| Literature DB >> 31374480 |
Sihyung Wang1, Jieun Kim2, Chanbin Lee3, Dayoung Oh4, Jinsol Han5, Tae-Jin Kim6, Sang-Woo Kim7, Young-Su Seo8, Seh-Hoon Oh9, Youngmi Jung10.
Abstract
Liver fibrosis is a major characteristic of liver disease. When the liver is damaged, quiescent hepatic stellate cells (HSCs) transdifferentiate into proliferative myofibroblastic/activated HSCs, which are the main contributors to liver fibrosis. Hence, a strategy for regulating HSC activation is important in the treatment of liver disease. Tumor necrosis factor-inducible gene 6 protein (TSG-6), a cytokine released from mesenchymal stem cells (MSCs), influences MSC stemness. Therefore, we investigated the biological effect of TSG-6 on HSCs. Human primary HSCs treated with TSG-6 showed significant downregulation of HSC activation markers and upregulation of senescence markers. TSG-6 promoted these cells to express stem cell markers and form spherical organoids, which exhibited elevated expression of stemness-related genes. These organoids differentiated into functional hepatocytic cells under specific culture conditions. Organoids derived from TSG-6-treated HSCs improved livers in organoid transplant mice subjected to CCl4 treatment (which induces liver fibrosis). Furthermore, HSC transdifferentiation by TSG-6 was mediated by Yes-associated protein 1. These findings demonstrate that TSG-6 induces the conversion of HSCs into stem cell-like cells in vitro and that organoids derived from TSG-6-treated HSCs can restore fibrotic liver, suggesting that direct reprogramming of HSCs by TSG-6 can be a useful strategy to control liver disease.Entities:
Keywords: HSC; Liver regeneration; Organoid; Reprogramming; TSG-6
Year: 2019 PMID: 31374480 DOI: 10.1016/j.biomaterials.2019.119375
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479