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Novel asymmetrically localizing components of human centrosomes identified by complementary proteomics methods

机译:通过互补蛋白质组学方法鉴定的人中心体的新型不对称定位成分

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摘要

Centrosomes in animal cells are dynamic organelles with a proteinaceous matrix of pericentriolar material assembled around a pair of centrioles. They organize the microtubule cytoskeleton and the mitotic spindle apparatus. Mature centrioles are essential for biogenesis of primary cilia that mediate key signalling events. Despite recent advances, the molecular basis for the plethora of processes coordinated by centrosomes is not fully understood. We have combined protein identification and localization, using PCP-SILAC mass spectrometry, BAC transgeneOmics, and antibodies to define the constituents of human centrosomes. From a background of non-specific proteins, we distinguished 126 known and 40 candidate centrosomal proteins, of which 22 were confirmed as novel components. An antibody screen covering 4000 genes revealed an additional 113 candidates. We illustrate the power of our methods by identifying a novel set of five proteins preferentially associated with mother or daughter centrioles, comprising genes implicated in cell polarity. Pulsed labelling demonstrates a remarkable variation in the stability of centrosomal protein complexes. These spatiotemporal proteomics data provide leads to the further functional characterization of centrosomal proteins.
机译:动物细胞中的中心体是动态细胞器,其周围围绕着一对中心粒,聚集了中心粒周围物质的蛋白质基质。他们组织微管细胞骨架和有丝分裂纺锤体。成熟的中心粒对于介导关键信号事件的原发性纤毛的生物发生至关重要。尽管有最近的进展,但由中心体协调的过多过程的分子基础尚未完全了解。我们结合了蛋白质鉴定和定位,使用PCP-SILAC质谱,BAC转基因组学和抗体来定义人中心体的成分。从非特异性蛋白质的背景,我们区分了126种已知和40种候选中心体蛋白,其中22种被确认为新组分。覆盖4000个基因的抗体筛选揭示了另外113个候选基因。我们通过鉴定一组优先与母或子中心体相关的五种蛋白质的新组合来说明我们方法的功效,这些蛋白质包括与细胞极性有关的基因。脉冲标记显示出中心体蛋白复合物稳定性的显着变化。这些时空蛋白质组学数据提供了中心体蛋白的进一步功能表征。

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