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

Nat Commun.. 2019; 
Beites T1, O'Brien K1, Tiwari D1, Engelhart CA1, Walters S1,2, Andrews J3, Yang HJ3, Sutphen ML3, Weiner DM3, Dayao EK3, Zimmerman M4, Prideaux B4, Desai PV5, Masquelin T5, Via LE3,6, Dartois V4, Boshoff HI3, Barry CE 3rd3,6, Ehrt S1, Schnappinger D7.
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Gene Synthesis The complemented strain was obtained by introducing ndh under the control of a strong promoter (pGMCtSq19-0×-Puv15-ndh) at the tweety phage attachment site. For complementation with LbNOX, a codon usage adapted gene (lbnoxMtb) was ordered from GenScript and cloned into an integrative plasmid (pGMCgS-0×-Ptb38-LbNOX-FLAG-SD1) that inserts at the Giles Get A Quote

摘要

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 growt... More

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