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Targeting self-antigens through allogeneic TCR gene transfer.

Moniek A de Witte ,
Miriam Coccoris ,
Monika C Wolkers ,
Marly D van den Boom ,
Elly M Mesman ,
Ji-Ying Song ,
Martin van der Valk ,
John B A G Haanen ,
Ton N M Schumacher

Abstract

Adoptive transfer of T-cell receptor (TCR) genes has been proposed as an attractive approach for immunotherapy in cases where the endogenous T-cell repertoire is insufficient. While there are promising data demonstrating the capacity of TCR-modified T cells to react to foreign antigen encounter, the feasibility of targeting tumor-associated self-antigens has not been addressed. Here we demonstrate that T-cell receptor gene transfer allows the induction of defined self-antigen-specific T-cell responses, even when the endogenous T-cell repertoire is nonreactive. Furthermore, we show that adoptive transfer of T-cell receptor genes can be used to induce strong antigen-specific T-cell responsiveness in partially MHC-mismatched hosts without detectable graft versus host disease. These results demonstrate the feasibility of using a collection of "off the shelf" T-cell receptor genes to target defined tumor-associated self-antigens and thereby form a clear incentive to test this immunotherapeutic approach in a clinical setting.

More about this publication

Blood

Volume 108
Issue nr. 3
Pages 870-7
Publication date 01-08-2006

Full text links

Publisher website (DOI) 10.1182/blood-2005-08-009357
Europe PubMed Central 16861342
Pubmed 16861342

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