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首页> 外文期刊>Brain research >Genomic response of the rat brain to global ischemia and reperfusion.
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Genomic response of the rat brain to global ischemia and reperfusion.

机译:大鼠大脑对整体缺血和再灌注的基因组反应。

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摘要

To identify genes that are involved in ischemia response of the brain, we have evaluated changes of gene expression in rat cerebrum after 15 min complete global ischemia, followed by reperfusion for 1 h, 6 h or 24 h. The expression profiles of approximately 30,000 transcripts from three subjects in each group (including sham-operated controls) were monitored employing oligonucleotide microarrays. About 20,000 transcripts were detectable in rat brains. The levels of 576 transcripts (approximately 2.9%) were significantly altered in response to experimental ischemia. 419 transcripts were up- and 157 downregulated; 39 transcripts changed after 1 h reperfusion, 174 after 6 h and 462 after 24 h. Results from quantitative real-time reverse transcription PCR of 18 selected genes showed excellent agreement with the microarray data. There is surprisingly little overlap between gene regulation patterns at different reperfusion times (only seven genes displayed significant changes in transcript levels at all reperfusion times. Several genes that were previously unknown to be involved in ischemia-response have been identified. Analyses of gene ontology patterns and the most strongly regulated transcripts showed that the immediate response to an ischemia/reperfusion is mediated by the induction of specific transcription factors and stress genes. Delayed gene expression response is characterised by inflammation and immune-related genes. These results support the hypothesis that the brain's response to ischemia is an active, specific and coordinated process.
机译:为了鉴定参与脑缺血反应的基因,我们评估了大鼠15分钟完全缺血后再灌注1 h,6 h或24 h后大脑中基因表达的变化。使用寡核苷酸微阵列监测每组中三个受试者(包括假手术对照)的大约30,000个转录物的表达谱。在大鼠脑中可检测到约20,000个转录本。 576个转录物的水平(约2.9%)响应于实验性缺血而显着改变。上调了419个成绩单,下调了157个成绩;再灌注1 h后39个转录本发生变化,6 h后174个变化,24 h后462个变化。 18个选定基因的实时定量逆转录PCR定量分析结果与微阵列数据非常吻合。令人惊讶的是,在不同的再灌注时间之间,基因调控模式之间几乎没有重叠(只有七个基因在所有再灌注时间中均显示出转录水平的显着变化。已鉴定出一些先前未知的参与缺血反应的基因。)调节最强的转录本表明,对缺血/再灌注的即时反应是由特定转录因子和应激基因的诱导介导的;延迟的基因表达反应的特征是炎症和免疫相关基因。这些结果支持以下假设:大脑对局部缺血的反应是一个活跃,特异性和协调的过程。

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