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Gyrase ATPase Domain as an Antitubercular Drug Discovery Platform: Structure‐Based Design and Lead Optimization of Nitrothiazolyl Carboxamide Analogues |
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| Authors: | Variam Ullas Jeankumar Janupally Renuka Sonali Kotagiri Shalini Saxena Shruti Singh Kakan Jonnalagadda Padma Sridevi Swapna Yellanki Pushkar Kulkarni Prof. Perumal Yogeeswari Prof. Dharmarajan Sriram |
| Affiliation: | 1. Department of Pharmacy, Birla Institute of Technology & Science Pilani, Hyderabad Campus, Shameerpet, R.R. District, Hyderabad 500078, Andhra Pradesh (India);2. Dr. Reddy's Institute of Life Sciences, University of Hyderabad Campus, Gachibowli, Hyderabad 500046 (India);3. Zephase Therapeutics (an incubated company at Dr. Reddy's Institute of Life Sciences), University of Hyderabad Campus, Gachibowli, Hyderabad 500046 (India) |
| Abstract: | In this study, we explored the pharmaceutically underexploited mycobacterial gyrase ATPase (GyrB) domain as a template for a structure‐based virtual screening of our in‐house (BITS Pilani) compound collection to discover new inhibitors targeting Mycobacterium tuberculosis (M.tb.) The hit identified was further customized by using a combination of molecular docking and medicinal chemistry strategies to obtain an optimized analogue displaying considerable in vitro enzyme efficacy and bactericidal properties against the M.tb. H37Rv strain. The binding affinity of the ligand toward the GyrB domain was reascertained by differential scanning fluorimetry experiments. Further evaluation of the hERG toxicity (a major limitation among the previously reported N‐linked aminopiperidine analogues) indicated these molecules to be completely devoid of cardiotoxicity, a significant achievement within this class. |
| Keywords: | DNA gyrase enzymes inhibitors tuberculosis virtual screening |