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Current Computer-Aided Drug Design

Editor-in-Chief

ISSN (Print): 1573-4099
ISSN (Online): 1875-6697

Water Molecules Increases Binding Affinity of Natural PI3Kγ Inhibitors Against Cancer

Author(s): Pooja Sharma, Aparna Shukla, Komal Kalani, Vijaya Dubey, Santosh Kumar Srivastava, Suaib Luqman and Feroz Khan

Volume 11, Issue 4, 2015

Page: [304 - 320] Pages: 17

DOI: 10.2174/1573409912666151124233847

Price: $65

Abstract

The PI3K pathway is a signal transduction process including oncogenes and receptor tyrosine kinase regulating cellular functions i.e., survival, protein synthesis, and metabolism. In the present work, we have investigated the role of water molecules on inhibitor’s binding orientation in crystal structures of PI3K pathway targets using molecular docking approach. AutoDock v4.2 docking software was employed to dock PI3Kγ and its known inhibitors viz., wortmannin, quercetin, myricetin and pyridyl-triazine. Besides, serpentine was also docked on the same binding pocket, subsequently its anticancer activity was evaluated through in vitro experiment. Docking studies have been performed in the presence as well as in absence of water molecules at the binding pocket, and results were compared with crystallographic structural data. The comparison was done on the basis of binding energy, RMSD, inhibition constant (Ki), conserved and bridging water molecules, and found that, while considering water molecules during docking experiments, it increases the binding affinity of PI3K inhibitors.

Keywords: PI3K, phosphoinositide-3-kinase, docking, water, AutoDock, wortmannin, quercetin, myricetin.


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