抑制 Survivin 可通过诱导肝星状细胞衰老和消耗肝巨噬细胞数量来改善肝纤维化

IF 3.6 3区 生物学 Q3 CELL BIOLOGY
Sachin Sharma, Shaikh Maryam Ghufran, Mehreen Aftab, Chhagan Bihari, Sampa Ghose, Subhrajit Biswas
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引用次数: 0

摘要

损伤肝脏中的肝星状细胞(HSCs)持续活化会导致肝脏损伤从纤维化发展为有害的肝硬化。在之前的一项研究中,我们发现存活素蛋白在造血干细胞早期活化过程中上调,从而引发肝纤维化的发生。然而,在已完全形成纤维化的肝脏中靶向存活素的治疗潜力还有待研究。在这项研究中,我们使用四氯化碳(CCl4)对小鼠进行了为期6周的肝纤维化化学诱导,随后使用一种存活素抑制剂(YM155)进行治疗。我们还通过组织学分析评估了存活素在纤维化人肝组织、原代造血干细胞和造血干细胞系中的表达。人和小鼠纤维化肝组织中的αSMA+造血干细胞显示出更强的存活素表达,而肝细胞和静止造血干细胞(qHSCs)则显示出最低表达。另外,活化的M2巨噬细胞亚型通过TGF-β-TGF-β受体-I/II信号传导诱导造血干细胞中存活素的表达。抑制造血干细胞中的存活素会促进细胞周期停滞和衰老,最终抑制造血干细胞的活化。在体内,YM155 处理增加了纤维化隔膜周围造血干细胞中细胞衰老制造者的表达,如 p53、p21 和 β-半乳糖苷酶。体内 YM155 治疗还减少了肝巨噬细胞数量和肝脏中炎性细胞因子的表达。总之,下调纤维化肝脏中的存活素可以通过诱导细胞衰老和调节巨噬细胞细胞因子的表达来减少造血干细胞的活化,从而共同改善肝纤维化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Survivin inhibition ameliorates liver fibrosis by inducing hepatic stellate cell senescence and depleting hepatic macrophage population

Survivin inhibition ameliorates liver fibrosis by inducing hepatic stellate cell senescence and depleting hepatic macrophage population

Persistent activation of hepatic stellate cells (HSCs) in the injured liver leads to the progression of liver injury from fibrosis to detrimental cirrhosis. In a previous study, we have shown that survivin protein is upregulated during the early activation of HSCs, which triggers the onset of liver fibrosis. However, the therapeutic potential of targeting survivin in a fully established fibrotic liver needs to be investigated. In this study, we chemically induced hepatic fibrosis in mice using carbon tetrachloride (CCl4) for 6 weeks, which was followed by treatment with a survivin suppressant (YM155). We also evaluated survivin expression in fibrotic human liver tissues, primary HSCs, and HSC cell line by histological analysis. αSMA+ HSCs in human and mice fibrotic liver tissues showed enhanced survivin expression, whereas the hepatocytes and quiescent (qHSCs) displayed minimal expression. Alternatively, activated M2 macrophage subtype induced survivin expression in HSCs through the TGF-β-TGF-β receptor-I/II signaling. Inhibition of survivin in HSCs promoted cell cycle arrest and senescence, which eventually suppressed their activation. In vivo, YM155 treatment increased the expression of cell senescence makers in HSCs around fibrotic septa such as p53, p21, and β-galactosidase. YM155 treatment in vivo also reduced the hepatic macrophage population and inflammatory cytokine expression in the liver. In conclusion, downregulation of survivin in the fibrotic liver decreases HSC activation by inducing cellular senescence and modulating macrophage cytokine expression that collectively ameliorates liver fibrosis.

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来源期刊
CiteScore
6.40
自引率
4.90%
发文量
40
期刊介绍: The Journal of Cell Communication and Signaling provides a forum for fundamental and translational research. In particular, it publishes papers discussing intercellular and intracellular signaling pathways that are particularly important to understand how cells interact with each other and with the surrounding environment, and how cellular behavior contributes to pathological states. JCCS encourages the submission of research manuscripts, timely reviews and short commentaries discussing recent publications, key developments and controversies. Research manuscripts can be published under two different sections : In the Pathology and Translational Research Section (Section Editor Andrew Leask) , manuscripts report original research dealing with celllular aspects of normal and pathological signaling and communication, with a particular interest in translational research. In the Molecular Signaling Section (Section Editor Satoshi Kubota) manuscripts report original signaling research performed at molecular levels with a particular interest in the functions of intracellular and membrane components involved in cell signaling.
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