生存素与染色体区域维护蛋白1的相互作用对于染色体乘客复合体的定位和功能至关重要。
The Survivin-Crm1 interaction is essential for chromosomal passenger complex localization and function.
作者信息
Knauer Shirley K, Bier Carolin, Habtemichael Negusse, Stauber Roland H
机构信息
Georg-Speyer-Haus, Paul-Ehrlich-Strasse 42-44, Frankfurt D-60596, Germany.
出版信息
EMBO Rep. 2006 Dec;7(12):1259-65. doi: 10.1038/sj.embor.7400824. Epub 2006 Nov 10.
Abstract
The chromosomal passenger complex (CPC) of Aurora-B, Borealin, INCENP (inner centromere protein) and Survivin coordinates essential chromosomal and cytoskeletal events during mitosis. Here, we show that the nuclear export receptor Crm1 is crucially involved in tethering the CPC to the centromere by interacting with a leucine-rich nuclear export signal (NES), evolutionarily conserved in all mammalian Survivin proteins. We show that inhibition of the Survivin-Crm1 interaction by treatment with leptomycin B or by RNA-interference-mediated Crm1 depletion prevents centromeric targeting of Survivin. The genetic inactivation of the Survivin-Crm1 interaction by mutation of the NES affects the correct localization and function of Survivin and the CPC during mitosis. By contrast, CPC assembly does not seem to require the Survivin-Crm1 interaction. Our report shows the functional significance of the Survivin-Crm1 interface and provides a novel link between the mitotic effector Crm1 and the CPC.
摘要
由极光激酶B、Borealin、内着丝粒蛋白(INCENP)和生存素组成的染色体乘客复合体(CPC)在有丝分裂过程中协调重要的染色体和细胞骨架事件。在此,我们表明核输出受体Crm1通过与富含亮氨酸的核输出信号(NES)相互作用,在将CPC拴系到着丝粒上发挥关键作用,该信号在所有哺乳动物生存素蛋白中具有进化保守性。我们发现,通过使用雷帕霉素B处理或RNA干扰介导的Crm1缺失来抑制生存素与Crm1的相互作用,可阻止生存素的着丝粒靶向定位。通过NES突变对生存素与Crm1相互作用进行基因失活,会影响有丝分裂期间生存素和CPC的正确定位及功能。相比之下,CPC组装似乎并不需要生存素与Crm1的相互作用。我们的报告展示了生存素与Crm1界面的功能重要性,并在有丝分裂效应因子Crm1和CPC之间建立了新的联系。
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