| Literature DB >> 32213626 |
Junmei Wang1, Farah Hasan1,2, Amanda C Frey3, Haiyan S Li4, Jungsun Park1, Ke Pan1, Cara Haymaker1, Chantale Bernatchez1, Dean A Lee2,5, Stephanie S Watowich2,4, Cassian Yee6,2,4.
Abstract
Clinical response rates after adoptive cell therapy (ACT) are highly correlated with in vivo persistence of the infused T cells. However, antigen-specific T cells found in tumor sites are often well-differentiated effector cells with limited persistence. Central memory CD8+ T cells, capable of self-renewal, represent desirable ACT products. We report here that exposure to a histone deacetylase inhibitor (HDACi) and IL21 could reprogram differentiated human CD8+ T cells into central memory-like T cells. Dedifferentiation of CD8+ T cells was initiated by increased H3 acetylation and chromatin accessibility at the CD28 promoter region. This led to IL21-mediated pSTAT3 binding to the CD28 region, and subsequent upregulation of surface CD28 and CD62L (markers of central memory T cells). The reprogrammed cells exhibited enhanced proliferation in response to both IL2 and IL15, and a stable memory-associated transcriptional signature (increased Lef1 and Tcf7). Our findings support the application of IL21 and HDACi for the in vitro generation of highly persistent T-cell populations that can augment the efficacy of adoptively transferred T cells. ©2020 American Association for Cancer Research.Entities:
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Year: 2020 PMID: 32213626 PMCID: PMC7269845 DOI: 10.1158/2326-6066.CIR-19-0619
Source DB: PubMed Journal: Cancer Immunol Res ISSN: 2326-6066 Impact factor: 11.151