Hepatocyte-specific Suppression of MicroRNA-221-3p Mitigates Liver Fibrosis

Overview

Journal J Hepatol

Publisher Elsevier

Specialty Gastroenterology

Date 2018 Dec 25

PMID 30582979

Citations 20

Authors

Hsin-Chieh Tsay

Qinggong Yuan

Asha Balakrishnan

Marina Kaiser

Selina Mobus

Emilia Kozdrowska

Marwa Farid

Pia-Katharina Tegtmeyer

Katharina Borst

Florian W R Vondran

Ulrich Kalinke

Andreas Kispert

Michael P Manns

Michael Ott

Amar Deep Sharma

Affiliations

Soon will be listed here.

Abstract

Background & Aims: Fibrosis, a cardinal feature of a dysfunctional liver, significantly contributes to the ever-increasing mortality due to end-stage chronic liver diseases. The crosstalk between hepatocytes and hepatic stellate cells (HSCs) plays a key role in the progression of fibrosis. Although ample efforts have been devoted to elucidate the functions of HSCs during liver fibrosis, the regulatory functions of hepatocytes remain elusive.

Methods: Using an unbiased functional microRNA (miRNA) screening, we investigated the ability of hepatocytes to regulate fibrosis by fine-tuning gene expression via miRNA modulation. The in vivo functional analyses were performed by inhibiting miRNA in hepatocytes using adeno-associated virus in carbon-tetrachloride- and 3,5-di-diethoxycarbonyl-1,4-dihydrocollidine-induced liver fibrosis.

Results: Blocking miRNA-221-3p function in hepatocytes during chronic liver injury facilitated recovery of the liver and faster resolution of the deposited extracellular matrix. Furthermore, we demonstrate that reduced secretion of C-C motif chemokine ligand 2, as a result of post-transcriptional regulation of GNAI2 (G protein alpha inhibiting activity polypeptide 2) by miRNA-221-3p, mitigates liver fibrosis.

Conclusions: Collectively, miRNA modulation in hepatocytes, an easy-to-target cell type in the liver, may serve as a potential therapeutic approach for liver fibrosis.

Lay Summary: Liver fibrosis majorly contributes to mortality resulting from various liver diseases. We discovered a small RNA known as miRNA-221-3p, whose downregulation in hepatocytes results in reduced liver fibrosis. Thus, inhibition of miRNA-221-3p may serve as one of the therapeutic approaches for treatment of liver fibrosis.

Citing Articles

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miRNA-221: A Potential Biomarker of Progressive Liver Injury in Chronic Liver Disease (CLD) due to Hepatitis B Virus (HBV) and Nonalcoholic Fatty Liver Disease (NAFLD).

Sutradhar P, Sultana N, Nessa A Int J Hepatol. 2024; 2024:4221368.

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He L, Xu J, Huang P, Bai Y, Chen H, Xu X Int J Mol Sci. 2024; 25(13).

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Prospective therapeutics for intestinal and hepatic fibrosis.

Li X, Yu M, Zhao Q, Yu Y Bioeng Transl Med. 2023; 8(6):e10579.

PMID: 38023697 PMC: 10658571. DOI: 10.1002/btm2.10579.