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Plk4-dependent phosphorylation of STIL is required for centriole duplication

机译:中心粒复制需要STIL的Plk4依赖性磷酸化

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Duplication of centrioles, namely the formation of a procentriole next to the parental centriole, is regulated by the polo-like kinase Plk4. Only a few other proteins, including STIL (SCL/TAL1 interrupting locus, SIL) and Sas-6, are required for the early step of centriole biogenesis. Following Plk4 activation, STIL and Sas-6 accumulate at the cartwheel structure at the initial stage of the centriole assembly process. Here, we show that STIL interacts with Plk4 in vivo . A STIL fragment harboring both the coiled-coil domain and the STAN motif shows the strongest binding affinity to Plk4. Furthermore, we find that STIL is phosphorylated by Plk4. We identified Plk4-specific phosphorylation sites within the C-terminal domain of STIL and show that phosphorylation of STIL by Plk4 is required to trigger centriole duplication.
机译:马球样激酶Plk4调节着重心的复制,即在亲本着重心旁边形成一个着重心。中心粒生物发生的早期步骤仅需要一些其他蛋白质,包括STIL(SCL / TAL1中断基因座,SIL)和Sas-6。在Plk4激活后,STIL和Sas-6在中心粒组装过程的初始阶段积累在车轮结构上。在这里,我们显示STIL在体内与Plk4相互作用。同时包含卷曲螺旋结构域和STAN基序的STIL片段显示出对Plk4的最强结合亲和力。此外,我们发现STIL被Plk4磷酸化。我们在STIL的C末端域内鉴定了Plk4特异性的磷酸化位点,并表明通过Plk4进行STIL的磷酸化是触发中心粒重复的必要条件。

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