Metabolic self-feeding in HBV-associated hepatocarcinoma centered on feedback between circulation lipids and the cellular MAPK/mTOR axis

Ying Zhu; Yingke Zhao; Zhouyu Ning; Yong Deng; Bing Li; Yun Sun; Zhiqiang Meng

doi:10.1186/s12964-024-01619-5

Cell Communication and Signaling (May 2024)

Metabolic self-feeding in HBV-associated hepatocarcinoma centered on feedback between circulation lipids and the cellular MAPK/mTOR axis

Ying Zhu,
Yingke Zhao,
Zhouyu Ning,
Yong Deng,
Bing Li,
Yun Sun,
Zhiqiang Meng

Affiliations

Ying Zhu: Minimally invasive therapy center, Shanghai Cancer Center, Fudan University Shanghai Cancer Center
Yingke Zhao: Minimally invasive therapy center, Shanghai Cancer Center, Fudan University Shanghai Cancer Center
Zhouyu Ning: Minimally invasive therapy center, Shanghai Cancer Center, Fudan University Shanghai Cancer Center
Yong Deng: Department of Research and Development, Department of Nuclear Medicine, Shanghai Proton and Heavy Ion Center, Fudan University Shanghai Cancer Center
Bing Li: Department of Research and Development, Department of Nuclear Medicine, Shanghai Proton and Heavy Ion Center, Fudan University Shanghai Cancer Center
Yun Sun: Department of Research and Development, Department of Nuclear Medicine, Shanghai Proton and Heavy Ion Center, Fudan University Shanghai Cancer Center
Zhiqiang Meng: Minimally invasive therapy center, Shanghai Cancer Center, Fudan University Shanghai Cancer Center

DOI: https://doi.org/10.1186/s12964-024-01619-5
Journal volume & issue: Vol. 22, no. 1
pp. 1 – 17

Abstract

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Abstract Introduction Hepatitis B Virus (HBV) is widely recognized as a “metabolic virus” that disrupts hepatic metabolic homeostasis, rendering it one of the foremost risk factors for hepatocellular carcinoma (HCC). Except for antiviral therapy, the fundamental principles underlying HBV− and HBV+ HCC have remained unchanged, limiting HCC treatment options. Objectives In this study, we aim to identify the distinctive metabolic profile of HBV-associated HCC, with the promise of identifying novel metabolic targets that confer survival advantages and ultimately impede cancer progression. Methods We employed a comprehensive methodology to evaluate metabolic alterations systematically. Initially, we analyzed transcriptomic and proteomic data obtained from a public database, subsequently validating these findings within our test cohort at both the proteomic and transcriptomic levels. Additionally, we conducted a comprehensive analysis of tissue metabolomics profiles, lipidomics, and the activity of the MAPK and AKT signaling pathway to corroborate the abovementioned changes. Results Our multi-omics approach revealed distinct metabolic dysfunctions associated with HBV-associated HCC. Specifically, we observed upregulated steroid hormone biosynthesis, primary bile acid metabolism, and sphingolipid metabolism in HBV-associated HCC patients’ serum. Notably, metabolites involved in primary bile acid and sphingolipids can activate the MAPK/mTOR pathway. Tissue metabolomics and lipidomics analyses further validated the serum metabolic alterations, particularly alterations in lipid composition and accumulation of unsaturated fatty acids. Conclusion Our findings emphasize the pivotal role of HBV in HCC metabolism, elucidating the activation of a unique MAPK/mTOR signaling axis by primary bile acids and sphingolipids. Moreover, the hyperactive MAPK/mTOR signaling axis transduction leads to significant reprogramming in lipid metabolism within HCC cells, further triggering the activation of the MAPK/mTOR pathway in turn, thereby establishing a self-feeding circle driven by primary bile acids and sphingolipids.

Published in Cell Communication and Signaling

ISSN: 1478-811X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General): Cytology
Website: https://biosignaling.biomedcentral.com/

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