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Proteomic analysis of multiple primary cilia reveals a novel mode of ciliary development in mammals

机译:多个原发纤毛的蛋白质组学分析揭示了哺乳动物纤毛发育的新模式

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Cilia are structurally and functionally diverse organelles, whose malfunction leads to ciliopathies. While recent studies have uncovered common ciliary transport mechanisms, limited information is available on the proteome of cilia, particularly that of sensory subtypes, which could provide insight into their functional and developmental diversities. In the present study, we performed proteomic analysis of unique, multiple 9+0 cilia in choroid plexus epithelial cells (CPECs). The analysis of juvenile swine CPEC cilia identified 868 proteins. Among them, 396 were shared with the proteome of 9+0 photoreceptor cilia (outer segment), whereas only 152 were shared with the proteome of 9+2 cilia and flagella. Various signaling molecules were enriched in a CPEC-specific ciliome subset, implicating multiplicity of sensory functions. The ciliome also included molecules for ciliary motility such as Rsph9. In CPECs from juvenile swine or adult mouse, Rsph9 was localized to a subpopulation of cilia, whereas they were non-motile. Live imaging of mouse choroid plexus revealed that neonatal CPEC cilia could beat vigorously, and the motility waned and was lost within 1–2 weeks. The beating characteristics of neonatal CPEC cilia were variable and different from those of typical 9+2 cilia of ependyma, yet an Efhc1-mediated mechanism to regulate the beating frequency was shared in both types of cilia. Notably, ultrastructural analysis revealed the presence of not only 9+0 but also 9+2 and atypical ciliary subtypes in neonatal CPEC. Overall, these results identified both conserved and variable components of sensory cilia, and demonstrated a novel mode of ciliary development in mammals.
机译:纤毛是结构和功能各异的细胞器,其功能失常会导致纤毛病。尽管最近的研究发现了常见的纤毛运输机制,但是关于纤毛蛋白质组的信息有限,尤其是感觉亚型的蛋白质组,这可以提供对其功能和发育多样性的见识。在本研究中,我们对脉络丛上皮细胞(CPEC)中独特的多个9 + 0纤毛进行了蛋白质组学分析。幼猪CPEC纤毛的分析鉴定出868种蛋白质。其中,396 +与9 + 0感光体纤毛(外节)的蛋白质组共有,而只有152与9 + 2纤毛和鞭毛的蛋白质组共有。各种信号分子富集于CPEC特有的纤毛虫亚群中,涉及多种感觉功能。纤毛虫还包括用于纤毛运动的分子,例如Rsph9。在来自幼猪或成年小鼠的CPEC中,Rsph9定位于纤毛亚群,而它们不活动。小鼠脉络丛的实时成像显示,新生的CPEC纤毛可以剧烈跳动,运动能力减弱并在1-2周内消失。新生儿CPEC纤毛的跳动特征是可变的,并且不同于典型的9 + 2室管膜纤毛,但两种纤毛都有Efhc1介导的调节跳动频率的机制。值得注意的是,超微结构分析显示,新生儿CPEC中不仅存在9 + 0,而且存在9 + 2和非典型睫状亚型。总体而言,这些结果确定了感觉纤毛的保守和可变组成部分,并证明了哺乳动物纤毛发育的新模式。

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