Homology modeling, molecular docking and electrostatic potential analysis of MurF ligase from Klebsiella pneumonia

Homology modeling, molecular docking and electrostatic potential analysis of MurF ligase from Klebsiella pneumonia

In spite of availability of moderately protective vaccine and antibiotics, new antibacterial agents are urgently needed to decrease the global incidence of Klebsiella pneumonia infections. MurF ligase, a key enzyme, which participates in the bacterial cell wall assembly, is indispensable to existenc...

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Veröffentlicht in:Bioinformation 2012-01, Vol.8 (10), p.466-473
Hauptverfasser: Sivaramakrishnan, Venkatabalasubramanian, Thiyagarajan, Chinnaiyan, Kalaivanan, Sivakumaran, Selvakumar, Raj, Anusuyadevi, Muthuswamy, Jayachandran, Kesavan Swaminathan
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Desmodium
Eubacteria
Hypothesis
Klebsiella
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container_end_page 473
container_issue 10
container_start_page 466
container_title Bioinformation
container_volume 8
creator Sivaramakrishnan, Venkatabalasubramanian
Thiyagarajan, Chinnaiyan
Kalaivanan, Sivakumaran
Selvakumar, Raj
Anusuyadevi, Muthuswamy
Jayachandran, Kesavan Swaminathan
description In spite of availability of moderately protective vaccine and antibiotics, new antibacterial agents are urgently needed to decrease the global incidence of Klebsiella pneumonia infections. MurF ligase, a key enzyme, which participates in the bacterial cell wall assembly, is indispensable to existence of K. pneumonia. MurF ligase lack mammalian vis-à-vis and have high specificity, uniqueness, and occurrence only in eubacteria, epitomizing them as promising therapeutic targets for intervention. In this study, we present a unified approach involving homology modeling and molecular docking studies on MurF ligase enzyme. As part of this study, a homology model of K. pneumonia (MurF ligase) enzyme was predicted for the first time in order to carry out structurebased drug design. The accuracy of the model was further validated using different computational approaches. The comparative molecular docking study on this enzyme was undertaken using different phyto-ligands from Desmodium sp. and a known antibiotic Ciprofloxacin. The docking analysis indicated the importance of hotspots (HIS 281 and ASN 282) within the MurF binding pocket. The Lipinski's rule of five was analyzed for all ligands considered for this study by calculating the ADME/Tox, drug likeliness using Qikprop simulation. Only ten ligands were found to comply with the Lipinski rule of five. Based on the molecular docking results and Lipinki values 6-Methyltetrapterol A was confirmed as a promising lead compound. The present study should therefore play a guiding role in the experimental design and development of 6-Methyltetrapterol A as a bactericidal agent.
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The Lipinski's rule of five was analyzed for all ligands considered for this study by calculating the ADME/Tox, drug likeliness using Qikprop simulation. Only ten ligands were found to comply with the Lipinski rule of five. Based on the molecular docking results and Lipinki values 6-Methyltetrapterol A was confirmed as a promising lead compound. 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subjects Desmodium
Eubacteria
Hypothesis
Klebsiella
title Homology modeling, molecular docking and electrostatic potential analysis of MurF ligase from Klebsiella pneumonia
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