Author: Vogels, Mijke W.; van Balkom, Bas W. M.; Heck, Albert J. R.; de Haan, Cornelis A. M.; Rottier, Peter J. M.; Batenburg, Joseph J.; Kaloyanova, Dora V.; Helms, J. Bernd
Title: Quantitative proteomic identification of host factors involved in the Salmonella typhimurium infection cycle Cord-id: ewe4k0m9 Document date: 2011_10_28
ID: ewe4k0m9
Snippet: To identify host factors involved in Salmonella replication, SILACâ€based quantitative proteomics was used to investigate the interactions of Salmonella typhimurium with the secretory pathway in human epithelial cells. Protein profiles of Golgiâ€enriched fractions isolated from S. typhimuriumâ€infected cells were compared with those of mockâ€infected cells, revealing significant depletion or enrichment of 105 proteins. Proteins annotated to play a role in membrane traffic were overrepresente
Document: To identify host factors involved in Salmonella replication, SILACâ€based quantitative proteomics was used to investigate the interactions of Salmonella typhimurium with the secretory pathway in human epithelial cells. Protein profiles of Golgiâ€enriched fractions isolated from S. typhimuriumâ€infected cells were compared with those of mockâ€infected cells, revealing significant depletion or enrichment of 105 proteins. Proteins annotated to play a role in membrane traffic were overrepresented among the depleted proteins whereas proteins annotated to the cytoskeleton showed a diverse behavior with some proteins being enriched, others being depleted from the Golgi fraction upon Salmonella infection. To study the functional relevance of identified proteins in the Salmonella infection cycle, small interfering RNA (siRNA) experiments were performed. siRNAâ€mediated depletion of a selection of affected proteins identified five host factors involved in Salmonella infection. Depletion of peroxiredoxinâ€6 (PRDX6), isoform βâ€4c of integrin βâ€4 (ITGB4), isoform 1 of protein lap2 (erbin interacting protein; ERBB2IP), stomatin (STOM) or TBC domain containing protein 10b (TBC1D10B) resulted in increased Salmonella replication. Surprisingly, in addition to the effect on Salmonella replication, depletion of STOM or ITGB4 resulted in a dispersal of intracellular Salmonella microcolonies. It can be concluded that by using SILACâ€based quantitative proteomics we were able to identify novel host cell proteins involved in the complex interplay between Salmonella and epithelial cells.
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