慢性肝病中ERG转录因子的僵化诱导调节作用

Sonia-Emilia Selicean, Eric Felli, Cong Wang, Yeldos Nulan, Juan José Lozano, Sergi Guixé-Muntet, Horia Ștefănescu, Jaime Bosch, Annalisa Berzigotti, Jordi Gracia-Sancho
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引用次数: 0

摘要

慢性肝病(CLD)的特点是肝窦状内皮细胞(LSECs)功能障碍。机械力和炎症是其中的主要因素。ETS相关基因(ERG)是一种内皮特异性转录因子,参与维持细胞的静止和平衡。我们的研究旨在了解ERG在CLD中的表达和调控。我们对不同疾病阶段人类肝硬化患者的ERG表达进行了表征,并将其与临床数据相关联。在原代健康和肝硬化大鼠LSEC以及人脐静脉内皮细胞(HUVECs)中研究了ERG对僵化和炎症的动态响应。ERG在肝硬化中明显下调,与疾病分期或病因无关,其表达受肝细胞基质硬度的调节。炎症会下调生理硬度细胞中的ERG,但不会下调高硬度细胞中的ERG,这表明炎症和硬度在抑制ERG方面起着互补作用。本研究概述了ERG作为肝硬化LSEC炎症和僵化反应转录因子的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Stiffness-induced modulation of ERG transcription factor in chronic liver disease

Stiffness-induced modulation of ERG transcription factor in chronic liver disease
Chronic liver disease (CLD) is characterised by liver sinusoidal endothelial cells (LSECs) dysfunction. Mechanical forces and inflammation are among the leading factors. ETS-related gene (ERG) is an endothelial-specific transcription factor, involved in maintaining cell quiescence and homeostasis. Our study aimed to understand the expression and modulation of ERG in CLD. ERG expression was characterised and correlated to clinical data in human liver cirrhosis at different disease stages. ERG dynamics in response to stiffness and inflammation were investigated in primary healthy and cirrhotic rat LSEC and in human umbilical vein endothelial cells (HUVECs). ERG is markedly downregulated in cirrhosis independently of disease stage or aetiology and its expression is modulated by substrate stiffness in ECs. Inflammation downregulates ERG in cells on physiological stiffness, but not on high stiffness, suggesting a complementary role of inflammation and stiffness in suppressing ERG. This study outlines ERG as an LSEC inflammation and stiffness-responsive transcription factor in cirrhosis.
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