Xanthates: Metabolism by Flavoprotein-Containing Monooxygenases and Antimycobacterial Activity.

Drug Metab Dispos

Department of Drug Toxicology, Institute of Neurobiology (S.G.Y., T.D.S.), and Institute of Microbiology (V.V.V.), Bulgarian Academy of Sciences, Sofia, Bulgaria; and Department of Pharmaceutical Chemistry, University of California, San Francisco, California (P.R.O.M.).

Published: August 2018

Ethionamide (ETH) plays a central role in the treatment of tuberculosis in patients resistant to the first-line drugs. The ETH, thioamide, and thiourea class of antituberculosis agents are prodrugs that are oxidatively converted to their active -oxides by the mycobacterial flavin-dependent monooxygenase (EtaA) of , thus initiating the chain of reactions that result in inhibition of mycolic acid biosynthesis and cell lysis. As part of a search for new lead candidates, we report here that several xanthates are oxidized by purified EtaA to -oxide metabolites (perxanthates), which are implicated in the antimycobacterial activity of these compounds. This process, which is analogous to that responsible for activation of ETH, is also catalyzed by human flavoprotein monooxygenase 3. EtaA was not inhibited in a time-dependent manner during the reaction. Xanthates with longer alkyl chains were oxidized more efficiently. EtaA oxidized octyl-xanthate ( = 5 M; = 1.023 nmolP/min; = 5.2 molP/min/molE) more efficiently than ETH (194 M; 1.46 nmolP/min; 7.73 nmolP/min/molE, respectively). Furthermore, the in vitro antimycobacterial activity of four xanthates against H37Hv was higher (minimum inhibitory concentration of around 1 M) than that of ETH (12 M).

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6034259PMC
http://dx.doi.org/10.1124/dmd.118.081984DOI Listing

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