High-throughput identification of antigen-specific TCRs by TCR gene capture | Zendy

Carsten Linnemann | Zendy; Bianca Heemskerk | Zendy; Pia Kvistborg | Zendy; Roelof J.C. Kluin | Zendy; Dmitriy A. Bolotin | Zendy; Xiaojing Chen | Zendy; Kaspar Bresser | Zendy; Marja Nieuwland | Zendy; Remko Schotte | Zendy; Samira Michels | Zendy; Raquel Gomez-Eerland | Zendy; Lorenz Jahn | Zendy; Pleun Hombrink | Zendy; Nicolas Legrand | Zendy; Chengyi J. Shu | Zendy; Ilgar Z. Mamedov | Zendy; Arno Velds | Zendy; Christian U. Blank | Zendy; John B.A.G. Haanen | Zendy; Maria A. Turchaninova | Zendy; Ron Kerkhoven | Zendy; Hergen Spits | Zendy; Sine Reker Hadrup | Zendy; Mirjam H.M. Heemskerk | Zendy; Thomas Blankenstein | Zendy; Dmitriy M. Chudakov | Zendy; Gavin Bendle | Zendy; Ton N. Schumacher | Zendy

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High-throughput identification of antigen-specific TCRs by TCR gene capture

Author(s) -

Carsten Linnemann,

Bianca Heemskerk,

Pia Kvistborg,

Roelof J.C. Kluin,

Dmitriy A. Bolotin,

Xiaojing Chen,

Kaspar Bresser,

Marja Nieuwland,

Remko Schotte,

Samira Michels,

Raquel Gomez-Eerland,

Lorenz Jahn,

Pleun Hombrink,

Nicolas Legrand,

Chengyi J. Shu,

Ilgar Z. Mamedov,

Arno Velds,

Christian U. Blank,

John B.A.G. Haanen,

Maria A. Turchaninova,

Ron Kerkhoven,

Hergen Spits,

Sine Reker Hadrup,

Mirjam H.M. Heemskerk,

Thomas Blankenstein,

Dmitriy M. Chudakov,

Gavin Bendle,

Ton N. Schumacher

Publication year - 2013

Publication title -

nature medicine

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 19.536

H-Index - 547

eISSN - 1546-170X

pISSN - 1078-8956

DOI - 10.1038/nm.3359

Subject(s) - t cell receptor , identification (biology) , gene , computational biology , antigen , throughput , biology , genetics , computer science , t cell , immune system , telecommunications , botany , wireless

The transfer of T cell receptor (TCR) genes into patient T cells is a promising approach for the treatment of both viral infections and cancer. Although efficient methods exist to identify antibodies for the treatment of these diseases, comparable strategies to identify TCRs have been lacking. We have developed a high-throughput DNA-based strategy to identify TCR sequences by the capture and sequencing of genomic DNA fragments encoding the TCR genes. We establish the value of this approach by assembling a large library of cancer germline tumor antigen-reactive TCRs. Furthermore, by exploiting the quantitative nature of TCR gene capture, we show the feasibility of identifying antigen-specific TCRs in oligoclonal T cell populations from either human material or TCR-humanized mice. Finally, we demonstrate the ability to identify tumor-reactive TCRs within intratumoral T cell subsets without knowledge of antigen specificities, which may be the first step toward the development of autologous TCR gene therapy to target patient-specific neoantigens in human cancer.

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