缺血对基因表达的影响。

J. Huang, R. Qi, John Quackenbush, E. Dauway, E. Lazaridis, T. Yeatman
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引用次数: 154

摘要

微阵列基因表达技术最近使得表征大量组织样本中数千个基因的RNA表达成为可能。我们假设通常与手术切除人体组织相关的热缺血会对基因表达谱产生重大影响。为了量化热缺血对人体组织的影响,我们从人结肠癌标本上快速解剖正常粘膜。将标本分开,室温保存至液氮速冻。等量组织在取出后5、10、15、20、40和60分钟冷冻。使用由2400个不同元素组成的斑点微阵列来检测来自每个时间点的mRNA。采用Eisen分层聚类法和贝叶斯统计方法分析热缺血对基因表达的影响。时间过程统计模型的应用表明,缺血诱导了三种模式,分别占可评价基因的68.2、17.8%和13.4%。模式1对应于5分钟基线表达水平在60分钟内平均变化27%,63.8%至少有80%概率属于该模式的基因在60分钟内平均表达增加,其余基因平均表达减少。模式II基因表现出最小的缺血相关影响,在60分钟内平均仅变化12%。与模式I相比,我们发现67.5%的至少80%概率属于该模式的基因随着时间的推移平均表达减少。剩下的32.5%在60分钟内平均增加了12%。最后,模式III基因(占样本的13.4%)对缺血表现出最大的敏感性,在60分钟内平均改变了50%,增加和减少的数量大致相同。观察到RNA过表达或低表达的折叠变化高达20倍以上。热缺血与手术切除人体组织有关,对基因表达有显著影响。这些数据支持仔细监测为基因谱目的采集的组织的缺血时间。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effects of ischemia on gene expression.
Microarray gene expression technology has recently made it feasible to characterize the RNA expression of thousands of genes across numerous tissue samples. We hypothesized that the warm ischemia commonly associated with the surgical extirpation of human tissue would have significant effects on gene expression profiles. To quantitate the effects of warm ischemia on human tissue, we rapidly dissected normal mucosa from a human colon cancer specimen. The specimen was divided and maintained at room temperature until snap-frozen in liquid nitrogen. Aliquots of tissue were frozen at times 5, 10, 15, 20, 40, and 60 min after extirpation. Spotted microarrays composed of 2400 distinct elements were used to assay mRNA derived from each time point in triplicate. Eisen's hierarchical clustering methodology and Bayesean statistical methods were then used to assay the effects of warm ischemia on gene expression. Application of time-course statistical models suggest that three patterns were induced by ischemia, accounting for 68.2, 17.8, and 13.4% of the evaluable genes, respectively. Pattern I corresponds to an average change of 27% over 60 min from 5 min baseline level of expression and 63.8% of the genes with at least 80% probability of membership in this pattern show average increases in expression over 60 min. The remainder decrease on average. Pattern II genes show the least ischemia-related effects, demonstrating an average change of only 12% over 60 min. In contrast to pattern I, we find that 67.5% of the genes with at least 80% probability of membership in this pattern are decreasing in expression on average over time. The remaining 32.5% in this pattern increase an average of 12% over 60 min. Finally, pattern III genes (13.4% of the sample) show the greatest sensitivity to ischemia, changing an average of 50% over 60 min, with about the same number increasing as are decreasing. Fold changes in RNA over- or under-expression were observed up to greater than 20-fold. Warm ischemia associated with the surgical extirpation of human tissues has significant effects on gene expression. These data support the careful monitoring of ischemic time for tissues harvested for the purpose of gene profiling.
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