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TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets

Adoptive therapy with TCR gene-engineered T cells provides an attractive and feasible treatment option for cancer patients. Further development of TCR gene therapy requires the implementation of T-cell target epitopes that prevent “on-target” reactivity towards healthy tissues and at the same time d...

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Autores principales: Straetemans, Trudy, van Brakel, Mandy, van Steenbergen, Sabine, Broertjes, Marieke, Drexhage, Joost, Hegmans, Joost, Lambrecht, Bart N., Lamers, Cor, Bruggen, Pierre van Der, Coulie, Pierre G., Debets, Reno
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3287115/
https://www.ncbi.nlm.nih.gov/pubmed/22400038
http://dx.doi.org/10.1155/2012/586314
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author Straetemans, Trudy
van Brakel, Mandy
van Steenbergen, Sabine
Broertjes, Marieke
Drexhage, Joost
Hegmans, Joost
Lambrecht, Bart N.
Lamers, Cor
Bruggen, Pierre van Der
Coulie, Pierre G.
Debets, Reno
author_facet Straetemans, Trudy
van Brakel, Mandy
van Steenbergen, Sabine
Broertjes, Marieke
Drexhage, Joost
Hegmans, Joost
Lambrecht, Bart N.
Lamers, Cor
Bruggen, Pierre van Der
Coulie, Pierre G.
Debets, Reno
author_sort Straetemans, Trudy
collection PubMed
description Adoptive therapy with TCR gene-engineered T cells provides an attractive and feasible treatment option for cancer patients. Further development of TCR gene therapy requires the implementation of T-cell target epitopes that prevent “on-target” reactivity towards healthy tissues and at the same time direct a clinically effective response towards tumor tissues. Candidate epitopes that meet these criteria are MAGE-C2(336-344)/HLA-A2 (MC2/A2) and MAGE-A3(243-258)/HLA-DP4 (MA3/DP4). We molecularly characterized TCRαβ genes of an MC2/A2-specific CD8 and MA3/DP4-specific CD4 T-cell clone derived from melanoma patients who responded clinically to MAGE vaccination. We identified MC2/A2 and MA3/DP4-specific TCR-Vα3/Vβ28 and TCR-Vα38/Vβ2 chains and validated these TCRs in vitro upon gene transfer into primary human T cells. The MC2 and MA3 TCR were surface-expressed and mediated CD8 T-cell functions towards melanoma cell lines and CD4 T-cell functions towards dendritic cells, respectively. We intend to start testing these MAGE-specific TCRs in phase I clinical trial.
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spelling pubmed-32871152012-03-07 TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets Straetemans, Trudy van Brakel, Mandy van Steenbergen, Sabine Broertjes, Marieke Drexhage, Joost Hegmans, Joost Lambrecht, Bart N. Lamers, Cor Bruggen, Pierre van Der Coulie, Pierre G. Debets, Reno Clin Dev Immunol Research Article Adoptive therapy with TCR gene-engineered T cells provides an attractive and feasible treatment option for cancer patients. Further development of TCR gene therapy requires the implementation of T-cell target epitopes that prevent “on-target” reactivity towards healthy tissues and at the same time direct a clinically effective response towards tumor tissues. Candidate epitopes that meet these criteria are MAGE-C2(336-344)/HLA-A2 (MC2/A2) and MAGE-A3(243-258)/HLA-DP4 (MA3/DP4). We molecularly characterized TCRαβ genes of an MC2/A2-specific CD8 and MA3/DP4-specific CD4 T-cell clone derived from melanoma patients who responded clinically to MAGE vaccination. We identified MC2/A2 and MA3/DP4-specific TCR-Vα3/Vβ28 and TCR-Vα38/Vβ2 chains and validated these TCRs in vitro upon gene transfer into primary human T cells. The MC2 and MA3 TCR were surface-expressed and mediated CD8 T-cell functions towards melanoma cell lines and CD4 T-cell functions towards dendritic cells, respectively. We intend to start testing these MAGE-specific TCRs in phase I clinical trial. Hindawi Publishing Corporation 2012 2012-02-12 /pmc/articles/PMC3287115/ /pubmed/22400038 http://dx.doi.org/10.1155/2012/586314 Text en Copyright © 2012 Trudy Straetemans et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Straetemans, Trudy
van Brakel, Mandy
van Steenbergen, Sabine
Broertjes, Marieke
Drexhage, Joost
Hegmans, Joost
Lambrecht, Bart N.
Lamers, Cor
Bruggen, Pierre van Der
Coulie, Pierre G.
Debets, Reno
TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets
title TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets
title_full TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets
title_fullStr TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets
title_full_unstemmed TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets
title_short TCR Gene Transfer: MAGE-C2/HLA-A2 and MAGE-A3/HLA-DP4 Epitopes as Melanoma-Specific Immune Targets
title_sort tcr gene transfer: mage-c2/hla-a2 and mage-a3/hla-dp4 epitopes as melanoma-specific immune targets
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3287115/
https://www.ncbi.nlm.nih.gov/pubmed/22400038
http://dx.doi.org/10.1155/2012/586314
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