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BCL6 overexpression in CD4 T cells induces Tfh-like transdifferentiation and enhances antitumor efficiency of CAR-T therapy in pancreatic cancer.

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Biochimica et biophysica acta. Molecular basis of disease 📖 저널 OA 8.2% 2023: 0/1 OA 2024: 0/6 OA 2025: 0/25 OA 2026: 6/40 OA 2023~2026 2024 Vol.1870(7) p. 167346
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Lin X, Dai Z, Tasiheng Y, Zhang R, Wang R, Dong J

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PDAC is a typical "cold tumor" characterized by low immune cell infiltration and a suppressive immune microenvironment.

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APA Lin X, Dai Z, et al. (2024). BCL6 overexpression in CD4 T cells induces Tfh-like transdifferentiation and enhances antitumor efficiency of CAR-T therapy in pancreatic cancer.. Biochimica et biophysica acta. Molecular basis of disease, 1870(7), 167346. https://doi.org/10.1016/j.bbadis.2024.167346
MLA Lin X, et al.. "BCL6 overexpression in CD4 T cells induces Tfh-like transdifferentiation and enhances antitumor efficiency of CAR-T therapy in pancreatic cancer.." Biochimica et biophysica acta. Molecular basis of disease, vol. 1870, no. 7, 2024, pp. 167346.
PMID 38986820 ↗

Abstract

PDAC is a typical "cold tumor" characterized by low immune cell infiltration and a suppressive immune microenvironment. We previously observed the existence of a rare group of follicular helper T cells (Tfh) that could enhance antitumor immune responses by recruiting other immune cells in PDAC. In this study, we ectopically expressed BCL6 in CD4 T cells, and successfully induced Tfh-like transdifferentiation in vitro. This strategy provided abundant Tfh-like cells (iTfhs) that can recruit CD8+ T cells like endogenous Tfhs. Subsequently, Chimeric Antigen Receptors (CARs) against both MSL (Mesothelin) and EPHA2 (Ephrin receptor A2) were used to modify iTfh cells, and the CAR-iTfh cells significantly improved infiltration and antitumor cytotoxicity of co-cultured CD8 T cells. After that, combinatory administration of CAR-iTfh & CAR-CD8 T cell therapy displayed a better effect in repressing the PDAC tumors in xenograft mouse models, compared to conventional CAR-CD4 & CAR-CD8 combinations, and the models received the CAR-iTfh & CAR-CD8 T cells displayed a significantly improved survival rate. Our study revealed the plasticity of T differentiation, expanded the source of Tfh-like cells for cell therapy, and demonstrated a novel and potentially more efficient cellular composition for CAR-T therapy.

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