| Literature DB >> 33761313 |
Yao He1, Liuhui Fu1, Yiping Li2, Wenyan Wang1, Mingli Gong2, Jing Zhang1, Xin Dong2, Jiaoyan Huang1, Quanbo Wang3, Charles R Mackay4, Yang-Xin Fu5, Yun Chen6, Xiaohuan Guo7.
Abstract
Recent studies in both mice and humans have suggested that gut microbiota could modulate tumor responsiveness to chemo- or immunotherapies. However, the underlying mechanism is not clear yet. Here, we found that gut microbial metabolites, especially butyrate, could promote the efficacy of oxaliplatin by modulating CD8+ T cell function in the tumor microenvironment. Butyrate treatment directly boosted the antitumor cytotoxic CD8+ T cell responses both in vitro and in vivo in an ID2-dependent manner by promoting the IL-12 signaling pathway. In humans, the oxaliplatin responder cancer patients exhibited a higher amount of serum butyrate than did non-responders, which could also increase ID2 expression and function of human CD8+ T cells. Together, our findings suggest that the gut microbial metabolite butyrate could promote antitumor therapeutic efficacy through the ID2-dependent regulation of CD8+ T cell immunity, indicating that gut microbial metabolites could be effective as a part of cancer therapy.Entities:
Keywords: CD8+ T cell; ID2; IL-12; antitumor therapy efficacy; butyrate; gut microbial metabolites
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Year: 2021 PMID: 33761313 DOI: 10.1016/j.cmet.2021.03.002
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287