Literature DB >> 21750319

CD3 limits the efficacy of TCR gene therapy in vivo.

Maryam Ahmadi1, Judith W King, Shao-An Xue, Cécile Voisine, Angelika Holler, Graham P Wright, Jonathan Waxman, Emma Morris, Hans J Stauss.   

Abstract

The function of T-cell receptor (TCR) gene modified T cells is dependent on efficient surface expression of the introduced TCR α/β heterodimer. We tested whether endogenous CD3 chains are rate-limiting for TCR expression and antigen-specific T-cell function. We show that co-transfer of CD3 and TCR genes into primary murine T cells enhanced TCR expression and antigen-specific T-cell function in vitro. Peptide titration experiments showed that T cells expressing introduced CD3 and TCR genes recognized lower concentration of antigen than T cells expressing TCR only. In vivo imaging revealed that TCR+CD3 gene modified T cells infiltrated tumors faster and in larger numbers, which resulted in more rapid tumor elimination compared with T cells modified by TCR only. After tumor clearance, TCR+CD3 engineered T cells persisted in larger numbers than TCR-only T cells and mounted a more effective memory response when rechallenged with antigen. The data demonstrate that provision of additional CD3 molecules is an effective strategy to enhance the avidity, anti-tumor activity and functional memory formation of TCR gene modified T cells in vivo.

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Year:  2011        PMID: 21750319     DOI: 10.1182/blood-2011-04-346338

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  48 in total

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Journal:  Cancer Immunol Immunother       Date:  2017-10-20       Impact factor: 6.968

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