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A fragment-based approach towards the discovery of N-substituted tropinones as inhibitors of Mycobacterium tuberculosis transcriptional regulator EthR2.

Eur J Med Chem. 2019; 
PrevetHugues,MouneMartin,TaninaAbdalkarim,KemmerChristian,HerledanAdrien,FritaRosangela,Wohlk?nigAlexandre,BourotteMarilyne,VillemagneBaptiste,LerouxFlorence,GitzingerMarc,BaulardAlain R,DéprezBenoit,WintjensRené,WillandNicolas,FlipoMa
Products/Services Used Details Operation
ORF cDNA Clones/MolecularCloud The resulting ORF was sequence optimized for expression in human/mouse, synthesized (Genscript) and introduced into pSEAP2-control (Clontech) using EcoRI/XbaI to generate the expression vector pCK289 (PSV40-EthR2-VP16-HA-pA). Get A Quote

摘要

Tuberculosis (TB) caused by the pathogen Mycobacterium tuberculosis, represents one of the most challenging threat to public health worldwide, and with the increasing resistance to approved TB drugs, it is needed to develop new strategies to address this issue. Ethionamide is one of the most widely used drugs for the treatment of multidrug-resistant TB. It is a prodrug that requires activation by mycobacterial monooxygenases to inhibit the enoyl-ACP reductase InhA, which is involved in mycolic acid biosynthesis. Very recently, we identified that inhibition of a transcriptional repressor, termed EthR2, derepresses a new bioactivation pathway that results in the boosting of ethionamide activation. H... More

关键词

EthR2,Ethionamide,Fragment-based drug design,Tropinone,Tubercul