Clinical Significance of Glycolytic Metabolic Activity in Hepatocellular Carcinoma

Author:

Jung Joann,Park Sowon,Jang Yeonwoo,Lee Sung-Hwan,Jeong Yun Seong,Yim Sun Young,Lee Ju-SeogORCID

Abstract

High metabolic activity is a hallmark of cancers, including hepatocellular carcinoma (HCC). However, the molecular features of HCC with high metabolic activity contributing to clinical outcomes and the therapeutic implications of these characteristics are poorly understood. We aimed to define the features of HCC with high metabolic activity and uncover its association with response to current therapies. By integrating gene expression data from mouse liver tissues and tumor tissues from HCC patients (n = 1038), we uncovered three metabolically distinct HCC subtypes that differ in clinical outcomes and underlying molecular biology. The high metabolic subtype is characterized by poor survival, the strongest stem cell signature, high genomic instability, activation of EPCAM and SALL4, and low potential for benefitting from immunotherapy. Interestingly, immune cell analysis showed that regulatory T cells (Tregs) are highly enriched in high metabolic HCC tumors, suggesting that high metabolic activity of cancer cells may trigger activation or infiltration of Tregs, leading to cancer cells’ evasion of anti-cancer immune cells. In summary, we identified clinically and metabolically distinct subtypes of HCC, potential biomarkers associated with these subtypes, and a potential mechanism of metabolism-mediated immune evasion by HCC cells.

Funder

NIH/NCI

the Duncan Family Institute for Cancer Prevention and Risk Assessment Seed Funding Research Program at MD Anderson Cancer Center

Institutional bridge fund from MD Anderson Cancer Center

Institutional Research Grant from MD Anderson Cancer Center

Korea University Hospital Research

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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