for H-2 class II expression (HLA-DR1+/+/IAβ0/0) exhibit an equivalent expression level of the transgene HLA-DR1 and a similar diversity in the TCR repertoire, but a slightly different number of CD4+ peripheral T cells, when compared to HLA-DR1 transgenic mice in which H-2 class II molecules were retained (HLA-DR1+/+/IAβ+/+). More importantly, a strong antigen-specific HLA-DR1-restricted response was observed in nearly all HLA-DR1+/+/IAβ0/0 mice immunized with HBV envelope protein (HBs) or capsid protein (HBc), whereas weak HBs- or HBc-specific HLA-DR1-restricted responses were detected in half of the immunized HLA-DR1+/+/IAβ+/+ mice. Conversely, strong HBs- or HBc-specific H-2-restricted T cell responses were detected in HLA-DR1+/+/IAβ+/+ mice but not in HLA-DR1+/+/IAβ0/0 mice. Our results indicate that the coexpression of endogenous H-2 class II molecules reduces the intensity of HLA-DR1-restricted antigen-specific responses in transgenic mice, by favoring murine over human MHC recognition and education. Thus, HLA-DR1+/+/IAβ0/0 mice represent a better model for identifying and characterizing HLA-DR1-restricted epitopes relevant for human disease.</abstract><cop>England</cop><pub>Oxford University Press</pub><pmid>15249541</pmid><doi>10.1093/intimm/dxh129</doi><tpages>8</tpages><oa>free_for_read</oa></addata></record>
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subjects	Animals antigen BC β constant BJ β junction BV β variable CD4-Positive T-Lymphocytes - immunology CDR complementarity determining region CTL cytotoxic T lymphocyte Cytokines - biosynthesis Epitope Mapping Genes, T-Cell Receptor beta H-2 Antigens - physiology HBc hepatitis B virus capsid protein HBs hepatitis B virus surface protein Hepatitis B Core Antigens - immunology Hepatitis B Surface Antigens - immunology Hepatitis B virus HLA-DR1 Antigen - physiology Humans major histocompatibility complex Mice Mice, Transgenic TH helper T lymphocyte transgenic mice vaccine
title	Comparison of HLA-DR1-restricted T cell response induced in HLA-DR1 transgenic mice deficient for murine MHC class II and HLA-DR1 transgenic mice expressing endogenous murine MHC class II molecules
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