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Acyl coenzyme A binding protein (ACBP encoded by diazepam binding inhibitor DBI) is involved in non-malignant liver diseases. Here, we show that DBI mRNA and circulating ACBP/DBI levels are increased in patients with hepatocellular carcinoma (HCC). We investigated its role in hepatocarcinogenesis in mice, inhibiting ACBP/DBI by three methods: (1) inducible whole-body or liver-specific knockout of DBI, (2) a point mutation of the ACBP/DBI receptor (GABRG2), and (3) induction of autoantibodies neutralizing ACBP/DBI. ACBP/DBI plays a major pro-carcinogenic role in HCC induced by intrahepatic transplantation of HCC cell lines, transgenic co-expression of the two oncogenes Myc and Ctnnb1, and chronic challenge with a Western-style diet together with either carbon tetrachloride (CCl4) or diethylnitrosamine. ACBP/DBI inhibition normalizes HCC-associated gene expression, reducing oncogenic alterations in cell cycle-, immunomodulatory-, and ferroptosis-regulatory genes. ACBP/DBI inhibition increases HCC responses to PD-1 blockade and sensitizes HCC to the therapeutic induction of ferroptosis. Hence, ACBP/DBI constitutes an actionable target involved in HCC pathogenesis.

Neutralization of acyl coenzyme A binding protein for the experimental prevention and treatment of hepatocellular carcinoma / Li, S., Motiño, O., Lambertucci, F., Pol, J., Chen, H., Pan, L., Durand, S., Rossin, F., Campani, C., Poupel, L., Klein, C., Montégut, L., Pérez-Lanzón, M., Anagnostopoulos, G., Nogueira-Recalde, U., Cerone, A., Aprahamian, F., Dong, Y., Lizarralde-Guerrero, M., Xue, E., et al.. - In: CELL REPORTS MEDICINE. - ISSN 2666-3791. - 6:7(2025). [10.1016/j.xcrm.2025.102232]

Neutralization of acyl coenzyme A binding protein for the experimental prevention and treatment of hepatocellular carcinoma

Maiuri, Maria Chiara
;
2025

Abstract

Acyl coenzyme A binding protein (ACBP encoded by diazepam binding inhibitor DBI) is involved in non-malignant liver diseases. Here, we show that DBI mRNA and circulating ACBP/DBI levels are increased in patients with hepatocellular carcinoma (HCC). We investigated its role in hepatocarcinogenesis in mice, inhibiting ACBP/DBI by three methods: (1) inducible whole-body or liver-specific knockout of DBI, (2) a point mutation of the ACBP/DBI receptor (GABRG2), and (3) induction of autoantibodies neutralizing ACBP/DBI. ACBP/DBI plays a major pro-carcinogenic role in HCC induced by intrahepatic transplantation of HCC cell lines, transgenic co-expression of the two oncogenes Myc and Ctnnb1, and chronic challenge with a Western-style diet together with either carbon tetrachloride (CCl4) or diethylnitrosamine. ACBP/DBI inhibition normalizes HCC-associated gene expression, reducing oncogenic alterations in cell cycle-, immunomodulatory-, and ferroptosis-regulatory genes. ACBP/DBI inhibition increases HCC responses to PD-1 blockade and sensitizes HCC to the therapeutic induction of ferroptosis. Hence, ACBP/DBI constitutes an actionable target involved in HCC pathogenesis.
2025
Neutralization of acyl coenzyme A binding protein for the experimental prevention and treatment of hepatocellular carcinoma / Li, S., Motiño, O., Lambertucci, F., Pol, J., Chen, H., Pan, L., Durand, S., Rossin, F., Campani, C., Poupel, L., Klein, C., Montégut, L., Pérez-Lanzón, M., Anagnostopoulos, G., Nogueira-Recalde, U., Cerone, A., Aprahamian, F., Dong, Y., Lizarralde-Guerrero, M., Xue, E., et al.. - In: CELL REPORTS MEDICINE. - ISSN 2666-3791. - 6:7(2025). [10.1016/j.xcrm.2025.102232]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11588/1045692
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