TCR Redirected T Cells for Cancer Treatment: Achievements, Hurdles, and Goals

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2020 Oct 5

PMID 33013822

Citations 52

Authors

Francesco Manfredi

Beatrice Claudia Cianciotti

Alessia Potenza

Elena Tassi

Maddalena Noviello

Andrea Biondi

Fabio Ciceri

Chiara Bonini

Eliana Ruggiero

Affiliations

Soon will be listed here.

Abstract

Adoptive T cell therapy (ACT) is a rapidly evolving therapeutic approach designed to harness T cell specificity and function to fight diseases. Based on the evidence that T lymphocytes can mediate a potent anti-tumor response, initially ACT solely relied on the isolation, expansion, and infusion of tumor-infiltrating or circulating tumor-specific T cells. Although effective in a subset of cases, in the first ACT clinical trials several patients experienced disease progression, in some cases after temporary disease control. This evidence prompted researchers to improve ACT products by taking advantage of the continuously evolving gene engineering field and by improving manufacturing protocols, to enable the generation of effective and long-term persisting tumor-specific T cell products. Despite recent advances, several challenges, including prioritization of antigen targets, identification, and optimization of tumor-specific T cell receptors, in the development of tools enabling T cells to counteract the immunosuppressive tumor microenvironment, still need to be faced. This review aims at summarizing the major achievements, hurdles and possible solutions designed to improve the ACT efficacy and safety profile in the context of liquid and solid tumors.

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