Litcius/Paper detail

Sirtuin 1 ameliorates defenestration in hepatic sinusoidal endothelial cells during liver fibrosis via inhibiting stress‐induced premature senescence

Xiaoying Luo, Yangqiu Bai, Shuli He, Suofeng Sun, Xiaoke Jiang, Zhiyu Yang, Di Lu, Pei‐Ru Wei, Yuan Liang, Cong Peng, Yaru Wang, Ruli Sheng, Shuangyin Han, Xiuling Li, Bingyong Zhang

2021Cell Proliferation40 citationsDOIOpen Access PDF

Abstract

Abstract Objective Premature senescence is related to progerin and involves in endothelial dysfunction and liver diseases. Activating sirtuin 1 (SIRT1) ameliorates liver fibrosis. However, the mechanisms of premature senescence in defenestration of hepatic sinusoidal endothelial cells (HSECs) and how SIRT1 affects HSECs fenestrae remain elusive. Methods We employed the CCl 4 ‐induced liver fibrogenesis rat models and cultured primary HSECs in vitro, administered with the SIRT1‐adenovirus vector, the activator of SIRT1 and knockdown NOX2. We measured the activity of senescence‐associated β‐galactosidase (SA‐β‐gal) in HSECs. Meanwhile, the protein expression of SIRT1, NOX2, progerin, Lamin A/C, Ac p53 K381 and total p53 was detected by Western blot, co‐immunoprecipitation and immunofluorescence. Results In vivo, premature senescence was triggered by oxidative stress during CCl 4 ‐induced HSECs defenestration and liver fibrogenesis, whereas overexpressing SIRT1 with adenovirus vector lessened premature senescence to relieve CCl 4 ‐induced HSECs defenestration and liver fibrosis. In vitro, HSECs fenestrae disappeared, with emerging progerin‐associated premature senescence; these effects were aggravated by H 2 O 2 . Nevertheless, knockdown of NOX2, activation of SIRT1 with resveratrol and SIRT1‐adenovirus vector inhibited progerin‐associated premature senescence to maintain fenestrae through deacetylating p53. Furthermore, more Ac p53 K381 and progerin co‐localized with the abnormal accumulation of actin filament (F‐actin) in the nuclear envelope of H 2 O 2 ‐treated HSECs; in contrast, these effects were rescued by overexpressing SIRT1. Conclusion SIRT1‐mediated deacetylation maintains HSECs fenestrae and attenuates liver fibrogenesis through inhibiting oxidative stress‐induced premature senescence.

Topics & Concepts

SenescenceSirtuinHepatic fibrosisFibrosisLiver fibrosisCell biologyMedicineBiologyChemistryInternal medicineBiochemistryAcetylationGeneSirtuins and Resveratrol in MedicineTelomeres, Telomerase, and SenescenceRetinoids in leukemia and cellular processes