Kinetic Analyses of the Siderophore Biosynthesis Inhibitor Salicyl-AMS and Analogues as MbtA Inhibitors and Antimycobacterial Agents

Kinetic Analyses of the Siderophore Biosynthesis Inhibitor Salicyl-AMS and Analogues as MbtA Inhibitors and Antimycobacterial Agents

There is a paramount need for expanding the drug armamentarium to counter the growing problem of drug-resistant tuberculosis. Salicyl-AMS, an inhibitor of salicylic acid adenylation enzymes, is a first-in-class antibacterial lead compound for the development of tuberculosis drugs targeting the biosy...

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Veröffentlicht in:Biochemistry (Easton) 2019-02, Vol.58 (6), p.833-847
Hauptverfasser: Bythrow, Glennon V, Mohandas, Poornima, Guney, Tezcan, Standke, Lisa C, Germain, Gabrielle A, Lu, Xuequan, Ji, Cheng, Levendosky, Keith, Chavadi, Sivagami Sundaram, Tan, Derek S, Quadri, Luis E. N
Format: Artikel
Sprache:eng
Schlagworte:
Adenosine - analogs & derivatives
Adenosine - chemistry
Adenosine - metabolism
Adenosine - pharmacology
Antitubercular Agents - chemistry
Antitubercular Agents - metabolism
Antitubercular Agents - pharmacology
Bacillus subtilis - enzymology
Drug Design
Escherichia coli - genetics
Kinetics
Ligases - antagonists & inhibitors
Ligases - chemistry
Ligases - metabolism
Microbial Sensitivity Tests
Molecular Structure
Mycobacterium smegmatis - drug effects
Mycobacterium tuberculosis - drug effects
Protein Binding
Siderophores - chemistry
Siderophores - metabolism
Siderophores - pharmacology
Structure-Activity Relationship
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Zusammenfassung:There is a paramount need for expanding the drug armamentarium to counter the growing problem of drug-resistant tuberculosis. Salicyl-AMS, an inhibitor of salicylic acid adenylation enzymes, is a first-in-class antibacterial lead compound for the development of tuberculosis drugs targeting the biosynthesis of salicylic-acid-derived siderophores. In this study, we determined the K i of salicyl-AMS for inhibition of the salicylic acid adenylation enzyme MbtA from Mycobacterium tuberculosis (MbtAtb), designed and synthesized two new salicyl-AMS analogues to probe structure–activity relationships (SAR), and characterized these two analogues alongside salicyl-AMS and six previously reported analogues in biochemical and cell-based studies. The biochemical studies included determination of kinetic parameters (K i app, k on app, k off, and t R) and analysis of the mechanism of inhibition. For these studies, we optimized production and purification of recombinant MbtAtb, for which K m and k cat values were determined, and used the enzyme in conjunction with an MbtAtb-optimized, continuous, spectrophotometric assay for MbtA activity and inhibition. The cell-based studies provided an assessment of the antimycobacterial activity and postantibiotic effect of the nine MbtAtb inhibitors. The antimycobacterial properties were evaluated using a strain of nonpathogenic, fast-growing Mycobacterium smegmatis that was genetically engineered for MbtAtb-dependent susceptibility to MbtA inhibitors. This convenient model system greatly facilitated the cell-based studies by bypassing the methodological complexities associated with the use of pathogenic, slow-growing M. tuberculosis. Collectively, these studies provide new information on the mechanism of inhibition of MbtAtb by salicyl-AMS and eight analogues, afford new SAR insights for these inhibitors, and highlight several suitable candidates for future preclinical evaluation.
ISSN:0006-2960
1520-4995
DOI:10.1021/acs.biochem.8b01153