| Literature DB >> 31423932 |
Jonathan Chee1,2, Chelsea Wilson1, Anthony Buzzai1, Ben Wylie1, Catherine A Forbes2, Mitchell Booth1, Nicola Principe2, Bree Foley1, Mark N Cruickshank1, Jason Waithman1.
Abstract
Activation of naïve CD8+ T cells stimulates proliferation and differentiation into cytotoxic T-lymphocytes (CTLs). Adoptive T Cell Therapy (ACT) involves multiple rounds of ex vivo activation to generate enough CTLs for reinfusion into patients, but this drives differentiation into terminal effector T cells. Less differentiated CTL populations, such as stem cell memory T cells, are more ideal candidates for ACT because of increased self-renewal and persistent properties. Ex vivo targeting of T cell differentiation with epigenetic modifiers is a potential strategy to improve cytotoxic T-lymphocyte (CTL) generation for ACT. We established a pipeline to assess the effects of epigenetic modifiers on CD8+ T cell proliferation, differentiation, and efficacy in a preclinical melanoma model. Single treatment with epigenetic modifiers inhibited T cell proliferation in vitro, producing CD44hiCD62Lhi effector-like T cells rather than a stem cell memory T cell phenotype. Most epigenetic modifying agents had no significant effect on ACT efficacy with the notable exception of the bromodomain and extraterminal (BET)-inhibitor JQ1 which was associated with a decrease in efficacy compared to unmodified T cells. These findings reveal the complexity of epigenetic targeting of T cell differentiation, highlighting the need to precisely define the epigenetic targeting strategies to improve CTL generation for ACT.Entities:
Keywords: BET inhibition; Cancer immunotherapy; T cell differentiation; adoptive cell therapy; cytotoxic T lymphocytes; melanoma
Mesh:
Substances:
Year: 2019 PMID: 31423932 PMCID: PMC6961692 DOI: 10.1080/15592294.2019.1656156
Source DB: PubMed Journal: Epigenetics ISSN: 1559-2294 Impact factor: 4.528