Plasticity of the Mycobacterium tuberculosis respiratory chain and its impact on tuberculosis drug development

Author:

Beites TiagoORCID,O’Brien Kathryn,Tiwari DivyaORCID,Engelhart Curtis A.ORCID,Walters Shaun,Andrews Jenna,Yang Hee-Jeong,Sutphen Michelle L.,Weiner Danielle M.,Dayao Emmanuel K.,Zimmerman Matthew,Prideaux Brendan,Desai Prashant V.,Masquelin Thierry,Via Laura E.,Dartois Véronique,Boshoff Helena I.ORCID,Barry Clifton E.ORCID,Ehrt SabineORCID,Schnappinger Dirk

Abstract

Abstract The viability of Mycobacterium tuberculosis (Mtb) depends on energy generated by its respiratory chain. Cytochrome bc1-aa3 oxidase and type-2 NADH dehydrogenase (NDH-2) are respiratory chain components predicted to be essential, and are currently targeted for drug development. Here we demonstrate that an Mtb cytochrome bc1-aa3 oxidase deletion mutant is viable and only partially attenuated in mice. Moreover, treatment of Mtb-infected marmosets with a cytochrome bc1-aa3 oxidase inhibitor controls disease progression and reduces lesion-associated inflammation, but most lesions become cavitary. Deletion of both NDH-2 encoding genes (Δndh-2 mutant) reveals that the essentiality of NDH-2 as shown in standard growth media is due to the presence of fatty acids. The Δndh-2 mutant is only mildly attenuated in mice and not differently susceptible to clofazimine, a drug in clinical use proposed to engage NDH-2. These results demonstrate the intrinsic plasticity of Mtb’s respiratory chain, and highlight the challenges associated with targeting the pathogen’s respiratory enzymes for tuberculosis drug development.

Funder

Bill and Melinda Gates Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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