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首页> 外文期刊>Human Molecular Genetics >CEP290 interacts with the centriolar satellite component PCM-1 and is required for Rab8 localization to the primary cilium.
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CEP290 interacts with the centriolar satellite component PCM-1 and is required for Rab8 localization to the primary cilium.

机译:CEP290与星状卫星组件PCM-1相互作用,是Rab8定位到初级纤毛的必需条件。

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摘要

Joubert syndrome (JS) is a developmental brain disorder characterized by cerebellar vermis hypoplasia, abnormal eye movement, ataxia and mental retardation. Mutations in CEP290 mutations are responsible for the cerebello-oculo-renal subtype of JS that includes kidney cysts and retinal degeneration, two phenotypes commonly linked to ciliopathies. CEP290 mutations are also associated with Meckel-Gruber syndrome and Bardet-Biedl syndrome (BBS). Here we demonstrate that CEP290 interacts with a centriolar satellite protein PCM-1, which is implicated in BBS4 function. CEP290 binds to PCM-1 and localizes to centriolar satellites in a PCM-1- and microtubule-dependent manner. The depletion of CEP290 disrupts subcellular distribution and protein complex formation of PCM-1. In accord with PCM-1's role in microtubule organization, CEP290 knockdown causes the disorganization of the cytoplasmic microtubule network. Moreover, we show that both CEP290 and PCM-1 are required for ciliogenesis and are involved in the ciliary targeting of Rab8, a small GTPase shown to collaborate with BBS protein complex to promote ciliogenesis. Our results suggest that PCM-1 is a potential mediator that may link CEP290 with BBS proteins in common molecular pathways.
机译:Joubert综合征(JS)是一种发展性脑部疾病,其特征是小脑ver部发育不全,眼球运动异常,共济失调和智力低下。 CEP290突变的突变是JS的小脑-眼-肾亚型的原因,其中包括肾囊肿和视网膜变性,这两种表型通常与纤毛病相关。 CEP290突变也与Meckel-Gruber综合征和Bardet-Biedl综合征(BBS)相关。在这里,我们证明CEP290与中心星状卫星蛋白PCM-1相互作用,这与BBS4功能有关。 CEP290结合PCM-1并以依赖PCM-1和微管的方式定位于中心粒状卫星。 CEP290的消耗破坏了PCM-1的亚细胞分布和蛋白质复合物的形成。与PCM-1在微管组织中的作用一致,CEP290敲低导致细胞质微管网络的混乱。此外,我们显示CEP290和PCM-1都是睫毛发生所必需的,并且参与了Rab8的纤毛靶向,Rab8是一种小GTP酶,可与BBS蛋白复合体协同促进纤毛发生。我们的结果表明,PCM-1是一种潜在的介体,可以将CEP290与BBS蛋白连接到常见的分子途径。

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