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首页> 外文期刊>Hepatology: Official Journal of the American Association for the Study of Liver Diseases >CX3CL1-CX3CR1 interaction prevents carbon tetrachloride-induced liver inflammation and fibrosis in mice.
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CX3CL1-CX3CR1 interaction prevents carbon tetrachloride-induced liver inflammation and fibrosis in mice.

机译:CX3CL1-CX3CR1相互作用可防止四氯化碳诱导的小鼠肝脏炎症和纤维化。

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Chronic liver disease is associated with hepatocyte injury, inflammation, and fibrosis. Chemokines and chemokine receptors are key factors for the migration of inflammatory cells such as macrophages and noninflammatory cells such as hepatic stellate cells (HSCs). The expression of CX3CR1 and its ligand, CX3CL1, is up-regulated in chronic liver diseases such as chronic hepatitis C. However, the precise role of CX3CR1 in the liver is still unclear. Here we investigated the role of the CX3CL1-CX3CR1 interaction in a carbon tetrachloride (CCl(4))-induced liver inflammation and fibrosis model. CX3CR1 was dominantly expressed in Kupffer cells in the liver. In contrast, the main source of CX3CL1 was HSCs. Mice deficient in CX3CR1 showed significant increases in inflammatory cell recruitment and cytokine production [including tumor necrosis factor alpha (TNF-alpha); monocyte chemoattractant protein 1; macrophage inflammatory protein 1beta; and regulated upon activation, normal T cell expressed, and secreted (RANTES)] after CCl(4) treatment versus wild-type (WT) mice. This suggested that CX3CR1 signaling prevented liver inflammation. Kupffer cells in CX3CR1-deficient mice after CCl(4) treatment showed increased expression of TNF-alpha and transforming growth factor beta and reduced expression of the anti-inflammatory markers interleukin-10 (IL-10) and arginase-1. Coculture experiments showed that HSCs experienced significantly greater activation by Kupffer cells from CCl(4)-treated CX3CR1-deficient mice versus WT mice. Indeed, augmented fibrosis was observed in CX3CR1-deficient mice versus WT mice after CCl(4) treatment. Finally, CX3CL1 treatment induced the expression of IL-10 and arginase-1 in WT cultured Kupffer cells through CX3CR1, which in turn suppressed HSC activation. CONCLUSION: The CX3CL1-CX3CR1 interaction inhibits inflammatory properties in Kupffer cells/macrophages and results in decreased liver inflammation and fibrosis.
机译:慢性肝病与肝细胞损伤,炎症和纤维化有关。趋化因子和趋化因子受体是炎性细胞(例如巨噬细胞)和非炎性细胞(例如肝星状细胞(HSC))迁移的关键因素。在诸如慢性丙型肝炎的慢性肝脏疾病中,CX3CR1及其配体CX3CL1的表达上调。但是,CX3CR1在肝脏中的确切作用仍不清楚。在这里我们调查了四氯化碳(CCl(4))诱导的肝脏炎症和纤维化模型中CX3CL1-CX3CR1相互作用的作用。 CX3CR1主要在肝脏的库普弗细胞中表达。相反,CX3CL1的主要来源是HSC。缺乏CX3CR1的小鼠表现出炎症细胞募集和细胞因子产生的显着增加[包括肿瘤坏死因子α(TNF-alpha);单核细胞趋化蛋白1;巨噬细胞炎性蛋白1beta;和激活后,正常的T细胞表达和分泌(RANTES)] CCl(4)治疗后与野生型(WT)小鼠。这表明CX3CR1信号传导可预防肝脏炎症。 CCl(4)处理后,CX3CR1缺陷型小鼠中的枯否细胞显示TNF-alpha和转化生长因子β的表达增加,抗炎标记白介素10(IL-10)和精氨酸酶1的表达降低。共培养实验表明,HSC经历了Kupffer细胞从CCl(4)处理的CX3CR1缺陷小鼠相对于WT小鼠明显更大的激活。确实,在CCl(4)处理后,在CX3CR1缺陷小鼠与WT小鼠中观察到纤维化增强。最后,CX3CL1处理通过CX3CR1诱导WT培养的Kupffer细胞中IL-10和精氨酸酶1的表达,从而抑制了HSC的活化。结论:CX3CL1-CX3CR1相互作用抑制了库普弗细胞/巨噬细胞的炎症特性,并导致肝脏炎症和纤维化减少。

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