Impact of Na+ -translocating NADH:quinone oxidoreductase (NQR) on iron uptake and nqrM expression in Vibrio cholerae  [23.11.19]

The Na+ -translocating NADH:quinone oxidoreductase (NQR) generates an electrochemical Na+ gradient in vivo which is crucial for expulsion of bactericidal drugs by secondary efflux systems. Moreover, this respiratory Na+ pump is the major catabolic NADH dehydrogenase required for the regeneration of NAD+. Electrons are delivered to ubiquinone (Q) which is reduced to ubiquinol (QH2), a substrate for downstream respiratory complexes.

Abstract

The Na⁺ - ion translocating NADH:quinone oxidoreductase (NQR) from Vibrio cholerae is a membrane bound respiratory enzyme which harbors flavins and Fe-S clusters as redox centers. The NQR is the main producer of sodium motive force (SMF) and drives energy-dissipating processes such as flagellar rotation, substrate uptake, ATP synthesis and cation-proton antiport. The NQR requires for its maturation besides the six structural genes, nqrABCDEF, a flavin attachment gene encoded by apbE and the nqrM gene, presumably a Fe delivery protein. We here describe growth studies and quantitative real time PCR for the V. cholerae O395N1 strain wildtype (wt) and its mutant strains, Δnqr and ΔubiC, impaired in respiration. In a comparative proteome analysis, FeoB, the membrane subunit of the uptake system for Fe²⁺ (Feo), was increased in V. cholerae Δnqr In this study, the upregulation is confirmed on the mRNA level, and results in improved growth rates of V. cholerae Δnqr with Fe²⁺ as iron source. We studied the expression of feoB on other respiratory enzyme deletion mutants like ΔubiC to identify if iron transport was specific to the absence of NQR resulted from impaired respiration. We show that the nqr operon comprises, besides the structural nqrABCDEF genes, the downstream apbE and nqrM genes on the same operon, and demonstrate induction of the nqr operon by iron in V. cholerae wt. In contrast, expression of the nqrM gene in V. cholerae Δnqr is repressed by iron. The lack of functional NQR has a strong impact on iron homeostasis in V. cholerae, and exemplifies that central respiratory metabolism is interwoven with iron uptake and regulation.Importance Investigating strategies of iron acquisition, storage and delivery in Vibrio cholerae is a prerequisite to understand how this pathogen thrives in hostile, iron-limited environments such as the human host. Besides highlighting the maturation of the respiratory complex NQR, this study points out the influence of NQR on iron metabolism thereby making it a potential drug target for antibiotics.

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