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生长因子剥夺或蛋白激酶C抑制诱导凋亡过程中基因表达的比较微阵列分析。

Comparative microarray analysis of gene expression during apoptosis-induction by growth factor deprivation or protein kinase C inhibition.

作者信息

Brachat A, Pierrat B, Brüngger A, Heim J

机构信息

Molecular and Cellular Biology Senior Scientific Expert Laboratory, Novartis Pharma AG, CH-4002 Basel, Switzerland.

出版信息

Oncogene. 2000 Oct 19;19(44):5073-82. doi: 10.1038/sj.onc.1203882.

DOI:10.1038/sj.onc.1203882
PMID:11042695
Abstract

The transcriptional response of mouse pro-B cells to two different apoptotic stimuli was investigated. First, interleukin-3 (IL-3) deprivation was used to trigger programmed cell death in IL-3 dependent FL5.12 cells. Alternatively, cells were treated with the protein kinase C (PKC) inhibitor staurosporine. The temporal pattern of gene expression was followed with cDNA microarrays, covering over 8700 different mouse cDNA sequences corresponding to approximately 7900 unique genes. Messenger RNA levels of 315 genes were found to be regulated by more than twofold upon IL-3 removal, while 125 genes reacted to staurosporine treatment. Cross-comparison revealed an intersection of 34 genes similarly regulated in both pathways and thus representing candidates for common apoptosis regulators. For many expressed sequence tags (ESTs) our data suggest for the first time functions in the control of apoptosis, stress response or the cell cycle. IL-3 removal led to the repression of genes required for proliferation and to the induction of genes, linked to apoptotic and signaling pathways. Staurosporine caused predominantly activation of genes, some of which had previously been described to be involved in inflammation. Our findings indicate that cellular responses to both apoptotic stimuli influence various physiological pathways which had not previously been known to be linked.

摘要

研究了小鼠前B细胞对两种不同凋亡刺激的转录反应。首先,利用白细胞介素-3(IL-3)剥夺来触发IL-3依赖性FL5.12细胞中的程序性细胞死亡。另外,用蛋白激酶C(PKC)抑制剂星形孢菌素处理细胞。用覆盖超过8700个不同小鼠cDNA序列(对应于约7900个独特基因)的cDNA微阵列追踪基因表达的时间模式。发现315个基因的信使RNA水平在去除IL-3后受到两倍以上的调节,而125个基因对星形孢菌素处理有反应。交叉比较揭示了34个基因的交集,这些基因在两条途径中受到类似调节,因此代表了常见凋亡调节因子的候选者。对于许多表达序列标签(EST),我们的数据首次表明其在细胞凋亡控制、应激反应或细胞周期中的功能。去除IL-3导致增殖所需基因的抑制以及与凋亡和信号通路相关基因的诱导。星形孢菌素主要导致基因激活,其中一些基因先前已被描述与炎症有关。我们的研究结果表明,细胞对两种凋亡刺激的反应影响了以前未知相互关联的各种生理途径。

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