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T-Cells Expressing a Highly Potent PRAME-Specific T-Cell Receptor in Combination with a Chimeric PD1-41BB Co-Stimulatory Receptor Show a Favorable Preclinical Safety Profile and Strong Anti-Tumor Reactivity.
Sailer, Nadja; Fetzer, Ina; Salvermoser, Melanie; Braun, Monika; Brechtefeld, Doris; Krendl, Christian; Geiger, Christiane; Mutze, Kathrin; Noessner, Elfriede; Schendel, Dolores J; Bürdek, Maja; Wilde, Susanne; Sommermeyer, Daniel.
Afiliación
  • Sailer N; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Fetzer I; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Salvermoser M; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Braun M; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Brechtefeld D; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Krendl C; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Geiger C; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Mutze K; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Noessner E; Immunoanalytics-Research Group Tissue Control of Immunocytes (TCI), Helmholtz Zentrum München, 81377 Munich, Germany.
  • Schendel DJ; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Bürdek M; Medigene AG, 82152 Planegg, Germany.
  • Wilde S; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
  • Sommermeyer D; Medigene Immunotherapies GmbH, 82152 Planegg, Germany.
Cancers (Basel) ; 14(8)2022 Apr 14.
Article en En | MEDLINE | ID: mdl-35454906
The hostile tumor microenvironment (TME) is a major challenge for the treatment of solid tumors with T-cell receptor (TCR)-modified T-cells (TCR-Ts), as it negatively influences T-cell efficacy, fitness, and persistence. These negative influences are caused, among others, by the inhibitory checkpoint PD-1/PD-L1 axis. The Preferentially Expressed Antigen in Melanoma (PRAME) is a highly relevant cancer/testis antigen for TCR-T immunotherapy due to broad expression in multiple solid cancer indications. A TCR with high specificity and sensitivity for PRAME was isolated from non-tolerized T-cell repertoires and introduced into T-cells alongside a chimeric PD1-41BB receptor, consisting of the natural extracellular domain of PD-1 and the intracellular signaling domain of 4-1BB, turning an inhibitory pathway into a T-cell co-stimulatory pathway. The addition of PD1-41BB to CD8+ T-cells expressing the transgenic PRAME-TCR enhanced IFN-γ secretion, improved cytotoxic capacity, and prevented exhaustion upon repetitive re-challenge with tumor cells in vitro without altering the in vitro safety profile. Furthermore, a single dose of TCR-Ts co-expressing PD1-41BB was sufficient to clear a hard-to-treat melanoma xenograft in a mouse model, whereas TCR-Ts without PD1-41BB could not eradicate the PD-L1-positive tumors. This cutting-edge strategy supports development efforts to provide more effective TCR-T immunotherapies for the treatment of solid tumors.
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Texto completo: 1 Bases de datos: MEDLINE Idioma: En Revista: Cancers (Basel) Año: 2022 Tipo del documento: Article País de afiliación: Alemania

Texto completo: 1 Bases de datos: MEDLINE Idioma: En Revista: Cancers (Basel) Año: 2022 Tipo del documento: Article País de afiliación: Alemania