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细胞凋亡并不需要细胞核和DNA片段化。

Cell nucleus and DNA fragmentation are not required for apoptosis.

作者信息

Schulze-Osthoff K, Walczak H, Dröge W, Krammer P H

机构信息

Division of Immunochemistry, Deutsches Krebsforschungszentrum, Heidelberg, FRG.

出版信息

J Cell Biol. 1994 Oct;127(1):15-20. doi: 10.1083/jcb.127.1.15.

Abstract

Apoptosis is the predominant form of cell death and occurs under a variety of physiological and pathological conditions. Cells undergoing apoptotic cell death reveal a characteristic sequence of cytological alterations including membrane blebbing and nuclear and cytoplasmic condensation. Activation of an endonuclease which cleaves genomic DNA into internucleosomal DNA fragments is considered to be the hallmark of apoptosis. However, no clear evidence exists that DNA degradation plays a primary and causative role in apoptotic cell death. Here we show that cells enucleated with cytochalasin B still undergo apoptosis induced either by treatment with menadione, an oxidant quinone compound, or by triggering APO-1/Fas, a cell surface molecule involved in physiological cell death. Incubation of enucleated cells with the agonistic monoclonal anti-APO-1 antibody revealed the key morphological features of apoptosis. Moreover, in non-enucleated cells inhibitors of endonuclease blocked DNA fragmentation, but not cell death induced by anti-APO-1. These data suggest that DNA degradation and nuclear signaling are not required for induction of apoptotic cell death.

摘要

细胞凋亡是细胞死亡的主要形式,发生在多种生理和病理条件下。经历凋亡性细胞死亡的细胞呈现出一系列特征性的细胞学改变,包括细胞膜起泡以及细胞核和细胞质浓缩。一种将基因组DNA切割成核小体间DNA片段的核酸内切酶的激活被认为是细胞凋亡的标志。然而,尚无明确证据表明DNA降解在凋亡性细胞死亡中起主要和因果作用。在此我们表明,用细胞松弛素B去核的细胞仍会经历由维生素K3(一种氧化醌化合物)处理或通过触发APO-1/Fas(一种参与生理性细胞死亡的细胞表面分子)诱导的凋亡。用激动性抗APO-1单克隆抗体孵育去核细胞揭示了凋亡的关键形态学特征。此外,在未去核的细胞中,核酸内切酶抑制剂可阻断DNA片段化,但不能阻断抗APO-1诱导的细胞死亡。这些数据表明,诱导凋亡性细胞死亡不需要DNA降解和核信号传导。

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