The unusual extended signal peptide region of the type V secretion system is phylogenetically restricted

Mickael Desvaux, Lisa Cooper-Charles, NA Filenko, Anthony Scott-Tucker, Susan Turner, Jeffrey Cole, Ian Henderson

Research output: Contribution to journalArticle

34 Citations (Scopus)

Abstract

The plasmid encoded toxin, Pet, is a prototypical member of the serine protease autotransporters of the Enterobacteriaceae. In addition to the passenger and beta-domains typical of autotransporters, in silico predictions indicate that Pet possesses an unusually long N-terminal signal sequence. The signal sequence can be divided into five regions termed N1 (charged), H1 (hydrophobic), N2, H2 and C (cleavage site) domains. The N1 and H1 regions, which we have termed the extended signal peptide region, demonstrate remarkable conservation. In contrast, the N2, H2 and C regions demonstrate significant variability and are reminiscent of typical Sec-dependent signal sequences. Despite several investigations, the function of the extended signal peptide region remains obscure and surprisingly it has not been proven that the extended signal peptide region is actually synthesized as part of the signal sequence. Here, we demonstrate that the extended signal peptide region is present only in Gram-negative bacterial proteins originating from the classes Beta- and Gammaproteobacteria, and more particularly only in proteins secreted via the Type V secretion pathway: autotransporters, TpsA exoproteins of the two-partner system and trimeric autotransporters. In vitro approaches demonstrate that the DNA region encoding the extended signal peptide region is transcribed and translated.
Original languageEnglish
Pages (from-to)22-30
Number of pages9
JournalFEMS Microbiology Letters
Volume264
DOIs
Publication statusPublished - 1 Nov 2006

Keywords

  • sec
  • inner membrane
  • two-partner secretion
  • autotransporter
  • type V secretion

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