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The kinase domain of CK1 enzymes contains the localization cue essential for compartmentalized signaling at the spindle pole

机译:CK1酶的激酶结构域包含在主轴杆上的划分信号传导的定位提示

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CK1 protein kinases contribute to multiple biological processes, but how they are tailored to function in compartmentalized signaling events is largely unknown. Hhp1 and Hhp2 (Hhp1/2) are the soluble CK1 family members in Schizosaccharomyces pombe. One of their functions is to inhibit the septation initiation network (SIN) during a mitotic checkpoint arrest. The SIN is assembled by Sid4 at spindle pole bodies (SPBs), and though Hhp1/2 colocalize there, it is not known how they are targeted there or whether their SPB localization is required for SIN inhibition. Here, we establish that Hhp1/2 localize throughout the cell cycle to SPBs, as well as to the nucleus, cell tips, and division site. We find that their catalytic domains but not their enzymatic function are used for SPB targeting and that this targeting strategy is conserved in human CK1d/e localization to centrosomes. Further, we pinpoint amino acids in the Hhp1 catalytic domain required for SPB interaction; mutation of these residues disrupts Hhp1 association with the core SPB protein Ppc89, and the inhibition of cytokinesis in the setting of spindle stress. Taken together, these data have enabled us to define a molecular mechanism used by CK1 enzymes to target a specific cellular locale for compartmentalized signaling.
机译:CK1蛋白激酶有助于多种生物过程,但它们如何在划分的信号传导事件中定制以在很大程度上未知。 HHP1和HHP2(HHP1 / 2)是Schizosaccharomyces Pombe中可溶性CK1家族成员。其中一个功能是在有丝分裂检查点骤停期间抑制荚膜发起网络(SIN)。 SIN由SID4组装在主轴杆体(SPB),虽然HHP1 / 2在那里结合,但尚不知道它们是如何在那里定向的,或者是否需要他们的SPB定位。在这里,我们在整个细胞周期中确定HHP1 / 2将整个细胞周期定位为SPB,以及核,细胞提示和分裂部位。我们发现它们的催化结构域但不是它们的酶促功能用于SPB靶向,并且该靶向策略在人类CK1D / E本地中保存到Centrosomes。此外,我们在SPB相互作用所需的HHP1催化结构域中定位氨基酸;这些残留物的突变破坏了与核心SPB蛋白PPC89的HHP1关联,以及在主轴应力的设置中抑制细胞因子。总之,这些数据使我们能够定义CK1酶使用的分子机制,以针对分隔型信号传导靶向特定的蜂窝区域环境。

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