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Merck
  • Proteomic characterization of the whole secretome of Legionella pneumophila and functional analysis of outer membrane vesicles.

Proteomic characterization of the whole secretome of Legionella pneumophila and functional analysis of outer membrane vesicles.

Infection and immunity (2008-02-06)
Frank Galka, Sun Nyunt Wai, Harald Kusch, Susanne Engelmann, Michael Hecker, Bernd Schmeck, Stefan Hippenstiel, Bernt Eric Uhlin, Michael Steinert
摘要

Secretion of effector molecules is one of the major mechanisms by which the intracellular human pathogen Legionella pneumophila interacts with host cells during infection. Specific secretion machineries which are responsible for the subfraction of secreted proteins (soluble supernatant proteins [SSPs]) and the production of bacterial outer membrane vesicles (OMVs) both contribute to the protein composition of the extracellular milieu of this lung pathogen. Here we present comprehensive proteome reference maps for both SSPs and OMVs. Protein identification and assignment analyses revealed a total of 181 supernatant proteins, 107 of which were specific to the SSP fraction and 33 of which were specific to OMVs. A functional classification showed that a large proportion of the identified OMV proteins are involved in the pathogenesis of Legionnaires' disease. Zymography and enzyme assays demonstrated that the SSP and OMV fractions possess proteolytic and lipolytic enzyme activities which may contribute to the destruction of the alveolar lining during infection. Furthermore, it was shown that OMVs do not kill host cells but specifically modulate their cytokine response. Binding of immunofluorescently stained OMVs to alveolar epithelial cells, as visualized by confocal laser scanning microscopy, suggested that there is delivery of a large and complex group of proteins and lipids in the infected tissue in association with OMVs. On the basis of these new findings, we discuss the relevance of protein sorting and compartmentalization of virulence factors, as well as environmental aspects of the vesicle-mediated secretion.

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Sigma-Aldrich
明胶 来源于牛皮, Type B, powder, BioReagent, suitable for cell culture
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明胶 来源于牛皮, gel strength ~225 g Bloom, Type B
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明胶 来源于牛皮, Type B
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弹性蛋白-刚果红, elastase substrate