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Identification of a substrate domain that determines system specificity in mycobacterial type VII secretion systems. | LitMetric

Identification of a substrate domain that determines system specificity in mycobacterial type VII secretion systems.

Sci Rep

Section Molecular Microbiology, Amsterdam Institute of Molecules, Medicines &Systems, Vrije Universiteit Amsterdam, Amsterdam, The Netherlands.

Published: February 2017

AI Article Synopsis

  • Type VII secretion (T7S) systems are essential for mycobacterial pathogens to move virulence factors across their tough cell membrane, with five different systems (ESX-1 to ESX-5) identified.
  • The T7S substrates typically include a specific secretion motif (YxxxD/E), but this does not dictate which T7S system they belong to; instead, the binding domain recognized by the EspG chaperone plays a crucial role in system specificity.
  • Experiments showed that altering the EspG-binding domain in ESX-1 substrates disrupted their secretion, and swapping it with the EspG-binding domain from the ESX-5 substrate led to their rerouting to the ESX-5

Article Abstract

Type VII secretion (T7S) systems are specialized machineries used by mycobacterial pathogens to transport important virulence factors across their highly hydrophobic cell envelope. There are up to five mycobacterial T7S systems, named ESX-1 to ESX-5, at least three of which specifically secrete a different subset of substrates. The T7S substrates or substrate complexes are defined by the general secretion motif YxxxD/E. However this motif does not determine system specificity. Here, we show that the substrate domain recognized by the EspG chaperone is the determinant factor for this specificity. We first show that the introduction of point mutations into the EspG-binding domain of the ESX-1 substrate pair PE35/PPE68_1 affects their secretion. Subsequently, we demonstrate that replacing this domain by the EspG-binding domain of the ESX-5 substrate PPE18 resulted in EspG dependence and exclusive rerouting to the ESX-5 system. This rerouting of PE35/PPE68_1 to the ESX-5 system had a negative effect on the secretion of endogenous ESX-5 substrates.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5311947PMC
http://dx.doi.org/10.1038/srep42704DOI Listing

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