| Literature DB >> 17159901 |
Kerstin Stingl1, Sonja Brandt, Eva-Maria Uhlemann, Roland Schmid, Karlheinz Altendorf, Carsten Zeilinger, Chantal Ecobichon, Agnès Labigne, Evert P Bakker, Hilde de Reuse.
Abstract
To date, the biological role of prokaryotic K(+) channels remains unknown. Helicobacter pylori contains a gene encoding a putative K(+) channel (HpKchA) of the two-transmembrane RCK (regulation of K(+) conductance) domain family, but lacks known bacterial K(+) uptake systems. A H. pylori DeltahpKchA mutant presented a strong growth defect at low K(+) concentration, which was compensated by KCl addition. The role of the separate RCK domain was investigated in H. pylori by mutagenesis of its internal start codon, which led to a K(+)-dependent intermediate growth phenotype, consistent with RCK activating channel function. Tagging HpKchA C-terminally, we detected a 1:1 stoichiometry of the full-length HpKchA and the separate RCK domain. We constructed single amino-acid exchanges within the unusual selectivity filter of HpKchA (ATGFGA) in H. pylori and observed complete loss (G74A), a slight defect (G76A or F75G) or wild-type (A77D) channel function. HpKchA was essential for colonization of the murine stomach. These data show, for the first time, a biological function for a prokaryotic K(+) channel, as a K(+) uptake system, essential for the persistence of H. pylori in the gastric environment.Entities:
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Year: 2006 PMID: 17159901 PMCID: PMC1782367 DOI: 10.1038/sj.emboj.7601471
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598