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首页> 外文期刊>American Journal of Physiology >Role of nitric oxide in the regulation of HIF-1alpha expression during hypoxia.
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Role of nitric oxide in the regulation of HIF-1alpha expression during hypoxia.

机译:一氧化氮在缺氧过程中对HIF-1alpha表达的调节作用。

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摘要

Hypoxia-inducible factor-1 (HIF-1), a heterodimeric transcription factor consisting of HIF-1alpha and HIF-1beta subunits, controls the expression of a large number of genes involved in the regulation of cellular responses to reduced oxygen availability. The oxygen-regulated subunit, HIF-1alpha, is stabilized in cells exposed to hypoxia. The regulation of hypoxic responses by nitric oxide (NO) is believed to have wide pathophysiological relevance, thus we investigated whether NO affects HIF-1 activation in hypoxic cells. Here we show that NO generated from NO donors prevented HIF-1alpha hypoxic accumulation in Hep 3B and PC-12 cells. Addition of a glutathione analog or peroxynitrite scavengers prevented the NO-induced inhibition of HIF-1alpha accumulation in both cell lines. Exposure to NO was associated with inhibition of mitochondrial electron transport and compensatory glycolysis, which maintained normal cellular ATP content. Succinate, a Krebs cycle intermediate and respiratory chain substrate, restored HIF-1alpha hypoxic induction in the cells, suggesting involvement of mitochondria in regulation of HIF-1alpha accumulation during hypoxia. Regulation of HIF-1alpha by NO is an additional important mechanism by which NO might modulate cellular responses to hypoxia in mammalian cells.
机译:缺氧诱导因子-1(HIF-1)是由HIF-1alpha和HIF-1beta亚基组成的异二聚体转录因子,控制着大量基因的表达,这些基因参与调节细胞对减少氧的利用的反应。氧调节的亚基HIF-1alpha在暴露于低氧的细胞中稳定。一氧化氮(NO)对缺氧反应的调节被认为具有广泛的病理生理相关性,因此我们研究了NO是否影响缺氧细胞中的HIF-1活化。在这里,我们显示从NO供体产生的NO阻止了Hep 3B和PC-12细胞中的HIF-1alpha低氧积累。添加谷胱甘肽类似物或过亚硝酸盐清除剂可防止NO诱导的两种细胞系中HIF-1α积累的抑制。暴露于NO与抑制线粒体电子运输和代偿性糖酵解有关,后者维持正常的细胞ATP含量。琥珀酸是一个克雷布斯循环的中间和呼吸链底物,恢复了细胞中HIF-1alpha的低氧诱导作用,表明线粒体参与了缺氧期间HIF-1alpha的调节。 NO对HIF-1alpha的调节是NO可能调节哺乳动物细胞对缺氧的细胞应答的另一重要机制。

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