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无细胞体系中程序化细胞周期蛋白降解的调控

Control of programmed cyclin destruction in a cell-free system.

作者信息

Luca F C, Ruderman J V

机构信息

Department of Anatomy and Cell Biology, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

J Cell Biol. 1989 Nov;109(5):1895-909. doi: 10.1083/jcb.109.5.1895.

Abstract

To ask what controls the periodic accumulation and destruction of the mitotic across the cell cycle, we have developed a cell-free system from clam embryos that reproduces several aspects of cyclin behavior. One or more rounds of cyclin proteolysis and resynthesis occur in vitro, and the destruction of the cyclins is highly specific. The onset, duration, and extent of cyclin destruction and the appropriately stagered disappearance of cyclin A and cyclin B are correctly regulated during the first cycle in the cell-free system. Just as in intact cells, lysates made from early interphase cells require further protein synthesis to reach the cyclin destruction point, and lysates made from later stages do not. Using the cell-free system we show that cyclin disappearance requires ATP and Mg2+. By combining lysates from different cell cycle stages, we show that (a) interphase lysates do not contain a dominant inhibitor of cyclin destruction and (b) the timing of cyclin destruction is determined by the cell cycle stage of the cytoplasm rather than the cell cycle stage of the substrate cyclins themselves. Among a large variety of agents tested, only a few affect cyclin destruction. Tosyl-lysine chlormethyl ketone (TLCK, a protease inhibitor), 6-dimethylaminopurine (6-DMAP, a kinase inhibitor), certain sulfhydryl-blocking agents, ZnCl2 and EDTA (but not EGTA) completely block cyclin destruction in vitro. Addition of 1 mM Ca2+ to the cell-free system has no effect on cyclin stability, but 5 mM Ca2+ leads to the rapid destruction of cyclins and a small number of other proteins.

摘要

为了探究在整个细胞周期中是什么控制着有丝分裂周期蛋白的周期性积累和降解,我们从蛤胚胎中开发了一种无细胞体系,该体系能重现周期蛋白行为的几个方面。在体外会发生一轮或多轮周期蛋白的蛋白水解和再合成,并且周期蛋白的降解具有高度特异性。在无细胞体系的第一个周期中,周期蛋白降解的起始、持续时间和程度以及周期蛋白A和周期蛋白B适当的阶段性消失都得到了正确调控。就像在完整细胞中一样,由早期间期细胞制成的裂解物需要进一步的蛋白质合成才能达到周期蛋白降解点,而由后期阶段制成的裂解物则不需要。利用无细胞体系我们发现周期蛋白的消失需要ATP和Mg2+。通过将来自不同细胞周期阶段的裂解物混合,我们发现:(a)间期裂解物不包含抑制周期蛋白降解的主要抑制剂;(b)周期蛋白降解的时间是由细胞质的细胞周期阶段决定的,而不是由底物周期蛋白本身的细胞周期阶段决定的。在测试的大量试剂中,只有少数会影响周期蛋白的降解。甲苯磺酰赖氨酸氯甲基酮(TLCK,一种蛋白酶抑制剂)、6-二甲基氨基嘌呤(6-DMAP,一种激酶抑制剂)、某些巯基阻断剂、ZnCl2和EDTA(但不是EGTA)能在体外完全阻断周期蛋白的降解。向无细胞体系中添加1 mM Ca2+对周期蛋白的稳定性没有影响,但5 mM Ca2+会导致周期蛋白和少量其他蛋白质的快速降解。

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