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大鼠颗粒细胞和黄体细胞核中一种脱氧核糖核酸酶I样内切核酸酶的鉴定。

Identification of a deoxyribonuclease I-like endonuclease in rat granulosa and luteal cell nuclei.

作者信息

Boone D L, Yan W, Tsang B K

机构信息

Department of Obstetrics & Gynecology, University of Ottawa, Ontario, Canada.

出版信息

Biol Reprod. 1995 Nov;53(5):1057-65. doi: 10.1095/biolreprod53.5.1057.

DOI:10.1095/biolreprod53.5.1057
PMID:8527508
Abstract

Apoptosis, a process recently implicated as the cellular mechanism underlying ovarian follicular atresia and luteal regression, is characterized by the internucleosomal degradation of DNA by a Ca2+/Mg(2+)-dependent endonuclease. Although hormones and growth factors have been demonstrated to modulate the DNA degradation associated with ovarian follicular apoptosis, the nature and identity of the endonuclease involved is not known. Ca2+/Mg(2+)-dependent endonuclease activity has a developmental pattern of expression in rat granulosa and luteal cell nuclei. Thus, the present study was conducted to establish the presence of an endonuclease in the nuclei of ovarian granulosa and luteal cells and to examine the biochemical properties of the enzyme relevant to apoptosis. Nuclei from diethyl-stilbestrol (DES)-, eCG-, and hCG-primed rat ovaries were isolated and exposed to Ca2+ and Mg2+ in vitro. Nuclei from rat ovaries primed with eCG and hCG, but not DES, substantially degraded their DNA in an apoptotic fashion, and this DNA degradation was Ca2+/Mg(2+)-dependent and inhibited by Zn2+. Protein extracts from the nuclei of DES-, eCG-, and hCG-treated rat ovaries were tested for endonuclease activity by a plasmid degradation assay. The extracts were found to contain endonuclease activity with the same developmental pattern and cation dependency as found in intact nuclei. These protein extracts were assessed for nuclease activity by zymography, and three nuclease activities were identified depending on the type of DNA used in the gel and the electrophoresis conditions used for protein separation.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

凋亡是一种最近被认为是卵巢卵泡闭锁和黄体退化潜在细胞机制的过程,其特征是DNA在一种Ca2+/Mg(2+)依赖性核酸内切酶作用下发生核小体间降解。尽管已经证明激素和生长因子可调节与卵巢卵泡凋亡相关的DNA降解,但所涉及的核酸内切酶的性质和身份尚不清楚。Ca2+/Mg(2+)依赖性核酸内切酶活性在大鼠颗粒细胞和黄体细胞核中有发育性表达模式。因此,本研究旨在确定卵巢颗粒细胞和黄体细胞核中是否存在核酸内切酶,并研究与凋亡相关的该酶的生化特性。从经己烯雌酚(DES)、马绒毛膜促性腺激素(eCG)和人绒毛膜促性腺激素(hCG)预处理的大鼠卵巢中分离细胞核,并在体外使其暴露于Ca2+和Mg2+。用eCG和hCG预处理而非DES预处理的大鼠卵巢细胞核以凋亡方式大量降解其DNA,且这种DNA降解是Ca2+/Mg(2+)依赖性的,并受到Zn2+的抑制。通过质粒降解试验检测经DES、eCG和hCG处理的大鼠卵巢细胞核的蛋白质提取物的核酸内切酶活性。发现这些提取物含有核酸内切酶活性,其发育模式和阳离子依赖性与完整细胞核中的相同。通过酶谱分析评估这些蛋白质提取物的核酸酶活性,根据凝胶中使用的DNA类型和蛋白质分离所用的电泳条件鉴定出三种核酸酶活性。(摘要截短于250字)

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