Scientific Reports (Jan 2018)

Unanticipated functional diversity among the TatA-type components of the Tat protein translocase

  • Ekaterina Eimer,
  • Wei-Chun Kao,
  • Julia Fröbel,
  • Anne-Sophie Blümmel,
  • Carola Hunte,
  • Matthias Müller

DOI
https://doi.org/10.1038/s41598-018-19640-3
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 12

Abstract

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Abstract Twin-arginine translocation (Tat) systems transport folded proteins that harbor a conserved arginine pair in their signal peptides. They assemble from hexahelical TatC-type and single-spanning TatA-type proteins. Many Tat systems comprise two functionally diverse, TatA-type proteins, denominated TatA and TatB. Some bacteria in addition express TatE, which thus far has been characterized as a functional surrogate of TatA. For the Tat system of Escherichia coli we demonstrate here that different from TatA but rather like TatB, TatE contacts a Tat signal peptide independently of the proton-motive force and restricts the premature processing of a Tat signal peptide. Furthermore, TatE embarks at the transmembrane helix five of TatC where it becomes so closely spaced to TatB that both proteins can be covalently linked by a zero-space cross-linker. Our results suggest that in addition to TatB and TatC, TatE is a further component of the Tat substrate receptor complex. Consistent with TatE being an autonomous TatAB-type protein, a bioinformatics analysis revealed a relatively broad distribution of the tatE gene in bacterial phyla and highlighted unique protein sequence features of TatE orthologs.