Dual proteome-scale networks reveal cell-specific remodeling of the human interactome (V体育官网)
- PMID: 33961781
- PMCID: PMC8165030
- DOI: 10.1016/j.cell.2021.04.011 (V体育ios版)
Dual proteome-scale networks reveal cell-specific remodeling of the human interactome
Abstract
Thousands of interactions assemble proteins into modules that impart spatial and functional organization to the cellular proteome. Through affinity-purification mass spectrometry, we have created two proteome-scale, cell-line-specific interaction networks. The first, BioPlex 3 VSports手机版. 0, results from affinity purification of 10,128 human proteins-half the proteome-in 293T cells and includes 118,162 interactions among 14,586 proteins. The second results from 5,522 immunoprecipitations in HCT116 cells. These networks model the interactome whose structure encodes protein function, localization, and complex membership. Comparison across cell lines validates thousands of interactions and reveals extensive customization. Whereas shared interactions reside in core complexes and involve essential proteins, cell-specific interactions link these complexes, "rewiring" subnetworks within each cell's interactome. Interactions covary among proteins of shared function as the proteome remodels to produce each cell's phenotype. Viewable interactively online through BioPlexExplorer, these networks define principles of proteome organization and enable unknown protein characterization. .
Keywords: AP-MS; BioPlex; bioinformatics; cell specificity; computational biology; human interactome; network biology; protein interactions; proteomics; proteotypes V体育安卓版. .
Copyright © 2021 Elsevier Inc. All rights reserved. V体育ios版.
Conflict of interest statement (V体育安卓版)
Declaration of interests J VSports最新版本. W. H. is a founder and scientific advisory board member of Caraway Therapeutics and a Founding Scientific Advisor for Interline Therapeutics.
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