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Functional design of bacterial superoxide:quinone oxidoreductase. | LitMetric

Functional design of bacterial superoxide:quinone oxidoreductase.

Biochim Biophys Acta Bioenerg

Department of Chemistry, Biochemistry and Pharmaceutical Sciences, University of Bern, 3012 Bern, Switzerland. Electronic address:

Published: October 2022

AI Article Synopsis

  • The superoxide anion, created when molecular oxygen gains an electron, is produced in large quantities and has various roles in cellular functions, including immune response and signaling.
  • Superoxide can lead to harmful compounds like hydroxyl anions, so it's crucial for cells to have mechanisms to neutralize it, which include enzymes like superoxide dismutase and the newly studied cytochrome b (CybB) from E. coli.
  • Research shows that CybB can effectively use superoxide and quinones as substrates, accelerating their reactions, which may indicate its significant physiological roles alongside other cytochrome b proteins.

Article Abstract

The superoxide anion - molecular oxygen reduced by a single electron - is produced in large amounts by enzymatic and adventitious reactions. It can perform a range of cellular functions, including bacterial warfare and iron uptake, signalling and host immune response in eukaryotes. However, it also serves as precursor for more deleterious species such as the hydroxyl anion or peroxynitrite and defense mechanisms to neutralize superoxide are important for cellular health. In addition to the soluble proteins superoxide dismutase and superoxide reductase, recently the membrane embedded diheme cytochrome b (CybB) from E. coli has been proposed to act as a superoxide:quinone oxidoreductase. Here, we confirm superoxide and cellular ubiquinones or menaquinones as natural substrates and show that quinone binding to the enzyme accelerates the reaction with superoxide. The reactivity of the substrates is in accordance with the here determined midpoint potentials of the two b hemes (+48 and -23 mV / NHE). Our data suggest that the enzyme can work near the diffusion limit in the forward direction and can also catalyse the reverse reaction efficiently under physiological conditions. The data is discussed in the context of described cytochrome b proteins and potential physiological roles of CybB.

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Source
http://dx.doi.org/10.1016/j.bbabio.2022.148583DOI Listing

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