Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo

In this study, we generated human MHC Class I-restricted CD4(+) T cells specific for Epstein-Barr virus (EBV) and cytomegalovirus (CMV), two herpesviridae associated with lymphoma, nasopharyngeal carcinoma and medulloblastoma, respectively. Retroviral transfer of virus-specific, HLA-A2-restricted TC...

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Autores principales: Xue, Shao-An, Gao, Liquan, Ahmadi, Maryam, Ghorashian, Sara, Barros, Rafael D, Pospori, Constandina, Holler, Angelika, Wright, Graham, Thomas, Sharyn, Topp, Max, Morris, Emma C, Stauss, Hans J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Landes Bioscience 2013
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3583927/
https://www.ncbi.nlm.nih.gov/pubmed/23483821
http://dx.doi.org/10.4161/onci.22590
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author Xue, Shao-An
Gao, Liquan
Ahmadi, Maryam
Ghorashian, Sara
Barros, Rafael D
Pospori, Constandina
Holler, Angelika
Wright, Graham
Thomas, Sharyn
Topp, Max
Morris, Emma C
Stauss, Hans J.
author_facet Xue, Shao-An
Gao, Liquan
Ahmadi, Maryam
Ghorashian, Sara
Barros, Rafael D
Pospori, Constandina
Holler, Angelika
Wright, Graham
Thomas, Sharyn
Topp, Max
Morris, Emma C
Stauss, Hans J.
author_sort Xue, Shao-An
collection PubMed
description In this study, we generated human MHC Class I-restricted CD4(+) T cells specific for Epstein-Barr virus (EBV) and cytomegalovirus (CMV), two herpesviridae associated with lymphoma, nasopharyngeal carcinoma and medulloblastoma, respectively. Retroviral transfer of virus-specific, HLA-A2-restricted TCR-coding genes generated CD4(+) T cells that recognized HLA-A2/peptide multimers and produced cytokines when stimulated with MHC Class II-deficient cells presenting the relevant viral peptides in the context of HLA-A2. Peptide titration revealed that CD4(+) T cells had a 10-fold lower avidity than CD8(+) T cells expressing the same TCR. The impaired avidity of CD4(+) T cells was corrected by simultaneously transferring TCR- and CD8-coding genes. The CD8 co-receptor did not alter the cytokine signature of CD4(+) T cells, which remained distinct from that of CD8(+) T cells. Using the xenogeneic NOD/SCID mouse model, we demonstrated that human CD4(+) T cells expressing a specific TCR and CD8 can confer efficient protection against the growth of tumors expressing the EBV or CMV antigens recognized by the TCR. In summary, we describe a robust approach for generating therapeutic CD4(+) T cells capable of providing MHC Class I-restricted immunity against MHC Class II-negative tumors in vivo.
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spelling pubmed-35839272013-03-11 Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo Xue, Shao-An Gao, Liquan Ahmadi, Maryam Ghorashian, Sara Barros, Rafael D Pospori, Constandina Holler, Angelika Wright, Graham Thomas, Sharyn Topp, Max Morris, Emma C Stauss, Hans J. Oncoimmunology Research Paper In this study, we generated human MHC Class I-restricted CD4(+) T cells specific for Epstein-Barr virus (EBV) and cytomegalovirus (CMV), two herpesviridae associated with lymphoma, nasopharyngeal carcinoma and medulloblastoma, respectively. Retroviral transfer of virus-specific, HLA-A2-restricted TCR-coding genes generated CD4(+) T cells that recognized HLA-A2/peptide multimers and produced cytokines when stimulated with MHC Class II-deficient cells presenting the relevant viral peptides in the context of HLA-A2. Peptide titration revealed that CD4(+) T cells had a 10-fold lower avidity than CD8(+) T cells expressing the same TCR. The impaired avidity of CD4(+) T cells was corrected by simultaneously transferring TCR- and CD8-coding genes. The CD8 co-receptor did not alter the cytokine signature of CD4(+) T cells, which remained distinct from that of CD8(+) T cells. Using the xenogeneic NOD/SCID mouse model, we demonstrated that human CD4(+) T cells expressing a specific TCR and CD8 can confer efficient protection against the growth of tumors expressing the EBV or CMV antigens recognized by the TCR. In summary, we describe a robust approach for generating therapeutic CD4(+) T cells capable of providing MHC Class I-restricted immunity against MHC Class II-negative tumors in vivo. Landes Bioscience 2013-01-01 /pmc/articles/PMC3583927/ /pubmed/23483821 http://dx.doi.org/10.4161/onci.22590 Text en Copyright © 2013 Landes Bioscience http://creativecommons.org/licenses/by-nc/3.0/ This is an open-access article licensed under a Creative Commons Attribution-NonCommercial 3.0 Unported License. The article may be redistributed, reproduced, and reused for non-commercial purposes, provided the original source is properly cited.
spellingShingle Research Paper
Xue, Shao-An
Gao, Liquan
Ahmadi, Maryam
Ghorashian, Sara
Barros, Rafael D
Pospori, Constandina
Holler, Angelika
Wright, Graham
Thomas, Sharyn
Topp, Max
Morris, Emma C
Stauss, Hans J.
Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo
title Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo
title_full Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo
title_fullStr Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo
title_full_unstemmed Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo
title_short Human MHC Class I-restricted high avidity CD4(+) T cells generated by co-transfer of TCR and CD8 mediate efficient tumor rejection in vivo
title_sort human mhc class i-restricted high avidity cd4(+) t cells generated by co-transfer of tcr and cd8 mediate efficient tumor rejection in vivo
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3583927/
https://www.ncbi.nlm.nih.gov/pubmed/23483821
http://dx.doi.org/10.4161/onci.22590
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