Literature DB >> 23530225

Substrate selectivity in glutamate-dependent acid resistance in enteric bacteria.

Ming-Feng Tsai1, Patrick McCarthy, Christopher Miller.   

Abstract

The bacterial antiporter GadC plays a central role in the glutamate (Glu)-dependent acid resistance system, which protects enteric bacteria against the extreme acidity of the human stomach. Upon acid shock, GadC imports Glu into the cytoplasm, where Glu decarboxylases consume a cytoplasmic proton, which ends up as a "virtual" proton in the decarboxylated product γ-aminobutyric acid (GABA) and is then exported via GadC. It was therefore proposed that GadC counters intracellular acidification by continually pumping out virtual protons. This scenario, however, is oversimplified. In gastric environments, GadC encounters substrates in multiple carboxyl protonation forms (outside: Glu(-), Glu(0), Glu(+); inside: GABA(0), GABA(+)). Of the six possible combinations of antiport partners, Glu(+)/GABA(0) results in proton influx, Glu(0)/GABA(0) and Glu(+)/GABA(+) are proton neutral, and Glu(-)/GABA(0), Glu(-)/GABA(+), or Glu(0)/GABA(+) lead to proton extrusion. Which of these exchanges does GadC catalyze? To attack this problem, we developed an oriented GadC liposome system holding a three-unit inward pH gradient to mimic the conditions facing bacteria in the stomach. By assessing the electrogenicity of substrate transport, we demonstrate that GadC selectively exchanges Glu(-) or Glu(0) with GABA(+), resulting in effective proton extrusion of >0.9 H(+) per turnover to counter proton invasion into acid-challenged bacteria. We further show that GadC selects among protonated substrates using a charge-based mechanism, rather than directly recognizing the protonation status of the carboxyl groups. This result paves the way for future work to identify the molecular basis of GadC's substrate selectivity.

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Year:  2013        PMID: 23530225      PMCID: PMC3625338          DOI: 10.1073/pnas.1301444110

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  10 in total

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Authors:  Dan Ma; Peilong Lu; Chuangye Yan; Chao Fan; Ping Yin; Jiawei Wang; Yigong Shi
Journal:  Nature       Date:  2012-03-11       Impact factor: 49.962

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4.  On the use of thiol-modifying agents to determine channel topology.

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5.  Glutamate decarboxylase-dependent acid resistance in orally acquired bacteria: function, distribution and biomedical implications of the gadBC operon.

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Authors:  M P Castanie-Cornet; T A Penfound; D Smith; J F Elliott; J W Foster
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9.  Substrate selectivity in arginine-dependent acid resistance in enteric bacteria.

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Journal:  Proc Natl Acad Sci U S A       Date:  2013-03-25       Impact factor: 11.205

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  10 in total
  23 in total

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5.  Substrate selectivity in arginine-dependent acid resistance in enteric bacteria.

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Journal:  Proc Natl Acad Sci U S A       Date:  2013-03-25       Impact factor: 11.205

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8.  Biochemical and spectroscopic properties of Brucella microti glutamate decarboxylase, a key component of the glutamate-dependent acid resistance system.

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