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From barrier to trigger: leveraging tumor hypoxia for precise control of CAR-T cell activity.

Created on 15 Jul 2026

Authors

Parisa Pedram Rad, Ali Reyhani, Mohammadreza Dashti

Published in

Molecular biology reports. Volume 53. Issue 1. Jul 15, 2026. Epub Jul 15, 2026.

Abstract

CAR-T cell therapy has revolutionized the treatment of hematologic malignancies, yet its translation to solid tumors remains a formidable challenge. A central determinant of this limitation is the hypoxic tumor microenvironment, which imposes profound immunosuppressive pressure on infiltrating CAR-T cells, impairing their persistence, effector function, and metabolic fitness. Rather than viewing hypoxia purely as an obstacle, emerging engineering paradigms are reframing it as a tumor-selective switch one that can be harnessed to spatially confine CAR-T cell activation, enhance metabolic fitness, and reduce off-tumor toxicity. This review critically examines how hypoxia subverts CAR-T cell immunity, and how next-generation hypoxia-responsive constructs, metabolic reprogramming strategies, and armored cytokine-secreting designs are beginning to turn this hostile microenvironment into a therapeutic advantage. We further discuss unresolved clinical challenges and the translational outlook for hypoxia-adapted CAR-T cells in solid tumor immunotherapy.

PMID:
42455334
Bibliographic data and abstract were imported from PubMed on 15 Jul 2026.

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