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Rifamycin congeners kanglemycins are active against rifampicin-resistant bacteria via a distinct mechanism.

Nat Commun. 2018; 
Peek J, Lilic M, Montiel D, Milshteyn A, Woodworth I, Biggins JB, Ternei MA, Calle PY, Danziger M, Warrier T, Saito K,, Braffman N, Fay A, Glickman MS, Darst SA, Campbell EA, Brady SF.
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Plasmid DNA Preparation Promoter DNA (−87 to +71 of Mtb rrnAP3)68 with an engineered mutation, +3 T > A, was synthesized (GenScript) and placed into the pUC57 plasmid to generate pUC57-AP3 GU. Get A Quote

摘要

Rifamycin antibiotics (Rifs) target bacterial RNA polymerases (RNAPs) and are widely used to treat infections including tuberculosis. The utility of these compounds is threatened by the increasing incidence of resistance (RifR). As resistance mechanisms found in clinical settings may also occur in natural environments, here we postulated that bacteria could have evolved to produce rifamycin congeners active against clinically relevant resistance phenotypes. We survey soil metagenomes and identify a tailoring enzyme-rich family of gene clusters encoding biosynthesis of rifamycin congeners (kanglemycins, Kangs) with potent in vivo and in vitro activity against the most common clinically relevant RifR mutations. O... More

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