Tissue-resident memory CAR T cells with stem-like characteristics display enhanced efficacy against solid and liquid tumors

具有干细胞样特征的组织驻留记忆 CAR-T 细胞对实体和液体肿瘤表现出增强的疗效

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作者:In-Young Jung, Estela Noguera-Ortega, Robert Bartoszek, Sierra M Collins, Erik Williams, Megan Davis, Julie K Jadlowsky, Gabriela Plesa, Donald L Siegel, Anne Chew, Bruce L Levine, Shelley L Berger, Edmund K Moon, Steven M Albelda, Joseph A Fraietta

Abstract

Chimeric antigen receptor (CAR) T cells demonstrate remarkable success in treating hematological malignancies, but their effectiveness in non-hematopoietic cancers remains limited. This study proposes enhancing CAR T cell function and localization in solid tumors by modifying the epigenome governing tissue-residency adaptation and early memory differentiation. We identify that a key factor in human tissue-resident memory CAR T cell (CAR-TRM) formation is activation in the presence of the pleotropic cytokine, transforming growth factor β (TGF-β), which enforces a core program of both "stemness" and sustained tissue residency by mediating chromatin remodeling and concurrent transcriptional changes. This approach leads to a practical and clinically actionable in vitro production method for engineering peripheral blood T cells into a large number of "stem-like" CAR-TRM cells resistant to tumor-associated dysfunction, possessing an enhanced ability to accumulate in situ and rapidly eliminate cancer cells for more effective immunotherapy.

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