Incomplete understanding of how hepatosteatosis transitions to fibrotic non-alcoholic steatohepatitis (NASH) has limited therapeutic options. Two molecules that are elevated in hepatocytes in human NASH liver are cholesterol, whose mechanistic link to NASH remains incompletely understood, and TAZ, a transcriptional regulator that promotes fibrosis but whose mechanism of increase in NASH is unknown. We now show that increased hepatocyte cholesterol upregulates TAZ and promotes fibrotic NASH. ASTER-B/C-mediated internalization of plasma membrane cholesterol activates soluble adenylyl cyclase (sAC; ADCY10), triggering a calcium-RhoA-mediated pathway that suppresses β-TrCP/proteasome-mediated TAZ degradation. In mice fed with a cholesterol-rich NASH-inducing diet, hepatocyte-specific silencing of ASTER-B/C, sAC, or RhoA decreased TAZ and ameliorated fibrotic NASH. The cholesterol-TAZ pathway is present in primary human hepatocytes, and associations among liver cholesterol, TAZ, and RhoA in human NASH liver are consistent with the pathway. Thus, hepatocyte cholesterol contributes to fibrotic NASH by increasing TAZ, suggesting new targets for therapeutic intervention.

Cholesterol Stabilizes TAZ in Hepatocytes to Promote Experimental Non-alcoholic Steatohepatitis / X. Wang, B. Cai, X. Yang, O.O. Sonubi, Z. Zheng, R. Ramakrishnan, H. Shi, L. Valenti, U.B. Pajvani, J. Sandhu, R.E. Infante, A. Radhakrishnan, D.F. Covey, K.L. Guan, J. Buck, L.R. Levin, P. Tontonoz, R.F. Schwabe, I. Tabas. - In: CELL METABOLISM. - ISSN 1550-4131. - 31:5(2020 May 05), pp. 969-986. [10.1016/j.cmet.2020.03.010]

Cholesterol Stabilizes TAZ in Hepatocytes to Promote Experimental Non-alcoholic Steatohepatitis

L. Valenti;
2020

Abstract

Incomplete understanding of how hepatosteatosis transitions to fibrotic non-alcoholic steatohepatitis (NASH) has limited therapeutic options. Two molecules that are elevated in hepatocytes in human NASH liver are cholesterol, whose mechanistic link to NASH remains incompletely understood, and TAZ, a transcriptional regulator that promotes fibrosis but whose mechanism of increase in NASH is unknown. We now show that increased hepatocyte cholesterol upregulates TAZ and promotes fibrotic NASH. ASTER-B/C-mediated internalization of plasma membrane cholesterol activates soluble adenylyl cyclase (sAC; ADCY10), triggering a calcium-RhoA-mediated pathway that suppresses β-TrCP/proteasome-mediated TAZ degradation. In mice fed with a cholesterol-rich NASH-inducing diet, hepatocyte-specific silencing of ASTER-B/C, sAC, or RhoA decreased TAZ and ameliorated fibrotic NASH. The cholesterol-TAZ pathway is present in primary human hepatocytes, and associations among liver cholesterol, TAZ, and RhoA in human NASH liver are consistent with the pathway. Thus, hepatocyte cholesterol contributes to fibrotic NASH by increasing TAZ, suggesting new targets for therapeutic intervention.
English
ADCY10; cholesterol; Gramd1/ASTER; Hippo; liver fibrosis; NASH; RhoA; sAC; TAZ; WWTR1
Settore MED/09 - Medicina Interna
Articolo
Esperti anonimi
Pubblicazione scientifica
   Liver Investigation: Testing Marker Utility in Steatohepatitis
   LITMUS
   EUROPEAN COMMISSION
   777377
5-mag-2020
6-apr-2020
Cell Press
31
5
969
986
18
Pubblicato
Periodico con rilevanza internazionale
scopus
Aderisco
info:eu-repo/semantics/article
Cholesterol Stabilizes TAZ in Hepatocytes to Promote Experimental Non-alcoholic Steatohepatitis / X. Wang, B. Cai, X. Yang, O.O. Sonubi, Z. Zheng, R. Ramakrishnan, H. Shi, L. Valenti, U.B. Pajvani, J. Sandhu, R.E. Infante, A. Radhakrishnan, D.F. Covey, K.L. Guan, J. Buck, L.R. Levin, P. Tontonoz, R.F. Schwabe, I. Tabas. - In: CELL METABOLISM. - ISSN 1550-4131. - 31:5(2020 May 05), pp. 969-986. [10.1016/j.cmet.2020.03.010]
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X. Wang, B. Cai, X. Yang, O.O. Sonubi, Z. Zheng, R. Ramakrishnan, H. Shi, L. Valenti, U.B. Pajvani, J. Sandhu, R.E. Infante, A. Radhakrishnan, D.F. Co...espandi
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/778688
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