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Genomics of the fetal hypothalamic cellular response to transient hypoxia: endocrine immune and metabolic responses

机译:胎儿下丘脑细胞对短暂性低氧反应的基因组学:内分泌免疫和代谢反应

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摘要

Fetuses respond to transient hypoxia (a common stressor in utero) with cellular responses that are appropriate for promoting survival of the fetus. The present experiment was performed to identify the acute genomic responses of the fetal hypothalamus to transient hypoxia. Three fetal sheep were exposed to 30 min of hypoxia and hypothalamic mRNA extracted from samples collected 30 min after return to normoxia. These samples were compared with those from four normoxic control fetuses by the Agilent 019921 ovine array. Differentially regulated genes were analyzed by network analysis and by gene ontology analysis, identifying statistically significant overrepresentation of biological processes. Real-time PCR of selected genes supported the validity of the array data. Hypoxia induced increased expression of genes involved in response to oxygen stimulus, RNA splicing, antiapoptosis, vascular smooth muscle proliferation, and positive regulation of Notch receptor target. Downregulated genes were involved in metabolism, antigen receptor-mediated immunity, macromolecular complex assembly, S-phase, translation elongation, RNA splicing, protein transport, and posttranscriptional regulation. We conclude that these results emphasize that the cellular response to hypoxia involves reduced metabolism, the involvement of the fetal immune system, and the importance of glucocorticoid signaling.
机译:胎儿对短暂的缺氧(子宫内常见的应激源)作出反应,并通过细胞反应来促进胎儿的存活。进行本实验以鉴定胎儿下丘脑对短暂性缺氧的急性基因组反应。将三只胎羊暴露于缺氧状态30分钟,并从恢复正常氧状态30分钟后收集的样品中提取下丘脑mRNA。通过Agilent 019921绵羊阵列将这些样品与来自四个常氧对照胎儿的样品进行比较。通过网络分析和基因本体分析对差异调节基因进行了分析,从而确定了生物学过程的统计学显着过量代表。选定基因的实时PCR支持阵列数据的有效性。缺氧诱导与氧刺激,RNA剪接,抗凋亡,血管平滑肌增生以及Notch受体靶标的正调控有关的基因表达增加。下调的基因参与代谢,抗原受体介导的免疫,大分子复合物装配,S期,翻译延伸,RNA剪接,蛋白质转运和转录后调控。我们得出结论,这些结果强调,对缺氧的细胞反应涉及代谢减少,胎儿免疫系统的参与以及糖皮质激素信号传导的重要性。

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