The origin of hepatocellular carcinoma depends on metabolic zonation.

Guo J; Liang R; Chung A; Li Z; Li B; Chen E; Li L; Wang J; Hsieh MH; Fang IX; Kroger B; Wang Y; Zhu M; Ren X; Mannino G; Jia Y; Wei Y; Moore S; Siegwart DJ; Chung SS; Wang Z; Sharma T; Komjeti S; Han Y; Gopal P; Xiao G; Wang T; Zhu H

doi:10.1126/science.adv7129

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The origin of hepatocellular carcinoma depends on metabolic zonation.

Science (New York, N.Y.) 2026 Vol.391(6784) p. eadv7129

Guo J, Liang R, Chung A, Li Z, Li B, Chen E, Li L, Wang J, Hsieh MH, Fang IX, Kroger B, Wang Y, Zhu M, Ren X, Mannino G, Jia Y, Wei Y, Moore S, Siegwart DJ, Chung SS, Wang Z, Sharma T, Komjeti S, Han Y, Gopal P, Xiao G, Wang T, Zhu H

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The origin of cancer is poorly understood because premalignant cells are rarely followed in their native environments.

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APA Guo J, Liang R, et al. (2026). The origin of hepatocellular carcinoma depends on metabolic zonation.. Science (New York, N.Y.), 391(6784), eadv7129. https://doi.org/10.1126/science.adv7129

MLA Guo J, et al.. "The origin of hepatocellular carcinoma depends on metabolic zonation.." Science (New York, N.Y.), vol. 391, no. 6784, 2026, pp. eadv7129.

PMID 41196951

DOI 10.1126/science.adv7129

Abstract

The origin of cancer is poorly understood because premalignant cells are rarely followed in their native environments. Although the spatial compartmentalization of metabolic functions is critical for proper liver function, it is unknown whether cancers arise from some zones but not others and whether there are metabolic determinants of cancer risk. Zone-specific, mosaic introduction of (catenin beta 1) and (AT-rich interaction domain 2) mutations, commonly co-mutated genes in hepatocellular carcinoma (HCC), in mouse models showed that position and metabolic context determine clone fates. /-driven cancers were much more likely to arise in zone 3. The zone 3 genes and were required for efficient HCC initiation, in part through inhibition of ferroptosis. In the liver, the zonal determinants of HCC development can reveal metabolic vulnerabilities of cancer.

MeSH Terms

Animals; Humans; Mice; beta Catenin; Carcinoma, Hepatocellular; Ferroptosis; Glutathione Transferase; Liver; Liver Neoplasms; Mutation; Transcription Factors

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