A multi-kinase inhibitor screen identifies inhibitors preserving stem-cell-like chimeric antigen receptor T cells

嵌合抗原受体 癌症研究 干细胞 激酶 细胞生物学 T细胞 生物 分子生物学 免疫学 免疫系统
作者
Feifei Song,Ourania Tsahouridis,Simone Stucchi,Tara Walhart,Sophie Mendell,P. Brian Hardy,Matthew Axtman,Shiva Krishna Reddy Guduru,Thomas S.K. Gilbert,Lee M. Graves,Laura E. Herring,Barbara Savoldo,Xingcong Ma,Mark G. Woodcock,J. Justin Milner,Anastasia Ivanova,Kenneth H. Pearce,Yang Xu,G Dotti
出处
期刊:Nature Immunology [Nature Portfolio]
被引量:1
标识
DOI:10.1038/s41590-024-02042-1
摘要

Chimeric antigen receptor T cells (CAR T cells) with T stem (TSCM) cell-like phenotypic characteristics promote sustained antitumor effects. We performed an unbiased and automated high-throughput screen of a kinase-focused compound set to identify kinase inhibitors (KIs) that preserve human TSCM cell-like CAR T cells. We identified three KIs, UNC10225387B, UNC10225263A and UNC10112761A, that combined in vitro increased the frequency of CD45RA+CCR7+TCF1hi TSCM cell-like CAR T cells from both healthy donors and patients with cancer. KI-treated CAR T cells showed enhanced antitumor effects both in vitro and in vivo in mouse tumor models. The KI cocktail maintains TSCM cell-like phenotype preferentially in CAR T cells originating from naive T cells and causes transcriptomic changes without arresting T cell activation or modulating the chromatin organization. Specific kinases, ITK, ADCK3, MAP3K4 and CDK13, targeted by the KI cocktail in a dose-dependent manner are directly associated with the preservation of TSCM cell-like CAR T cells. Knockdown of these kinases individually or in combination enriches for TSCM cell-like CAR T cells, but only CAR T cells generated in the presence of the KI cocktail show robust expansion and differentiation on stimulation with tumor cells. Overall, transient pharmacological inhibition of strategically targeted kinases maintains stem-like features in CAR T cells and improves their antitumor activity. Dotti and colleagues performed an unbiased, high-throughput screen of kinase inhibitors to identify a three-kinase inhibitor cocktail capable of preserving a stem-cell-like subset in chimeric antigen receptor T cells.
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