4.5 Article

Intermolecular cross-linking of monomers in Helicobacter pylori Na+/H+ antiporter NhaA at the dimer interface inhibits antiporter activity

Journal

BIOCHEMICAL JOURNAL
Volume 426, Issue -, Pages 99-108

Publisher

PORTLAND PRESS LTD
DOI: 10.1042/BJ20091339

Keywords

Blue-native PAGE (BN-PAGE); cross-link; dimerization; fluorescence resonance energy transfer (FRET); Helicobacter pylori; Na+/H+ antiporter

Funding

  1. Japanese Ministry of Education, Science, Sports, Technology and Culture

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We have previously shown that HPNhaA (Helicobacter pylori Na+/H+ antiporter) forms ail oligomer in a native membrane of Escherichia coli, and conformational changes of oligomer occur between monomers of the oligomer during ion transport. In the present study, we use Blue-native PAGE to show that HPNhaA ;forms a dimer. Cysteine-scanning mutagenesis of residues 5561 in a putative beta-sheet region of loop1 and subsequent functional analyses revealed that the Q58C mutation resulted in ail intermolecular disulfide bond. G56C, 159C and G60C Were found to be cross-linked by bifunctional cross-linkers. Furthermore, the Q58E mutant did not form a dinner, possibly Clue to electrostatic repulsion between monomers. These results imply that Gln-58 and the flanking sequence In the putative beta-sheet of the monomer are located close to the identical residues in the dimer. The Q58C mutant of NhaA was almost inactive under non-reducing conditions, and activity was restored Unden reducing conditions. This result showed that cross-linking at the dimer interface reduces transporter activity by interfering with the flexible association between the monomers. A mutant HPNhaA protein with three amino acid Substitutions at residues 57-59 did not form a dimer. and yet was active. indicating that the monomer is functional.

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