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Engineering another class of anti-tubercular lead: Hit to lead optimization of an intriguing class of gyrase ATPase inhibitors.

Author
Abstract
:

A structure based medium throughput virtual screening campaign of BITS-Pilani in house chemical library to identify novel binders of Mycobacterium tuberculosis gyrase ATPase domain led to the discovery of a quinoline scaffold. Further medicinal chemistry explorations on the right hand core of the early hit, engendered a potent lead demonstrating superior efficacy both in the enzyme and whole cell screening assay. The binding affinity shown at the enzyme level was further corroborated by biophysical characterization techniques. Early pharmacokinetic evaluation of the optimized analogue was encouraging and provides interesting potential for further optimization.

Year of Publication
:
2016
Journal
:
European journal of medicinal chemistry
Volume
:
122
Number of Pages
:
216-231
Date Published
:
2016
ISSN Number
:
0223-5234
URL
:
https://linkinghub.elsevier.com/retrieve/pii/S0223-5234(16)30532-3
DOI
:
10.1016/j.ejmech.2016.06.042
Short Title
:
Eur J Med Chem
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