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Sardiu ME, et al.  (2009) Determining protein complex connectivity using a probabilistic deletion network derived from quantitative proteomics. PLoS One 4(10):e7310

Abstract: Protein complexes are key molecular machines executing a variety of essential cellular processes. Despite the availability of genome-wide protein-protein interaction studies, determining the connectivity between proteins within a complex remains a major challenge. Here we demonstrate a method that is able to predict the relationship of proteins within a stable protein complex. We employed a combination of computational approaches and a systematic collection of quantitative proteomics data from wild-type and deletion strain purifications to build a quantitative deletion-interaction network map and subsequently convert the resulting data into an interdependency-interaction model of a complex. We applied this approach to a data set generated from components of the Saccharomyces cerevisiae Rpd3 histone deacetylase complexes, which consists of two distinct small and large complexes that are held together by a module consisting of Rpd3, Sin3 and Ume1. The resulting representation reveals new protein-protein interactions and new submodule relationships, providing novel information for mapping the functional organization of a complex.

Status: Published Type: Journal Article | Research Support, N.I.H., Extramural | Research Support, Non-U.S. Gov't PubMed ID: 19806189

Topics addressed in this paper

Number of different genes curated to this paper: 19

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Topics Topics not linked to Genes Genes linked to topics (#1 - 10 )
ASH1 BMH1 CTI6 DEP1 DOT6 EAF3 HHT2 KAP95 PHO23 RCO1
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Computational analysis yg ball
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Omics yg ball
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Topics Genes linked to topics (#11 - 19 )
RPD3 RXT2 RXT3 SAP30 SDS3 SIN3 SRP1 UME1 UME6
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Function/Process blue ball
Large-scale protein interaction blue ball blue ball blue ball
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Primary Literature blue ball blue ball blue ball
Protein-protein Interactions blue ball blue ball blue ball blue ball blue ball blue ball blue ball blue ball blue ball
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