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Spatial and proteomic profiling reveals centrosome‐independent features of centriolar satellites

机译:空间和蛋白质组分析揭示了星状卫星的不依赖于中心体的特征

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摘要

Centriolar satellites are small electron‐dense granules that cluster in the vicinity of centrosomes. Satellites have been implicated in multiple critical cellular functions including centriole duplication, centrosome maturation, and ciliogenesis, but their precise composition and assembly properties have remained poorly explored. Here, we perform in vivo proximity‐dependent biotin identification (BioID) on 22 human satellite proteins, to identify 2,113 high‐confidence interactions among 660 unique polypeptides. Mining this network, we validate six additional satellite components. Analysis of the satellite interactome, combined with subdiffraction imaging, reveals the existence of multiple unique microscopically resolvable satellite populations that display distinct protein interaction profiles. We further show that loss of satellites in PCM1‐depleted cells results in a dramatic change in the satellite interaction landscape. Finally, we demonstrate that satellite composition is largely unaffected by centriole depletion or disruption of microtubules, indicating that satellite assembly is centrosome‐independent. Together, our work offers the first systematic spatial and proteomic profiling of human centriolar satellites and paves the way for future studies aimed at better understanding the biogenesis and function(s) of these enigmatic structures.
机译:中心卫星是聚集在中心体附近的小的电子致密颗粒。卫星与多种关键的细胞功能有关,包括中心粒复制,中心体成熟和纤毛发生,但对它们的精确组成和组装特性的研究仍很少。在这里,我们对22种人类卫星蛋白进行了体内邻近依赖性生物素鉴定(BioID),以鉴定660种独特多肽之间的2,113个高可信度相互作用。挖掘该网络,我们验证了六个附加卫星组件。对卫星相互作用组的分析与亚衍射成像相结合,揭示了存在多个独特的可显微分辨的卫星种群,这些种群显示出不同的蛋白质相互作用曲线。我们进一步表明,丢失PCM1的单元中的卫星丢失会导致卫星交互作用格局发生巨大变化。最后,我们证明了卫星组成在很大程度上不受中心粒耗竭或微管破坏的影响,这表明卫星组装是独立于中心体的。在一起,我们的工作提供了人类中心粒卫星的第一个系统的空间和蛋白质组分析,并为将来的研究铺平了道路,旨在更好地了解这些神秘结构的生物发生和功能。

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