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一种哺乳动物体外中心粒复制系统:细胞周期蛋白依赖性激酶2/细胞周期蛋白E及核仁素/B23参与中心体复制的证据

A mammalian in vitro centriole duplication system: evidence for involvement of CDK2/cyclin E and nucleophosmin/B23 in centrosome duplication.

作者信息

Tarapore Pheruza, Okuda Masaru, Fukasawa Kenji

机构信息

Department of Cell Biology, University of Cincinnati College of Medicine, P.O. Box 670521, Ohio 45267-0521, USA.

出版信息

Cell Cycle. 2002 Jan;1(1):75-81.

Abstract

Centrosome duplication in mammalian cells is a highly regulated process, occurs in coordination of other cell cycle events. However, molecular exploration of this important cellular process had been difficult due to unavailability of a simple assay system. Here, using centrosomes loosely associated with nuclei isolated from cultured cells, we developed a cell-free centriole (duplication unit of the centrosome) duplication system: unduplicated centrosomes bound to the nuclei are able to undergo duplication in the presence of G1/S extracts. We show that the ability of G1/S extracts to induce centriole duplication in vitro depends on the presence of active CDK2/cyclin E. It has been shown that dissociation of centro-somal nucleophosmin (NPM)/B23 triggered by CDK2/cyclin E-mediated phosphorylation is required for initiation of centrosome duplication. We show that centriole duplication is blocked when nuclei were preincubated with the anti-NPM/B23 antibody that prevents phosphorylation of NPM/B23 by CDK2/cyclin E. These studies provide not only direct evidence for the requirement of CDK2/cyclin E and phosphorylation of NPM/B23 for centrosomes to initiate duplication, but a valuable experimental system for further exploration of the molecular regulation of centrosome duplication in somatic cells of higher animals.

摘要

哺乳动物细胞中的中心体复制是一个高度受调控的过程,与其他细胞周期事件协调发生。然而,由于缺乏简单的检测系统,对这一重要细胞过程的分子探索一直很困难。在这里,我们利用从培养细胞中分离出的与细胞核松散结合的中心体,开发了一种无细胞的中心粒(中心体的复制单位)复制系统:与细胞核结合的未复制中心体在存在G1/S提取物的情况下能够进行复制。我们表明,G1/S提取物在体外诱导中心粒复制的能力取决于活性CDK2/细胞周期蛋白E的存在。已经表明,CDK2/细胞周期蛋白E介导的磷酸化引发的中心体核磷蛋白(NPM)/B23的解离是中心体复制起始所必需的。我们表明,当细胞核与抗NPM/B23抗体预孵育时,中心粒复制被阻断,该抗体可阻止CDK,2/细胞周期蛋白E对NPM/B23的磷酸化。这些研究不仅为CDK2/细胞周期蛋白E和NPM/B23磷酸化对中心体起始复制的必要性提供了直接证据,也为进一步探索高等动物体细胞中中心体复制的分子调控提供了一个有价值的实验系统。

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