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Molecular Architecture of the Centriole Proteome: The Conserved WD40 Domain Protein POC1 Is Required for Centriole Duplication and Length Control

机译:中心蛋白质组的分子结构:中心复制和长度控制需要保守的WD40域蛋白POC1。

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摘要

Centrioles are intriguing cylindrical organelles composed of triplet microtubules. Proteomic data suggest that a large number of proteins besides tubulin are necessary for the formation and maintenance of a centriole's complex structure. Expansion of the preexisting centriole proteome from the green alga Chlamydomonas reinhardtii revealed additional human disease genes, emphasizing the significance of centrioles in normal human tissue homeostasis. We found that two classes of ciliary disease genes were highly represented among the basal body proteome: cystic kidney disease (especially nephronophthisis) syndromes, including Meckel/Joubert-like and oral-facial-digital syndrome, caused by mutations in CEP290, MKS1, OFD1, and AHI1/Jouberin proteins and cone-rod dystrophy syndrome genes, including UNC-119/HRG4, NPHP4, and RPGR1. We further characterized proteome of the centriole (POC) 1, a highly abundant WD40 domain-containing centriole protein. We found that POC1 is recruited to nascent procentrioles and localizes in a highly asymmetrical pattern in mature centrioles corresponding to sites of basal-body fiber attachment. Knockdown of POC1 in human cells caused a reduction in centriole duplication, whereas overexpression caused the appearance of elongated centriole-like structures. Together, these data suggest that POC1 is involved in early steps of centriole duplication as well as in the later steps of centriole length control.
机译:中心粒是由三重态微管组成的圆柱形细胞器。蛋白质组学数据表明,除了微管蛋白外,大量蛋白质对于中心粒复杂结构的形成和维持也是必需的。绿藻衣藻中已有的中心粒蛋白质组的扩增揭示了其他人类疾病基因,强调了中心粒在正常人体组织稳态中的重要性。我们发现在基础身体蛋白质组中高度代表了两种睫状疾病基因:囊性肾脏疾病(尤其是肾病)综合征,包括由CEP290,MKS1,OFD1突变引起的Meckel / Joubert样和口腔-面部数字综合征,AHI1 / Jouberin蛋白和视锥细胞营养不良综合征基因,包括UNC-119 / HRG4,NPHP4和RPGR1。我们进一步表征了蛋白质组的中心蛋白(POC)1,高度丰富的WD40域包含的中心蛋白。我们发现POC1被募集到新生的procentrioles,并在高度不对称的模式中定位在成熟的centrioles中,对应于基体纤维附着的位置。抑制人类细胞中的POC1导致了中心粒重复的减少,而过表达则导致了伸长的中心粒状结构的出现。总之,这些数据表明POC1参与了中心粒复制的早期步骤以及中心粒长度控制的后续步骤。

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