Integrative analysis reveals associations between oral microbiota dysbiosis and host genetic and epigenetic aberrations in oral cavity squamous cell carcinoma
journal contribution
posted on 2025-10-22, 04:13 authored by Liuyang Cai, Hengyan Zhu, Qianqian Mou, Po Yee Wong, Linlin Lan, Cherrie WK Ng, Pu Lei, Man Kit Cheung, Daijuanru Wang, Eddy WY Wong, Eric LauEric Lau, Zenon WC Yeung, Ronald Lai, Katie Meehan, Sherwood Fung, Kwan Chee A Chan, Vivian WY Lui, Alfred SL Cheng, Jun Yu, Paul KS Chan, Jason YK Chan, Zigui ChenAbstractDysbiosis of the human oral microbiota has been reported to be associated with oral cavity squamous cell carcinoma (OSCC) while the host-microbiota interactions with respect to the potential impact of pathogenic bacteria on host genomic and epigenomic abnormalities remain poorly studied. In this study, the mucosal bacterial community, host genome-wide transcriptome and DNA CpG methylation were simultaneously profiled in tumors and their adjacent normal tissues of OSCC patients. Significant enrichment in the relative abundance of seven bacteria species (Fusobacterium nucleatum, Treponema medium, Peptostreptococcus stomatis, Gemella morbillorum, Catonella morbi, Peptoanaerobacter yurli and Peptococcus simiae) were observed in OSCC tumor microenvironment. These tumor-enriched bacteria formed 254 positive correlations with 206 up-regulated host genes, mainly involving signaling pathways related to cell adhesion, migration and proliferation. Integrative analysis of bacteria-transcriptome and bacteria-methylation correlations identified at least 20 dysregulated host genes with inverted CpG methylation in their promoter regions associated with enrichment of bacterial pathogens, implying a potential of pathogenic bacteria to regulate gene expression, in part, through epigenetic alterations. An in vitro model further confirmed that Fusobacterium nucleatum might contribute to cellular invasion via crosstalk with E-cadherin/β-catenin signaling, TNFα/NF-κB pathway and extracellular matrix remodeling by up-regulating SNAI2 gene, a key transcription factor of epithelial-mesenchymal transition (EMT). Our work using multi-omics approaches explored complex host-microbiota interactions and provided important insights into genetic and functional basis in OSCC tumorigenesis, which may serve as a precursor for hypothesis-driven study to better understand the causational relationship of pathogenic bacteria in this deadly cancer.
Funding
The authors thank the anonymous participants who provided samples for this study. We also thank Novogene (HK) Co., Ltd., China for the assistance with host gene long non-coding RNA sequencing (lncRNA-seq) and human DNA CpG methylation sequencing, and the Core Utilities of Cancer Genomics and Pathobiology (CUCGP) at Department of Anatomical and Cellular Pathology of the Chinese University of Hong Kong for the service of 16S rRNA gene sequencing. This work was partially supported by funding agents from the Stanley Ho Medical Foundation (J.Y.K.C.), the Research Grants Council of the Hong Kong Special Administrative Region, China (project numbers CUHK14108818 to J.Y.K.C. and CUHK14161017 to Z.C.), the Food and Health Bureau, Hong Kong SAR, China (reference no. 19202041 to Z.C.), and the Research Matching Grant (reference no. 8601687 to P.K.S.C.) from the Research Grants Council of the Hong Kong Special Administrative Region, China. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.
Funder: Food and Health Bureau of the Government of the Hong Kong Special Administrative Region | Health and Medical Research Fund (HMRF)
Funder: Stanley Ho Medical Foundation
Funder: Research Grants Council of the Hong Kong Special Administrative Region, China | Grant ID: 19202041
Funder: Food and Health Bureau, Hong Kong SAR, China | Grant ID: 8601687
Funder: Research Matching Grant
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