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对称型Mad2二聚体的晶体结构揭示了纺锤体检验点中Mad2调控的见解。

Insights into mad2 regulation in the spindle checkpoint revealed by the crystal structure of the symmetric mad2 dimer.

作者信息

Yang Maojun, Li Bing, Liu Chyong-Jy, Tomchick Diana R, Machius Mischa, Rizo Josep, Yu Hongtao, Luo Xuelian

机构信息

Department of Pharmacology, The University of Texas Southwestern Medical Center, Dallas, Texas, United States of America.

出版信息

PLoS Biol. 2008 Mar 4;6(3):e50. doi: 10.1371/journal.pbio.0060050.

Abstract

In response to misaligned sister chromatids during mitosis, the spindle checkpoint protein Mad2 inhibits the anaphase-promoting complex or cyclosome (APC/C) through binding to its mitotic activator Cdc20, thus delaying anaphase onset. Mad1, an upstream regulator of Mad2, forms a tight core complex with Mad2 and facilitates Mad2 binding to Cdc20. In the absence of its binding proteins, free Mad2 has two natively folded conformers, termed N1-Mad2/open-Mad2 (O-Mad2) and N2-Mad2/closed Mad2 (C-Mad2), with C-Mad2 being more active in APC/C(Cdc20) inhibition. Here, we show that whereas O-Mad2 is monomeric, C-Mad2 forms either symmetric C-Mad2-C-Mad2 (C-C) or asymmetric O-Mad2-C-Mad2 (O-C) dimers. We also report the crystal structure of the symmetric C-C Mad2 dimer, revealing the basis for the ability of unliganded C-Mad2, but not O-Mad2 or liganded C-Mad2, to form symmetric dimers. A Mad2 mutant that predominantly forms the C-C dimer is functional in vitro and in living cells. Finally, the Mad1-Mad2 core complex facilitates the conversion of O-Mad2 to C-Mad2 in vitro. Collectively, our results establish the existence of a symmetric Mad2 dimer and provide insights into Mad1-assisted conformational activation of Mad2 in the spindle checkpoint.

摘要

在有丝分裂过程中,为应对未对齐的姐妹染色单体,纺锤体检查点蛋白Mad2通过与有丝分裂激活因子Cdc20结合来抑制后期促进复合物或周期体(APC/C),从而延迟后期开始。Mad1是Mad2的上游调节因子,它与Mad2形成紧密的核心复合物,并促进Mad2与Cdc20的结合。在没有其结合蛋白的情况下,游离的Mad2有两种天然折叠构象,称为N1-Mad2/开放型Mad2(O-Mad2)和N2-Mad2/封闭型Mad2(C-Mad2),其中C-Mad2在抑制APC/C(Cdc20)方面更具活性。在这里,我们表明,O-Mad2是单体,而C-Mad2形成对称的C-Mad2-C-Mad2(C-C)或不对称的O-Mad2-C-Mad2(O-C)二聚体。我们还报告了对称C-C Mad2二聚体的晶体结构,揭示了未结合配体的C-Mad2而非O-Mad2或结合配体的C-Mad2形成对称二聚体的能力基础。一种主要形成C-C二聚体的Mad2突变体在体外和活细胞中都具有功能。最后,Mad1-Mad2核心复合物在体外促进O-Mad2向C-Mad2的转化。总的来说,我们的结果证实了对称Mad2二聚体的存在,并为纺锤体检查点中Mad1辅助的Mad2构象激活提供了见解。

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