Lipid accumulation inhibition strategies alleviate Fusobacterium nucleatum-infected colorectal cancer

Zhongkun Zhou; Yuqing Niu; Yunhao Ma; Dekui Zhang; Yiqing Wang; Rui Ji; Jianfang Zhao; Chi Ma; Hongmei Zhu; Yingqian Liu; Lixue Tu; Juan Lu; Baizhuo Zhang; Hua Zhang; Xin Ma; Peng Chen

doi:10.1186/s40168-025-02133-7

Microbiome (Aug 2025)

Lipid accumulation inhibition strategies alleviate Fusobacterium nucleatum-infected colorectal cancer

Zhongkun Zhou,
Yuqing Niu,
Yunhao Ma,
Dekui Zhang,
Yiqing Wang,
Rui Ji,
Jianfang Zhao,
Chi Ma,
Hongmei Zhu,
Yingqian Liu,
Lixue Tu,
Juan Lu,
Baizhuo Zhang,
Hua Zhang,
Xin Ma,
Peng Chen

Affiliations

Zhongkun Zhou: School of Pharmacy, Lanzhou University
Yuqing Niu: School of Pharmacy, Lanzhou University
Yunhao Ma: School of Pharmacy, Lanzhou University
Dekui Zhang: The Second Hospital of Lanzhou University
Yiqing Wang: The First Hospital of Lanzhou University
Rui Ji: The First Hospital of Lanzhou University
Jianfang Zhao: The Third People‘s Hospital of Gansu Province
Chi Ma: The Second Hospital of Lanzhou University
Hongmei Zhu: School of Pharmacy, Lanzhou University
Yingqian Liu: School of Pharmacy, Lanzhou University
Lixue Tu: School of Pharmacy, Lanzhou University
Juan Lu: School of Pharmacy, Lanzhou University
Baizhuo Zhang: School of Pharmacy, Lanzhou University
Hua Zhang: School of Pharmacy, Lanzhou University
Xin Ma: School of Pharmacy, Lanzhou University
Peng Chen: School of Pharmacy, Lanzhou University

DOI: https://doi.org/10.1186/s40168-025-02133-7
Journal volume & issue: Vol. 13, no. 1
pp. 1 – 21

Abstract

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Abstract Background Fusobacterium nucleatum (F. nucleatum) is prevalent in colorectal cancer (CRC), and it can promote proliferation and induce chemoresistance via multiple pathways. The development of treatment strategies for F. nucleatum-infected CRC is of great importance. Methods Shotgun metagenomic and metabolomic analyses of human feces, as well as metabolomic analysis of human blood, were performed to reveal the dysbiosis and metabolic dysregulation in CRC. Furthermore, the effects of Bifidobacterium animalis (B. animalis) on F. nucleatum and CRC were assessed in vitro and in vivo. Using a mouse CRC model, the function of bile salt hydrolase (BSH) in B. animalis was verified through heterologous expression in Escherichia coli (E. coli). Bile acids and drug library screening experiments were performed to inhibit F. nucleatum and tumor proliferation. Results We identified an increase in F. nucleatum, enrichment of lipid metabolites, and depletion of Bifidobacterium in CRC patients. Furthermore, B. animalis inhibited F. nucleatum and CRC cells growth in an acid-dependent manner and reduced F. nucleatum-induced tumor increasement in mice. Mechanistically, F. nucleatum caused lipid accumulation, exacerbated inflammation, and intestinal barrier disruption, whereas B. animalis alleviated these changes, increased the Simpson diversity index, reduced lipid metabolites, and altered secondary bile acid composition in mice. Moreover, E. coli-BSH and ursodeoxycholic acid (UDCA) inhibited F. nucleatum-induced lipid accumulation and FASN/CPT1/NF-κB upregulation. Additionally, they alleviated F. nucleatum-related intestinal tumorigenesis in vivo. Targeting F. nucleatum-infected CRC cells and subcutaneous tumors in mice, penfluridol or the combination of orlistat and 5-FU exhibited superior inhibitory effects compared to 5-FU alone. Conclusions F. nucleatum and lipid metabolites are enriched in CRC patients. Furthermore, BSH-expressing E. coli, UDCA, and penfluridol can alleviate F. nucleatum-induced lipid accumulation and tumor growth in mice. Video Abstract Graphical Abstract

Published in Microbiome

ISSN: 2049-2618 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Microbiology: Microbial ecology
Website: https://microbiomejournal.biomedcentral.com

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