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暴露于热疗(HS)或4-氢过氧环磷酰胺(4CP)的第9天小鼠胚胎中诱导的基因表达变化:使用cDNA微阵列进行分析。

Alterations in gene expression induced in day-9 mouse embryos exposed to hyperthermia (HS) or 4-hydroperoxycyclophosphamide (4CP): analysis using cDNA microarrays.

作者信息

Mikheeva Svetlana, Barrier Marianne, Little Sally A, Beyer Richard, Mikheev Andrei M, Kerr M Kathleen, Mirkes Philip E

机构信息

Birth Defects Research Laboratory, Division of Genetics and Developmental Medicine, Department of Pediatrics, University of Washington, Seattle, Washington 98195, USA.

出版信息

Toxicol Sci. 2004 Jun;79(2):345-59. doi: 10.1093/toxsci/kfh080. Epub 2004 Feb 19.

Abstract

Teratogen-induced alterations in gene expression play an important role in the genesis of malformations in animals. The recent development of DNA microarrays now offers the opportunity to monitor global changes in gene expression and therefore the potential to obtain significant new information concerning both normal and abnormal development. RNA was isolated from day-9 mouse embryos at 1 and 5 h after exposure to hyperthermia (HS) or 4-hydroperoxycyclophosphamide (4CP) and compared to RNA isolated from concurrent controls using mouse cDNA microarrays. Cy5/Cy3 intensity data were extracted using Spot-on Image software and then normalized using the statistical software program R/maanova. Differentially expressed genes were identified using a linear mixed-effects model and p values derived from t-test statistics. Approximately 9000 genes show statistically significant alterations in expression in day-9 mouse embryos exposed to HS or 4CP. HS and 4CP also induce alterations in the expression of distinct sets of genes, e.g., DNA replication/repair, cell cycle, signal transduction, and transcription-related genes. As expected, a variety of heat shock genes are upregulated by HS but not 4CP. Among genes whose expression is altered by both HS and 4CP, cluster analysis identified three p53 target genes (Cyclin G1, Gtse1, and Mdm2), and follow up studies confirmed that p53 is activated in embryos exposed to these two teratogens. In addition, cluster analyses also revealed that HS but not 4CP induces the downregulation of genes encoding key enzymes in the cholesterol biosynthesis pathway. Thus, our microarray data have identified one potentially important pathway (p53) common to both HS- and 4CP-induced teratogenesis and another pathway (cholesterol biosynthesis) potentially important, but specific to HS-induced teratogenesis.

摘要

致畸剂引起的基因表达改变在动物畸形的发生中起重要作用。DNA微阵列技术的最新发展为监测基因表达的整体变化提供了机会,从而有可能获得有关正常和异常发育的重要新信息。在暴露于高温(HS)或4-氢过氧环磷酰胺(4CP)后1小时和5小时,从第9天的小鼠胚胎中分离RNA,并使用小鼠cDNA微阵列与同时期对照的RNA进行比较。使用Spot-on Image软件提取Cy5/Cy3强度数据,然后使用统计软件程序R/maanova进行标准化。使用线性混合效应模型和t检验统计得出的p值来鉴定差异表达的基因。在暴露于HS或4CP的第9天小鼠胚胎中,约9000个基因的表达有统计学上的显著改变。HS和4CP还诱导不同基因集的表达改变,例如DNA复制/修复、细胞周期、信号转导和转录相关基因。正如预期的那样,多种热休克基因被HS上调,但未被4CP上调。在其表达被HS和4CP均改变的基因中,聚类分析鉴定出三个p53靶基因(细胞周期蛋白G1、Gtse1和Mdm2),后续研究证实p53在暴露于这两种致畸剂的胚胎中被激活。此外,聚类分析还显示,HS而非4CP诱导胆固醇生物合成途径中关键酶编码基因的下调。因此,我们的微阵列数据确定了一条在HS和4CP诱导的致畸作用中共同的潜在重要途径(p53),以及另一条潜在重要但特定于HS诱导的致畸作用的途径(胆固醇生物合成)。

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