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交联辅助空间蛋白质组学绘制亚细胞器蛋白质组和膜蛋白拓扑结构。

Cross-link assisted spatial proteomics to map sub-organelle proteomes and membrane protein topologies.

机构信息

Department of Structural Biology, Leibniz-Forschungsinstitut für Molekulare Pharmakologie (FMP), Robert-Roessle-Str. 10 13125, Berlin, Germany.

Department of Molecular Physiology and Cell Biology, Leibniz-Forschungsinstitut für Molekulare Pharmakologie (FMP), Robert-Roessle-Str. 10 13125, Berlin, Germany.

出版信息

Nat Commun. 2024 Apr 17;15(1):3290. doi: 10.1038/s41467-024-47569-x.

Abstract

The functions of cellular organelles and sub-compartments depend on their protein content, which can be characterized by spatial proteomics approaches. However, many spatial proteomics methods are limited in their ability to resolve organellar sub-compartments, profile multiple sub-compartments in parallel, and/or characterize membrane-associated proteomes. Here, we develop a cross-link assisted spatial proteomics (CLASP) strategy that addresses these shortcomings. Using human mitochondria as a model system, we show that CLASP can elucidate spatial proteomes of all mitochondrial sub-compartments and provide topological insight into the mitochondrial membrane proteome. Biochemical and imaging-based follow-up studies confirm that CLASP allows discovering mitochondria-associated proteins and revising previous protein sub-compartment localization and membrane topology data. We also validate the CLASP concept in synaptic vesicles, demonstrating its applicability to different sub-cellular compartments. This study extends the scope of cross-linking mass spectrometry beyond protein structure and interaction analysis towards spatial proteomics, and establishes a method for concomitant profiling of sub-organelle and membrane proteomes.

摘要

细胞器官和亚区的功能取决于其蛋白质含量,可以通过空间蛋白质组学方法来描述。然而,许多空间蛋白质组学方法在解析细胞器亚区、平行分析多个亚区以及/或描述膜相关蛋白质组方面存在局限性。在这里,我们开发了一种交联辅助空间蛋白质组学(CLASP)策略来解决这些缺点。我们用人线粒体作为模型系统,表明 CLASP 可以阐明所有线粒体亚区的空间蛋白质组,并提供对线粒体膜蛋白质组的拓扑见解。基于生化和成像的后续研究证实,CLASP 允许发现与线粒体相关的蛋白质,并修正以前的蛋白质亚区定位和膜拓扑数据。我们还在突触小泡中验证了 CLASP 概念,证明其适用于不同的亚细胞区室。这项研究将交联质谱的范围从蛋白质结构和相互作用分析扩展到空间蛋白质组学,并建立了一种同时分析亚细胞器和膜蛋白质组的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/33dd/11024108/4d97335e8f15/41467_2024_47569_Fig1_HTML.jpg

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