Intratumoral Microbiota Composition Regulates Chemoimmunotherapy Response in Esophageal Squamous Cell Carcinoma

Hong Wu(University of Electronic Science and Technology of China), Xuefeng Leng(Sichuan Cancer Hospital), Qianshi Liu(University of Electronic Science and Technology of China), Tianqin Mao(Sichuan Cancer Hospital), Tao Jiang(Shanghai Pulmonary Hospital), Yiqiang Liu(University of Electronic Science and Technology of China), Feifei Li(University of Electronic Science and Technology of China), Chenhui Cao(University of Electronic Science and Technology of China), Jun Fan(University of Electronic Science and Technology of China), Liang Chen(University of Science and Technology of China), Yaqi Chen(Huazhong University of Science and Technology Hospital), Quan Yao(Sichuan Cancer Hospital), Shun Lu(Sichuan Cancer Hospital), Renchuan Liang(University of Electronic Science and Technology of China), Lanlin Hu(University of Electronic Science and Technology of China), Mingxin Liu(University of Electronic Science and Technology of China), Yejian Wan(University of Electronic Science and Technology of China), Zhaoshen Li(University of Electronic Science and Technology of China), Jun Peng(Sichuan Cancer Hospital), Qiyu Luo(Sichuan Cancer Hospital), Hang Zhou(Sichuan Cancer Hospital), Jun Yin(Sichuan Cancer Hospital), Ke Xu(Sichuan Cancer Hospital), Mei Lan(Sichuan Cancer Hospital), Xinhao Peng(Sichuan Cancer Hospital), Haitao Lan(Sichuan Academy of Medical Sciences & Sichuan Provincial People's Hospital), Gang Li(University of Electronic Science and Technology of China), Yongtao Han(Sichuan Cancer Hospital), Xia Zhang(Army Medical University), Zhi‐Xiong Jim Xiao(Sichuan University), Jinyi Lang(Sichuan Cancer Hospital), Guihua Wang(Huazhong University of Science and Technology Hospital), Chuan Xu(University of Electronic Science and Technology of China)
Cancer Research
July 11, 2023
Cited by 126Open Access
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Abstract

Neoadjuvant chemoimmunotherapy (NACI) has shown promise in the treatment of resectable esophageal squamous cell carcinoma (ESCC). The microbiomes of patients can impact therapy response, and previous studies have demonstrated that intestinal microbiota influences cancer immunotherapy by activating gut immunity. Here, we investigated the effects of intratumoral microbiota on the response of patients with ESCC to NACI. Intratumoral microbiota signatures of β-diversity were disparate and predicted the treatment efficiency of NACI. The enrichment of Streptococcus positively correlated with GrzB+ and CD8+ T-cell infiltration in tumor tissues. The abundance of Streptococcus could predict prolonged disease-free survival in ESCC. Single-cell RNA sequencing demonstrated that responders displayed a higher proportion of CD8+ effector memory T cells but a lower proportion of CD4+ regulatory T cells. Mice that underwent fecal microbial transplantation or intestinal colonization with Streptococcus from responders showed enrichment of Streptococcus in tumor tissues, elevated tumor-infiltrating CD8+ T cells, and a favorable response to anti-PD-1 treatment. Collectively, this study suggests that intratumoral Streptococcus signatures could predict NACI response and sheds light on the potential clinical utility of intratumoral microbiota for cancer immunotherapy. SIGNIFICANCE: Analysis of intratumoral microbiota in patients with esophageal cancer identifies a microbiota signature that is associated with chemoimmunotherapy response and reveals that Streptococcus induces a favorable response by stimulating CD8+ T-cell infiltration. See related commentary by Sfanos, p. 2985.


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