| Literature DB >> 28422756 |
Kinga Majchrzak1,2,3,4, Michelle H Nelson1,3,4, Jacob S Bowers1,3,4, Stefanie R Bailey1,3,4, Megan M Wyatt1,3,4, John M Wrangle5, Mark P Rubinstein1,3, Juan C Varela5, Zihai Li1, Richard A Himes6,7,8, Sherine Sl Chan7,8, Chrystal M Paulos1,3,4.
Abstract
ICOS costimulation generates Th17 cells with durable memory responses to tumor. Herein, we found that ICOS induces PI3K/p110δ/Akt and Wnt/β-catenin pathways in Th17 cells. Coinhibiting PI3Kδ and β-catenin altered the biological fate of Th17 cells. Th17 cells inhibited of both pathways expressed less RORγt, which, in turn, reduced their ability to secrete IL-17. Unexpectedly, these cells were more effective (than uninhibited cells) at regressing tumor when infused into mice, leading to long-term curative responses. PI3Kδ inhibition expanded precursor Th17 cells with a central memory phenotype that expressed nominal regulatory properties (low FoxP3), while β-catenin inhibition enhanced Th17 multifunctionality in vivo. Remarkably, upon TCR restimulation, RORγt and IL-17 rebounded in Th17 cells treated with PI3Kδ and β-catenin inhibitors. Moreover, these cells regained β-catenin, Tcf7, and Akt expression, licensing them to secrete heightened IL-2, persist, and eradicate solid tumors without help from endogenous NK and CD8 T cells. This finding shines a light on ways to repurpose FDA-approved drugs to augment T cell-based cancer immunotherapies.Entities:
Keywords: Immunology; Oncology
Year: 2017 PMID: 28422756 PMCID: PMC5396523 DOI: 10.1172/jci.insight.90547
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708