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首页> 外文期刊>Liver international : >Hypoxia-inducible factor-1alpha regulates the expression of genes in hypoxic hepatic stellate cells important for collagen deposition and angiogenesis.
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Hypoxia-inducible factor-1alpha regulates the expression of genes in hypoxic hepatic stellate cells important for collagen deposition and angiogenesis.

机译:缺氧诱导因子-1Alpha调节对胶原沉积和血管生成的缺氧肝星状细胞中基因的表达。

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BACKGROUND/AIMS: Several studies have shown that regions of hypoxia develop in the liver during chronic injury. Furthermore, it has been demonstrated that hypoxia stimulates the release of mediators from hepatic stellate cells (HSCs) that may affect the progression of fibrosis. The mechanism by which hypoxia modulates gene expression in HSCs is not known. Recent studies demonstrated that the hypoxia-activated transcription factor, hypoxia-inducible factor (HIF)-1alpha, is critical for the development of fibrosis. Accordingly, the hypothesis was tested that HIF-1alpha is activated in HSCs and regulates the expression of genes important for HSC activation and liver fibrosis. METHODS: Hepatic stellate cells were isolated from mice and exposed to hypoxia. HIF-1alpha and HIF-2alpha activation were measured, and gene expression was analysed by gene array analysis. To identify the genes regulated by HIF-1alpha, HSCs were isolated from control and HIF-1alpha-deficient mice. RESULTS: Exposure of primary mouse HSCs to 0.5% oxygen activated HIF-1alpha and HIF-2alpha. mRNA levels of numerous genes were increased in HSCs exposed to 0.5% oxygen, many of which are important for HSC function, angiogenesis and collagen synthesis. Of the mRNAs increased, chemokine receptor (Ccr) 1, Ccr5, macrophage migration inhibitory factor, interleukin-13 receptor alpha1 and prolyl-4-hydroxylase alpha2 (P4h alpha2) were completely HIF-1alpha dependent. Upregulation of the vascular endothelial growth factor and the placental growth factor was partially HIF-1alpha dependent and upregulation of angiopoietin-like 4 and P4h alpha1 was HIF-1alpha independent. CONCLUSIONS: Results from these studies demonstrate that hypoxia, through activation of HIF-1alpha, regulates the expression of genes that may alter the sensitivity of HSCs to certain activators and chemotaxins, and regulates the expression of genes important for angiogenesis and collagen synthesis.
机译:背景/目标:几项研究表明,慢性损伤期间缺氧区域在肝脏中发育。此外,已经证明缺氧刺激可能影响纤维化进展的肝星状细胞(HSC)的介质释放。缺氧调节HSC中基因表达的机制是不知道的。最近的研究表明,缺氧活化的转录因子,缺氧诱导因子(HIF)-1Alpha对纤维化的发展至关重要。因此,测试假设,即HIF-1α在HSC中被激活,并调节对HSC活化和肝纤维化重要的基因的表达。方法:从小鼠中分离肝星状细胞并暴露于缺氧。测量HIF-1Alpha和HIF-2Alpha激活,并通过基因阵列分析分析基因表达。为了鉴定HIF-1Alpha调节的基因,从对照和HIF-1Alpha缺陷小鼠中分离HSC。结果:原发性小鼠HSC的暴露于0.5%氧活化HIF-1α和HIF-2Alpha。在暴露于0.5%氧的HSC中,许多基因的mRNA水平增加,其中许多对于HSC功能,血管生成和胶原合成是重要的。 MRNA增加,趋化因子受体(CCR)1,CCR5,巨噬细胞迁移抑制因子,白细胞介素-13受体α1和脯氨酰-4-羟化酶α2(P4Hα2)是完全HIF-1α的依赖性。血管内皮生长因子的上调和胎盘生长因子是部分HIF-1α的依赖性和上调血管发成素4和P4Hα1的上调是HIF-1α独立的。结论:这些研究的结果表明,通过激活HIF-1α的激活来调节可能改变HSCs对某些活化剂和趋化素的基因的表达,并调节对血管生成和胶原合成重要的基因的表达。

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