Disruption of SUV39H1-Mediated H3K9 Methylation Sustains CAR T-cell Function

SUV39H1 介导的 H3K9 甲基化的破坏可维持 CAR-T 细胞功能

阅读：9

作者：Nayan Jain #, Zeguo Zhao #, Richard P Koche, Chenling Antelope, Yosi Gozlan, Antonino Montalbano, David Brocks, Michael Lopez, Anton Dobrin, Yuzhe Shi, Gertrude Gunset, Theodoros Giavridis, Michel Sadelain

期刊：

Cancer Discovery

影响因子：

29.700

时间：

2024

起止号：

2024 Jan 12;14(1):142-157.

doi：

10.1158/2159-8290.CD-22-1319

研究方向：

细胞生物学

细胞类型：

T细胞

Significance

T cells engineered with CD28-based CARs possess robust effector function and antigen sensitivity but are hampered by limited persistence, which may result in tumor relapse. We report an epigenetic strategy involving disruption of the SUV39H1-mediated histone-silencing program that promotes the functional persistence of CD28-based CAR T cells. See related article by López-Cobo et al., p. 120. This article is featured in Selected Articles from This Issue, p. 5.

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