HIF-1α 促进缺氧依赖性细胞迁移

Liyuan Li, Chikezie O Madu, Andrew Lu, Yi Lu
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摘要

众所周知,缺氧诱导因子-1α(HIF-1α)是血管内皮生长因子基因启动子的转录激活因子。它可被缺氧诱导。然而,迄今为止还没有研究将 HIF-1α 介导的效应与缺氧或 VEGF 介导的效应区分开来。本研究通过在小鼠胚胎成纤维细胞(MEF)中使用 HIF-1α 基因敲除(HIF-1α KO)细胞系统,分析了细胞迁移与 HIF-1α、缺氧和血管内皮生长因子的激活。研究观察了缺氧介导的HIF-1α诱导和VEGF转活化:与常氧相比,HIF-1α WT品系在缺氧条件下的VEGF转活化(作为HIF-1α诱导的指标)显著增加;相反,HIF-1α KO品系在缺氧条件下的VEGF转活化没有增加。HIF-1α 促进细胞迁移:与 HIF-1α WT 细胞相比,HIF-1α-KO 细胞在正常缺氧和低氧条件下的迁移都明显减少。通过腺病毒介导的基因转移恢复 WT HIF-1α 的表达,可以部分缓解 HIF-1α KO 细胞迁移能力明显下降的问题。有趣的是,缺氧对细胞迁移没有影响:在缺氧和常氧条件下,HIF-1α WT 和 HIF-1α KO 株的细胞迁移率相似。总之,这些数据表明,HIF-1α 在 MEF 细胞迁移中的作用与缺氧介导的效应无关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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HIF-1α Promotes A Hypoxia-Independent Cell Migration.

Hypoxia-inducible factor-1α (HIF-1α) is known as a transactivator for VEGF gene promoter. It can be induced by hypoxia. However, no study has been done so far to dissect HIF-1α-mediated effects from hypoxia or VEGF-mediated effects. By using a HIF-1α knockout (HIF-1α KO) cell system in mouse embryonic fibroblast (MEF) cells, this study analyzes cell migration and HIF-1α, hypoxia and VEGF activation. A hypoxia-mediated HIF-1α induction and VEGF transactivation were observed: both HIF-1α WT lines had significantly increased VEGF transactivation, as an indicator for HIF-1α induction, in hypoxia compared to normoxia; in contrast, HIF-1α KO line had no increased VEGF transactivation under hypoxia. HIF-1α promotes cell migration: HIF-1α-KO cells had a significantly reduced migration compared to that of the HIF-1α WT cells under both normoxia and hypoxia. The significantly reduced cell migration in HIF-1α KO cells can be partially rescued by the restoration of WT HIF-1α expression mediated by adenoviral-mediated gene transfer. Interestingly, hypoxia has no effect on cell migration: the cells had a similar cell migration rate under hypoxic and normoxic conditions for both HIF-1α WT and HIF-1α KO lines, respectively. Collectively, these data suggest that HIF-1α plays a role in MEF cell migration that is independent from hypoxia-mediated effects.

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