Characterization of the landscape of the intratumoral microbiota reveals that Streptococcus anginosus increases the risk of gastric cancer initiation and progression

Li Yuan(Chinese Academy of Sciences), Li‐Bin Pan(Chinese Academy of Sciences), Yunzhe Wang(Fudan University), J. Zhao(Zhejiang Cancer Hospital), Luo Fang(Chinese Academy of Sciences), Ying Zhou(Chinese Academy of Sciences), Ruihong Xia(Zhejiang Cancer Hospital), Yubo Ma(Zhejiang Cancer Hospital), Zhengchen Jiang(Zhejiang Cancer Hospital), Zhiyuan Xu(Zhejiang Cancer Hospital), Can Hu(Zhejiang Cancer Hospital), Yanan Wang(Fudan University), Shengjie Zhang(Zhejiang Cancer Hospital), Bo Zhang(Chinese Academy of Sciences), Haiying Ding(Chinese Academy of Sciences), Mengxuan Chen(Shimadzu (China)), Haibo Cheng(Nanjing University of Chinese Medicine), Ajay Goel(City of Hope), Zhao Zhang(Shanghai Medical College of Fudan University), Xiangdong Cheng(Zhejiang Cancer Hospital)
Cell Discovery
November 26, 2024
Cited by 42Open Access
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Abstract

Abstract As a critical component of the tumour immune microenvironment (TIME), the resident microbiota promotes tumorigenesis across a variety of cancer types. Here, we integrated multiple types of omics data, including microbiome, transcriptome, and metabolome data, to investigate the functional role of intratumoral bacteria in gastric cancer (GC). The microbiome was used to categorize GC samples into six subtypes, and patients with a high abundance of Streptococcus or Pseudomonas had a markedly worse prognosis. Further assays revealed that Streptococcus anginosus (SA) promoted tumour cell proliferation and metastasis while suppressing the differentiation and infiltration of CD8 + T cells. However, antibiotic treatment significantly suppressed tumorigenesis in SA + mice in vivo. We further demonstrated that the SA arginine pathway increased the abundance of ornithine, which may be a major contributor to reshaping of the TIME. Our findings demonstrated that SA, a novel risk factor, plays significant roles in the initiation and progression of GC, suggesting that SA might be a promising target for the diagnosis and treatment of GC.


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