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凋亡过程中p34cdc2依赖性激酶活性增加:脱氧核糖核酸酶I导致DNA降解的一种可能激活机制。

Increased p34cdc2-dependent kinase activity during apoptosis: a possible activation mechanism of DNase I leading to DNA breakdown.

作者信息

Schroter M, Peitsch M C, Tschopp J

机构信息

Institute of Biochemistry, University of Lausanne, Epalinges, Switzerland.

出版信息

Eur J Cell Biol. 1996 Feb;69(2):143-50.

PMID:8907614
Abstract

Cells undergoing apoptosis typically exhibit distinctive morphological characteristics. Early events include the rounding up of the cell, chromatin condensation, nuclear membrane breakdown and blebbing of the cellular membrane. Strikingly similar changes take place in the cell cycle progression, at the entry into mitosis, suggesting a link between mitosis and apoptosis. Here we show that expression of active p34cdc2 at inappropriate phases during the cell cycle leads to morphological changes reminiscent of apoptosis, including DNA degradation. Cells cotransfected with the active mutant of p34cdc2 and DNase I displayed degraded DNA, which was absent in p34cdc2 wild-type and DNase I-transfected cells, in spite of similar DNase activities. Upon induction of apoptosis in thymocytes, transient p34cdc2 activation was detected prior to lamina breakdown and nuclease activation. P34cdc2 activation was also observed during APO-1 (Fas/CD95)-induced apoptosis in a B lymphoblastoma cell line. Our results suggest that unscheduled activation of p34cdc2 may participate in the initiation of the typical apoptotic phenotype.

摘要

正在经历凋亡的细胞通常表现出独特的形态特征。早期事件包括细胞变圆、染色质浓缩、核膜破裂以及细胞膜起泡。在细胞周期进程中,进入有丝分裂时会发生惊人相似的变化,这表明有丝分裂与凋亡之间存在联系。在此我们表明,在细胞周期的不适当阶段表达活性p34cdc2会导致类似于凋亡的形态变化,包括DNA降解。共转染了p34cdc2活性突变体和DNase I的细胞显示出DNA降解,尽管DNase活性相似,但在p34cdc2野生型和转染了DNase I的细胞中却不存在这种情况。在胸腺细胞诱导凋亡后,在核纤层破裂和核酸酶激活之前检测到短暂的p34cdc2激活。在B淋巴瘤细胞系中APO-1(Fas/CD95)诱导的凋亡过程中也观察到了p34cdc2激活。我们的结果表明,p34cdc2的异常激活可能参与了典型凋亡表型的起始。

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