Blocking hepatocarcinogenesis by a cytochrome P450 family member with female-preferential expression

• Published in: Gut Vol. 71; no. 11; pp. 2313 - 2324
• Main Authors: Ji, Fubo, Zhang, Jianjuan, Liu, Niya, Gu, Yuanzhuo, Zhang, Yan, Huang, Peipei, Zhang, Nachuan, Lin, Shengda, Pan, Ran, Meng, Zhuoxian, Feng, Xin-Hua, Roessler, Stephanie, Zheng, Xin, Ji, Junfang
• Format: Journal Article
• Language: English
• Published: England BMJ Publishing Group Ltd and British Society of Gastroenterology 01.11.2022; BMJ Publishing Group LTD
• Subjects: Animal models; c-Myc protein; carcinogenesis; Cell cycle; Cell growth; Cytochrome P450; Disease prevention; Enzymatic activity; Females; Gender differences; Genes; Hepatitis B; Hepatocellular carcinoma; Hepatology; Hormones; Liver; Liver cancer; Liver diseases; Lymphocytes; Metabolites; Mortality; Myc protein; Patients; Plasmids; Sex; Sex chromosomes; Transcription activation; Transcriptomes; Tumors; Viruses; Womens health; carcinogenesis; hepatocellular carcinoma; cytochrome P450
• ISSN: 0017-5749; 1468-3288; 1468-3288
• DOI: 10.1136/gutjnl-2021-326050

ObjectsThe incidence of hepatocellular carcinoma (HCC) shows an obvious male dominance in rodents and humans. We aimed to identify the key autosomal liver-specific sex-related genes and investigate their roles in hepatocarcinogenesis.DesignTwo HCC cohorts (n=551) with available transcriptome and metabolome data were used. Class comparisons of omics data and ingenuity pathway analysis were performed to explore sex-related molecules and their associated functions. Functional assays were employed to investigate roles of the key candidates, including cellular assays, molecular assays and multiple orthotopic HCC mouse models.ResultsA global comparison of multiple omics data revealed 861 sex-related molecules in non-tumour liver tissues between female and male HCC patients, which denoted a significant suppression of cancer-related diseases and functions in female liver than male. A member of cytochrome P450 family, CYP39A1, was one of the top liver-specific candidates with significantly higher levels in female vs male liver. In HCC tumours, CYP39A1 expression was dramatically reduced in over 90% HCC patients. Exogenous CYP39A1 significantly blocked tumour formation in both female and male mice and partially reduced the sex disparity of hepatocarcinogenesis. The HCC suppressor role of CYP39A1 did not rely on its known P450 enzyme activity but its C-terminal region, by which CYP39A1 impeded the transcriptional activation activity of c-Myc, leading to a significant inhibition of hepatocarcinogenesis.ConclusionsThe liver-specific CYP39A1 with female-preferential expression was a strong suppressor of HCC development. Strategies to up-regulate CYP39A1 might be promising methods for HCC treatment in both women and men in future.