C‐type lectin‐like receptors in peptide‐specific HLA class I‐restricted cytotoxic T lymphocytes: differential expression and modulation of effector functions in clones sharing identical TCR structure and epitope specificity

C‐type lectin‐like inhibitory receptors are heterodimers consisting of CD94 and NKG2‐A‐B molecules expressed on NK cells and on a subset of activated T lymphocytes. Their inhibitory effects on NK cytotoxicity and on the NK‐like activity of T cell clones have been demonstrated, but no data are curren...

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Veröffentlicht in:	European journal of immunology 1998-04, Vol.28 (4), p.1134-1142
Hauptverfasser:	Noppen, Christoph, Schaefer, Christoph, Zajac, Paul, Schütz, Alexander, Kocher, Thomas, Kloth, Judith, Heberer, Michael, Colonna, Marco, De Libero, Gennaro, Spagnoli, Giulio C.
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Schlagworte:	Amino Acid Sequence Antigens, CD - immunology Base Sequence CD94 Clone Cells Epitopes - immunology Histocompatibility Antigens Class I - biosynthesis Histocompatibility Antigens Class I - immunology Humans Killer cell inhibitory receptor Lectins, C-Type Membrane Glycoproteins - immunology Molecular Sequence Data NK Cell Lectin-Like Receptor Subfamily D NKG2‐A‐B Receptors, Antigen, T-Cell, alpha-beta - immunology T lymphocyte T-Lymphocyte Subsets - immunology T-Lymphocytes, Cytotoxic - immunology
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container_title	European journal of immunology
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creator	Noppen, Christoph Schaefer, Christoph Zajac, Paul Schütz, Alexander Kocher, Thomas Kloth, Judith Heberer, Michael Colonna, Marco De Libero, Gennaro Spagnoli, Giulio C.
description	C‐type lectin‐like inhibitory receptors are heterodimers consisting of CD94 and NKG2‐A‐B molecules expressed on NK cells and on a subset of activated T lymphocytes. Their inhibitory effects on NK cytotoxicity and on the NK‐like activity of T cell clones have been demonstrated, but no data are currently available on antigen‐specific class I‐restricted cytotoxic T lymphocytes (CTL). We have generated a panel of HLA‐A2.1‐restricted CTL clones directed against a nonapeptide derived from a melanoma‐associated antigen, dopachrome tautomerase (TRP‐2). All clones were CD8+ and TCR α β+. About half of them expressed a CD94bright phenotype, whereas the remaining were CD94dim. Only the CD94bright CTL expressed the NKG2‐A‐B gene, consistent with the expression of a C‐type, lectin‐like, inhibitory CD94/NKG2‐A‐B heterodimer. Both CD94bright and CD94dim clones appeared to require similar amounts of synthetic epitope sensitizing target cells. Addition of anti‐CD94 mAb resulted in a significant increase of specific killing by CD94bright, but not by CD94dim clones in the presence of suboptimal concentrations of peptide, whereas, when optimal amounts were used, the mAb did not induce a significant modulation of the cytotoxicity. Antigen‐induced inward [Ca2+]i fluxes were unaffected, but an enhancement of TCR down‐modulation could be observed in the presence of anti‐CD94 mAb at high concentration of antigenic peptide. The analysis of the TCR‐Vβ repertoire of the CTL clones by RT‐PCR and immunofluorescence revealed that all clones regardless of CD94 phenotype shared Vβ22 expression. Most importantly, sequence analysis showed that they all expressed identical Vβ22 TCR rearranged with Jβ2.1 and Cβ2. Taken together, these data indicate that different expression of functionally active lectin‐like inhibitory receptors can be detected in CTL clones sharing identical TCR sequence and peptide specificity.
doi_str_mv	10.1002/(SICI)1521-4141(199804)28:04<1134::AID-IMMU1134>3.0.CO;2-G
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Their inhibitory effects on NK cytotoxicity and on the NK‐like activity of T cell clones have been demonstrated, but no data are currently available on antigen‐specific class I‐restricted cytotoxic T lymphocytes (CTL). We have generated a panel of HLA‐A2.1‐restricted CTL clones directed against a nonapeptide derived from a melanoma‐associated antigen, dopachrome tautomerase (TRP‐2). All clones were CD8+ and TCR α β+. About half of them expressed a CD94bright phenotype, whereas the remaining were CD94dim. Only the CD94bright CTL expressed the NKG2‐A‐B gene, consistent with the expression of a C‐type, lectin‐like, inhibitory CD94/NKG2‐A‐B heterodimer. Both CD94bright and CD94dim clones appeared to require similar amounts of synthetic epitope sensitizing target cells. 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Their inhibitory effects on NK cytotoxicity and on the NK‐like activity of T cell clones have been demonstrated, but no data are currently available on antigen‐specific class I‐restricted cytotoxic T lymphocytes (CTL). We have generated a panel of HLA‐A2.1‐restricted CTL clones directed against a nonapeptide derived from a melanoma‐associated antigen, dopachrome tautomerase (TRP‐2). All clones were CD8+ and TCR α β+. About half of them expressed a CD94bright phenotype, whereas the remaining were CD94dim. Only the CD94bright CTL expressed the NKG2‐A‐B gene, consistent with the expression of a C‐type, lectin‐like, inhibitory CD94/NKG2‐A‐B heterodimer. Both CD94bright and CD94dim clones appeared to require similar amounts of synthetic epitope sensitizing target cells. Addition of anti‐CD94 mAb resulted in a significant increase of specific killing by CD94bright, but not by CD94dim clones in the presence of suboptimal concentrations of peptide, whereas, when optimal amounts were used, the mAb did not induce a significant modulation of the cytotoxicity. Antigen‐induced inward [Ca2+]i fluxes were unaffected, but an enhancement of TCR down‐modulation could be observed in the presence of anti‐CD94 mAb at high concentration of antigenic peptide. The analysis of the TCR‐Vβ repertoire of the CTL clones by RT‐PCR and immunofluorescence revealed that all clones regardless of CD94 phenotype shared Vβ22 expression. Most importantly, sequence analysis showed that they all expressed identical Vβ22 TCR rearranged with Jβ2.1 and Cβ2. Taken together, these data indicate that different expression of functionally active lectin‐like inhibitory receptors can be detected in CTL clones sharing identical TCR sequence and peptide specificity.</description><subject>Amino Acid Sequence</subject><subject>Antigens, CD - immunology</subject><subject>Base Sequence</subject><subject>CD94</subject><subject>Clone Cells</subject><subject>Epitopes - immunology</subject><subject>Histocompatibility Antigens Class I - biosynthesis</subject><subject>Histocompatibility Antigens Class I - immunology</subject><subject>Humans</subject><subject>Killer cell inhibitory receptor</subject><subject>Lectins, C-Type</subject><subject>Membrane Glycoproteins - immunology</subject><subject>Molecular Sequence Data</subject><subject>NK Cell Lectin-Like Receptor Subfamily D</subject><subject>NKG2‐A‐B</subject><subject>Receptors, Antigen, T-Cell, alpha-beta - immunology</subject><subject>T lymphocyte</subject><subject>T-Lymphocyte Subsets - immunology</subject><subject>T-Lymphocytes, Cytotoxic - immunology</subject><issn>0014-2980</issn><issn>1521-4141</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>1998</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNqFUk1v00AQtRColMJPQNoTag8O-2EndqiQgoHUUqpIkF44sFqvZ-mC4zW7a1Hf-An8Ri78DdZNmgtCvdiemTfvjWdeFL0heEIwpi9PP5ZFeUZSSuKEJOSU5HmGkzOazXFyTghL5vNF-TYuLy-vxug1m-BJsX5F4-WD6PjQ9jA6xpgkMQ3Nj6Mnzn3FGOfTND-KjvJ0mrKUHkd_it8_f_mhA9SA9LoNUaO_AbIgofPGOqRb1IVPXUOouQ6kVlqii9UCyUY4h8qQtuC81dJDjeTgjTc3AbJBzbDtrk3IgJujWisFFlqvRYPgpgs9TpsWibZGW1P3jfBjaBSCAJRBG6m-lWPydgjZmBYcctfC6vYLCvMEKhm4NsUHFOR76XsLt3TQaW_CL91Nq_3wNHqkROPg2f59El29f7cpLuLVelkWi1Usk3zcVZoKRUSlckrxtGKiVhWTIqtYktYzzCosc8GAqTrLE5pXRIoqo8lsxlIpaFqxk-jFjrez5nsf1sK32kloGtGC6R2f5RmZsbD8-4BkmpBpOF0AftoBpTXOWVC8s3or7MAJ5qNdOB_twse78_HufGcXTjMenqNBOA924Xd24YxjXqw55ctA_nw_RV9toT5Q7_0R6p939R-6geEf5XuF_6N7yLG_PCPoHg</recordid><startdate>199804</startdate><enddate>199804</enddate><creator>Noppen, Christoph</creator><creator>Schaefer, Christoph</creator><creator>Zajac, Paul</creator><creator>Schütz, Alexander</creator><creator>Kocher, Thomas</creator><creator>Kloth, Judith</creator><creator>Heberer, Michael</creator><creator>Colonna, Marco</creator><creator>De Libero, Gennaro</creator><creator>Spagnoli, Giulio C.</creator><general>WILEY‐VCH Verlag GmbH</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>199804</creationdate><title>C‐type lectin‐like receptors in peptide‐specific HLA class I‐restricted cytotoxic T lymphocytes: differential expression and modulation of effector functions in clones sharing identical TCR structure and epitope specificity</title><author>Noppen, Christoph ; 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Their inhibitory effects on NK cytotoxicity and on the NK‐like activity of T cell clones have been demonstrated, but no data are currently available on antigen‐specific class I‐restricted cytotoxic T lymphocytes (CTL). We have generated a panel of HLA‐A2.1‐restricted CTL clones directed against a nonapeptide derived from a melanoma‐associated antigen, dopachrome tautomerase (TRP‐2). All clones were CD8+ and TCR α β+. About half of them expressed a CD94bright phenotype, whereas the remaining were CD94dim. Only the CD94bright CTL expressed the NKG2‐A‐B gene, consistent with the expression of a C‐type, lectin‐like, inhibitory CD94/NKG2‐A‐B heterodimer. Both CD94bright and CD94dim clones appeared to require similar amounts of synthetic epitope sensitizing target cells. Addition of anti‐CD94 mAb resulted in a significant increase of specific killing by CD94bright, but not by CD94dim clones in the presence of suboptimal concentrations of peptide, whereas, when optimal amounts were used, the mAb did not induce a significant modulation of the cytotoxicity. Antigen‐induced inward [Ca2+]i fluxes were unaffected, but an enhancement of TCR down‐modulation could be observed in the presence of anti‐CD94 mAb at high concentration of antigenic peptide. The analysis of the TCR‐Vβ repertoire of the CTL clones by RT‐PCR and immunofluorescence revealed that all clones regardless of CD94 phenotype shared Vβ22 expression. Most importantly, sequence analysis showed that they all expressed identical Vβ22 TCR rearranged with Jβ2.1 and Cβ2. Taken together, these data indicate that different expression of functionally active lectin‐like inhibitory receptors can be detected in CTL clones sharing identical TCR sequence and peptide specificity.</abstract><cop>Weinheim</cop><pub>WILEY‐VCH Verlag GmbH</pub><pmid>9565352</pmid><doi>10.1002/(SICI)1521-4141(199804)28:04<1134::AID-IMMU1134>3.0.CO;2-G</doi><tpages>9</tpages><oa>free_for_read</oa></addata></record>
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subjects	Amino Acid Sequence Antigens, CD - immunology Base Sequence CD94 Clone Cells Epitopes - immunology Histocompatibility Antigens Class I - biosynthesis Histocompatibility Antigens Class I - immunology Humans Killer cell inhibitory receptor Lectins, C-Type Membrane Glycoproteins - immunology Molecular Sequence Data NK Cell Lectin-Like Receptor Subfamily D NKG2‐A‐B Receptors, Antigen, T-Cell, alpha-beta - immunology T lymphocyte T-Lymphocyte Subsets - immunology T-Lymphocytes, Cytotoxic - immunology
title	C‐type lectin‐like receptors in peptide‐specific HLA class I‐restricted cytotoxic T lymphocytes: differential expression and modulation of effector functions in clones sharing identical TCR structure and epitope specificity
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