Alternate quinone coupling in a new class of succinate dehydrogenase may potentiate mycobacterial respiratory control

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Abstract

There is a paucity of information on the unique components that pathogens use to form respiratory chains. It is not known why mycobacteria encode multiple succinate dehydrogenases (SDHs) to perform menaquinone-linked succinate oxidation, a thermodynamically unfavorable reaction (ΔG° = +21 kJ·mol−1). In other bacteria, specific di-heme SDHs overcome this using the proton motive force. It is unknown if this holds true in mycobacteria. Here, succinate dehydrogenase 1 (Sdh1) from Mycobacterium smegmatis was purified and found to not contain heme cofactors. Proteoliposomes, containing Sdh1, are active with coenzyme Q2 (Km ~ 12 μm), are competitively inhibited by menaquinone (Ki ~ 25 μm) and do not generate or consume electrochemical gradients. Sdh1 may use higher potential quinones in vivo and forms a novel SDH class, which we term ‘Type F’.

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CITATION STYLE

APA

Hards, K., Rodriguez, S. M., Cairns, C., & Cook, G. M. (2019). Alternate quinone coupling in a new class of succinate dehydrogenase may potentiate mycobacterial respiratory control. FEBS Letters, 593(5), 475–486. https://doi.org/10.1002/1873-3468.13330

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