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SAS-6 卷曲螺旋结构及其与 SAS-5 的相互作用提示了线虫中心体组装中的一种调控机制。

SAS-6 coiled-coil structure and interaction with SAS-5 suggest a regulatory mechanism in C. elegans centriole assembly.

机构信息

Max F Perutz Laboratories, Medical University of Vienna, Vienna, Austria.

出版信息

EMBO J. 2012 Nov 14;31(22):4334-47. doi: 10.1038/emboj.2012.280. Epub 2012 Oct 12.

Abstract

The centriole is a conserved microtubule-based organelle essential for both centrosome formation and cilium biogenesis. Five conserved proteins for centriole duplication have been identified. Two of them, SAS-5 and SAS-6, physically interact with each other and are codependent for their targeting to procentrioles. However, it remains unclear how these two proteins interact at the molecular level. Here, we demonstrate that the short SAS-5 C-terminal domain (residues 390-404) specifically binds to a narrow central region (residues 275-288) of the SAS-6 coiled coil. This was supported by the crystal structure of the SAS-6 coiled-coil domain (CCD), which, together with mutagenesis studies, indicated that the association is mediated by synergistic hydrophobic and electrostatic interactions. The crystal structure also shows a periodic charge pattern along the SAS-6 CCD, which gives rise to an anti-parallel tetramer. Overall, our findings establish the molecular basis of the specific interaction between SAS-5 and SAS-6, and suggest that both proteins individually adopt an oligomeric conformation that is disrupted upon the formation of the hetero-complex to facilitate the correct assembly of the nine-fold symmetric centriole.

摘要

中心粒是一种保守的微管细胞器,对于中心体的形成和纤毛发生都是必不可少的。已经鉴定出五种与中心粒复制相关的保守蛋白。其中两种,SAS-5 和 SAS-6,相互物理相互作用,并且它们的靶向到前中心粒是相互依赖的。然而,这些两种蛋白在分子水平上如何相互作用仍不清楚。在这里,我们证明短的 SAS-5 C 端结构域(残基 390-404)特异性地结合到 SAS-6 卷曲螺旋的狭窄中心区域(残基 275-288)。这得到了 SAS-6 卷曲螺旋结构域(CCD)的晶体结构的支持,该结构域与突变研究一起表明,这种关联是由协同的疏水和静电相互作用介导的。晶体结构还显示了 SAS-6 CCD 上沿的周期性电荷模式,这导致了反平行四聚体。总的来说,我们的研究结果确定了 SAS-5 和 SAS-6 之间特异性相互作用的分子基础,并表明这两种蛋白单独采用寡聚构象,当形成异源复合物时,这种构象被破坏,以促进九倍对称的中心粒的正确组装。

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