Title of article
Bisubstrate Adenylation Inhibitors of Biotin Protein Ligase from Mycobacterium tuberculosis Original Research Article
Author/Authors
Benjamin P. Duckworth، نويسنده , , Todd W. Geders، نويسنده , , Divya Tiwari، نويسنده , , Helena I. Boshoff، نويسنده , , Paul A. Sibbald، نويسنده , , Clifton E. Barry III، نويسنده , , Dirk Schnappinger، نويسنده , , Barry C. Finzel، نويسنده , , Courtney C. Aldrich، نويسنده ,
Issue Information
ماهنامه با شماره پیاپی سال 2011
Pages
10
From page
1432
To page
1441
Abstract
The mycobacterial biotin protein ligase (MtBPL) globally regulates lipid metabolism in Mtb through the posttranslational biotinylation of acyl coenzyme A carboxylases involved in lipid biosynthesis that catalyze the first step in fatty acid biosynthesis and pyruvate coenzyme A carboxylase, a gluconeogenic enzyme vital for lipid catabolism. Here we describe the design, development, and evaluation of a rationally designed bisubstrate inhibitor of MtBPL. This inhibitor displays potent subnanomolar enzyme inhibition and antitubercular activity against multidrug resistant and extensively drug resistant Mtb strains. We show that the inhibitor decreases in vivo protein biotinylation of key enzymes involved in fatty acid biosynthesis and that the antibacterial activity is MtBPL dependent. Additionally, the gene encoding BPL was found to be essential in M. smegmatis. Finally, the X-ray cocrystal structure of inhibitor bound MtBPL was solved providing detailed insight for further structure-activity analysis. Collectively, these data suggest that MtBPL is a promising target for further antitubercular therapeutic development.
Journal title
Chemistry and Biology
Serial Year
2011
Journal title
Chemistry and Biology
Record number
1160162
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