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相互作用蛋白质组学鉴定 NEURL4 和 HECT E3 连接酶 HERC2 为中心体结构的新型调节剂。

Interaction proteomics identify NEURL4 and the HECT E3 ligase HERC2 as novel modulators of centrosome architecture.

机构信息

Samuel Lunenfeld Research Institute, Mount Sinai Hospital, Toronto, Ontario M5G 1X5, Canada.

出版信息

Mol Cell Proteomics. 2012 Jun;11(6):M111.014233. doi: 10.1074/mcp.M111.014233. Epub 2012 Jan 19.

Abstract

Centrosomes are composed of a centriole pair surrounded by an intricate proteinaceous matrix referred to as pericentriolar material. Although the mechanisms underpinning the control of centriole duplication are now well understood, we know relatively little about the control of centrosome size and shape. Here we used interaction proteomics to identify the E3 ligase HERC2 and the neuralized homologue NEURL4 as novel interaction partners of the centrosomal protein CP110. Using high resolution imaging, we find that HERC2 and NEURL4 localize to the centrosome and that interfering with their function alters centrosome morphology through the appearance of aberrant filamentous structures that stain for a subset of pericentriolar material proteins including pericentrin and CEP135. Using an RNA interference-resistant transgene approach in combination with structure-function analyses, we show that the association between CP110 and HERC2 depends on nonoverlapping regions of NEURL4. Whereas CP110 binding to NEURL4 is dispensable for the regulation of pericentriolar material architecture, its association with HERC2 is required to maintain normal centrosome integrity. NEURL4 is a substrate of HERC2, and together these results indicate that the NEURL4-HERC2 complex participates in the ubiquitin-dependent regulation of centrosome architecture.

摘要

中心体由一对中心粒组成,周围是一种复杂的蛋白质基质,称为中心粒周围物质。尽管控制中心粒复制的机制现在已经被很好地理解,但我们对控制中心体大小和形状的机制知之甚少。在这里,我们使用相互作用蛋白质组学来鉴定 E3 连接酶 HERC2 和神经化同源物 NEURL4 作为中心体蛋白 CP110 的新的相互作用伙伴。使用高分辨率成像,我们发现 HERC2 和 NEURL4 定位于中心体,并且干扰它们的功能通过出现异常丝状结构来改变中心体形态,这些丝状结构染色包括中心粒蛋白和 CEP135 在内的一组中心粒周围物质蛋白。使用 RNA 干扰抗性转基因方法结合结构-功能分析,我们表明 CP110 与 HERC2 之间的关联取决于 NEURL4 的非重叠区域。虽然 CP110 与 NEURL4 的结合对于调节中心粒周围物质结构不是必需的,但它与 HERC2 的关联对于维持正常的中心体完整性是必需的。NEURL4 是 HERC2 的底物,这些结果表明 NEURL4-HERC2 复合物参与了中心体结构的泛素依赖性调节。

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