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Proteomic mapping of cytosol-facing outer mitochondrial and ER membranes in living human cells by proximity biotinylation

机译:通过邻近生物素化对活体人细胞中面向细胞溶质的外线粒体和ER膜的蛋白质组学作图

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摘要

The cytosol-facing membranes of cellular organelles contain proteins that enable signal transduction, regulation of morphology and trafficking, protein import and export, and other specialized processes. Discovery of these proteins by traditional biochemical fractionation can be plagued with contaminants and loss of key components. Using peroxidase-mediated proximity biotinylation, we captured and identified endogenous proteins on the outer mitochondrial membrane (OMM) and endoplasmic reticulum membrane (ERM) of living human fibroblasts. The proteomes of 137 and 634 proteins, respectively, are highly specific and highlight 94 potentially novel mitochondrial or ER proteins. Dataset intersection identified protein candidates potentially localized to mitochondria-ER contact sites. We found that one candidate, the tail-anchored, PDZ-domain-containing OMM protein SYNJ2BP, dramatically increases mitochondrial contacts with rough ER when overexpressed. Immunoprecipitation-mass spectrometry identified ribosome-binding protein 1 (RRBP1) as SYNJ2BP’s ERM binding partner. Our results highlight the power of proximity biotinylation to yield insights into the molecular composition and function of intracellular membranes.
机译:细胞器面向细胞质的膜包含蛋白质,这些蛋白质能够进行信号转导,形态和运输调节,蛋白质进出口以及其他专门过程。通过传统的生化分级分离发现这些蛋白质可能会受到污染物和关键成分损失的困扰。使用过氧化物酶介导的邻近生物素化,我们捕获并鉴定了活人成纤维细胞的线粒体外膜(OMM)和内质网膜(ERM)上的内源性蛋白质。 137和634蛋白的蛋白质组分别具有高度特异性,突出了94种潜在的新型线粒体或ER蛋白。数据集交叉点确定了可能定位于线粒体-ER接触位点的蛋白质候选物。我们发现,一种候选蛋白,即尾部锚定的,含PDZ域的OMM蛋白SYNJ2BP,在过表达时会大大增加线粒体与粗糙ER的接触。免疫沉淀质谱法鉴定出核糖体结合蛋白1(RRBP1)是SYNJ2BP的ERM结合伴侣。我们的结果强调了近距离生物素化的能力,可深入了解细胞内膜的分子组成和功能。

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