Intratumoral accumulation of gut microbiota facilitates CD47-based immunotherapy via STING signaling

肠道微生物群的肿瘤内积累通过 STING 信号促进基于 CD47 的免疫治疗

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作者:Yaoyao Shi, Wenxin Zheng, Kaiting Yang, Katharine G Harris, Kaiyuan Ni, Lai Xue, Wenbin Lin, Eugene B Chang, Ralph R Weichselbaum, Yang-Xin Fu

Abstract

Most studies focus on how intestinal microbiota influence cancer immunotherapy through activating gut immunity. However, immunotherapies related to innate responses such as CD47 blockade rely on the rapid immune responses within the tumor microenvironment. Using one defined anaerobic gut microbiota to track whether microbiota interact with host immunity, we observed that Bifidobacterium facilitates local anti-CD47 immunotherapy on tumor tissues through the capacity to accumulate within the tumor microenvironment. Systemic administration of Bifidobacterium leads to its accumulation within the tumor and converts the nonresponder mice into responders to anti-CD47 immunotherapy in a stimulator of interferon genes (STING)- and interferon-dependent fashion. Local delivery of Bifidobacterium potently stimulates STING signaling and increases cross-priming of dendritic cells after anti-CD47 treatment. Our study identifies the mechanism by which gut microbiota preferentially colonize in tumor sites and facilitate immunotherapy via STING signaling.

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