Vitamin E Enhances Cancer Immunotherapy by Reinvigorating Dendritic Cells via Targeting Checkpoint SHP1

癌症免疫疗法 癌症研究 免疫疗法 免疫系统 树突状细胞 癌症 医学 免疫学 化学 内科学
作者
Xiangliang Yuan,Yimin Duan,Yi Xiao,Kai Sun,Yutao Qi,Yuan Zhang,Zamal Ahmed,Davide Moiani,Jun Yao,Hongzhong Li,Lin Zhang,Arseniy E. Yuzhalin,Ping Li,Chen‐Yu Zhang,Akosua Badu-Nkansah,Yohei Saito,Xiang-hua Liu,Wen‐Ling Kuo,Haoqiang Ying,Shao‐Cong Sun
出处
期刊:Cancer Discovery [American Association for Cancer Research]
卷期号:12 (7): 1742-1759 被引量:116
标识
DOI:10.1158/2159-8290.cd-21-0900
摘要

Abstract Despite the popular use of dietary supplements during conventional cancer treatments, their impacts on the efficacies of prevalent immunotherapies, including immune-checkpoint therapy (ICT), are unknown. Surprisingly, our analyses of electronic health records revealed that ICT-treated patients with cancer who took vitamin E (VitE) had significantly improved survival. In mouse models, VitE increased ICT antitumor efficacy, which depended on dendritic cells (DC). VitE entered DCs via the SCARB1 receptor and restored tumor-associated DC functionality by directly binding to and inhibiting protein tyrosine phosphatase SHP1, a DC-intrinsic checkpoint. SHP1 inhibition, genetically or by VitE treatment, enhanced tumor antigen cross-presentation by DCs and DC-derived extracellular vesicles (DC-EV), triggering systemic antigen-specific T-cell antitumor immunity. Combining VitE with DC-recruiting cancer vaccines or immunogenic chemotherapies greatly boosted ICT efficacy in animals. Therefore, combining VitE supplement or SHP1-inhibited DCs/DC-EVs with DC-enrichment therapies could substantially augment T-cell antitumor immunity and enhance the efficacy of cancer immunotherapies. Significance: The impacts of nutritional supplements on responses to immunotherapies remain unexplored. Our study revealed that dietary vitamin E binds to and inhibits DC checkpoint SHP1 to increase antigen presentation, prime antitumor T-cell immunity, and enhance immunotherapy efficacy. VitE-treated or SHP1-silenced DCs/DC-EVs could be developed as potent immunotherapies. This article is highlighted in the In This Issue feature, p. 1599
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