Targeting ER protein TXNDC5 in hepatic stellate cell mitigates liver fibrosis by repressing non-canonical TGFβ signalling

Chen-Ting Hung; Tung-Hung Su; Yen-Ting Chen; Yueh-Feng Wu; You-Tzung Chen; Sung-Jan Lin; Shuei-Liong Lin; Kai-Chien Yang

doi:10.1136/gutjnl-2021-325065

Targeting ER protein TXNDC5 in hepatic stellate cell mitigates liver fibrosis by repressing non-canonical TGFβ signalling

Gut. 2022 Sep;71(9):1876-1891. doi: 10.1136/gutjnl-2021-325065. Epub 2021 Dec 21.

Authors

Chen-Ting Hung¹, Tung-Hung Su^{2

3}, Yen-Ting Chen¹, Yueh-Feng Wu⁴, You-Tzung Chen⁵, Sung-Jan Lin^{4

6

7

8}, Shuei-Liong Lin^{3

7

9

10}, Kai-Chien Yang^{11

3

7

12}

Affiliations

¹ Graduate Institute and Department of Pharmacology, National Taiwan University College of Medicine, Taipei, Taiwan.
² Hepatitis Research Center, National Taiwan University Hospital, Taipei, Taiwan.
³ Department of Internal Medicine, National Taiwan University Hospital, Taipei, Taiwan.
⁴ Department of Biomedical Engineering, College of Medicine and College of Engineering, National Taiwan University, Taipei, Taiwan.
⁵ Graduate Institute of Medical Genomics and Proteomics, National Taiwan University College of Medicine, Taipei, Taiwan.
⁶ Department of Dermatology, National Taiwan University Hospital and College of Medicine, Taipei, Taiwan.
⁷ Research Center for Developmental Biology & Regenerative Medicine, National Taiwan University, Taipei, Taiwan.
⁸ Center for Frontier Medicine, National Taiwan University Hospital, Taipei, Taiwan.
⁹ Graduate Institute and Department of Physiology, National Taiwan University College of Medicine, Taipei, Taiwan.
¹⁰ Department of Integrated Diagnostics & Therapeutics, National Taiwan University Hospital, Taipei, Taiwan.
¹¹ Graduate Institute and Department of Pharmacology, National Taiwan University College of Medicine, Taipei, Taiwan kcyang@ntu.edu.tw.
¹² Institute of Biomedical Sciences, Academia Sinica, Taipei, Taiwan.

PMID: 34933915
DOI: 10.1136/gutjnl-2021-325065

Abstract

Background and objectives: Liver fibrosis (LF) occurs following chronic liver injuries. Currently, there is no effective therapy for LF. Recently, we identified thioredoxin domain containing 5 (TXNDC5), an ER protein disulfide isomerase (PDI), as a critical mediator of cardiac and lung fibrosis. We aimed to determine if TXNDC5 also contributes to LF and its potential as a therapeutic target for LF.

Design: Histological and transcriptome analyses on human cirrhotic livers were performed. Col1a1-GFP^Tg , Alb-Cre;Rosa26-tdTomato and Tie2-Cre/ERT2;Rosa26-tdTomato mice were used to determine the cell type(s) where TXNDC5 was induced following liver injury. In vitro investigations were conducted in human hepatic stellate cells (HSCs). Col1a2-Cre/ERT2;Txndc5^fl/fl (Txndc5^cKO ) and Alb-Cre;Txndc5^fl/fl (Txndc5^Hep-cKO ) mice were generated to delete TXNDC5 in HSCs and hepatocytes, respectively. Carbon tetrachloride treatment and bile duct ligation surgery were employed to induce liver injury/fibrosis in mice. The extent of LF was quantified using histological, imaging and biochemical analyses.

Results: TXNDC5 was upregulated markedly in human and mouse fibrotic livers, particularly in activated HSC at the fibrotic foci. TXNDC5 was induced by transforming growth factor β1 (TGFβ1) in HSCs and it was both required and sufficient for the activation, proliferation, survival and extracellular matrix production of HSC. Mechanistically, TGFβ1 induces TXNDC5 expression through increased ER stress and ATF6-mediated transcriptional regulation. In addition, TXNDC5 promotes LF by redox-dependent JNK and signal transducer and activator of transcription 3 activation in HSCs through its PDI activity, activating HSCs and making them resistant to apoptosis. HSC-specific deletion of Txndc5 reverted established LF in mice.

Conclusions: ER protein TXNDC5 promotes LF through redox-dependent HSC activation, proliferation and excessive extracellular matrix production. Targeting TXNDC5, therefore, could be a potential novel therapeutic strategy to ameliorate LF.

Keywords: apoptosis; fibrogenesis; gene targeting; hepatic stellate cell; liver cirrhosis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Carbon Tetrachloride / adverse effects
Carbon Tetrachloride / metabolism
Fibrosis
Hepatic Stellate Cells* / metabolism
Hepatocytes / metabolism
Humans
Liver / metabolism
Liver Cirrhosis* / pathology
Mice
Protein Disulfide-Isomerases / adverse effects
Protein Disulfide-Isomerases / genetics
Protein Disulfide-Isomerases / metabolism
Thioredoxins / genetics
Thioredoxins / metabolism

Substances

Thioredoxins
Carbon Tetrachloride
Protein Disulfide-Isomerases
TXNDC5 protein, human