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Intracellular accumulation of high levels of γ-aminobutyrate by Listeria monocytogenes 10403S in response to low pH: Uncoupling of γ-aminobutyrate synthesis from efflux in a chemically defined medium

  • Kimon Andreas G. Karatzas
  • , Orla Brennan
  • , Sinéad Heavin
  • , John Morrissey
  • , Conor P. O'Byrne
  • University of Galway

Research output: Contribution to journalArticlepeer-review

Abstract

It is well established that the glutamate decarboxylase (GAD) system is central to the survival of Listeria monocytogenes at low pH, both in acidic foods and within the mammalian stomach. The accepted model proposes that under acidic conditions extracellular glutamate is transported into the cell in exchange for an intracellular γ-aminobutyrate (GABA1). The glutamate is then decarboxylated to GABA1, a reaction that consumes a proton, thereby helping to prevent acidification of the cytoplasm. In this study, we show that glutamate supplementation had no influence on either growth rate at pH 5.0 or survival at pH 2.5 when L. monocytogenes 10403S was grown in a chemically defined medium (DM), In response to acidification, cells grown in DM failed to efflux GABA, even when glutamate was added to the medium. In contrast, in brain heart infusion (BHI), the same strain produced significant extracellular GABA (GABAe) in response to acidification. In addition, high levels Of GABAi (>80 mM) were found in the cytoplasm in response to low pH in both growth media. Medium-swap and medium-mixing experiments revealed that the GABA efflux apparatus was nonfunctional in DM, even when glutamate was present. It was also found that the GadT2D2 antiporter/decarboxylase system was transcribed poorly in DM-grown cultures while overexpression of gadDlTl and gadD3 occurred in response to pH 3.5. Interestingly, BHI-grown cells did not respond with upregulation of any of the GAD system genes when challenged at pH 3.5. The accumulation of GABAi in cells grown in DM in the absence of extracellular glutamate indicates that intracellular glutamate is the source of the GABA1. These results demonstrate that GABA production can be uncoupled from GABA efflux, a finding that alters the way we should view the operation of bacterial GAD systems.

Original languageEnglish
Pages (from-to)3529-3537
Number of pages9
JournalApplied and Environmental Microbiology
Volume76
Issue number11
DOIs
Publication statusPublished - Jun 2010

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