Affiliation:
1. Molecular Bio-computation and Drug Design Laboratory, School of Health Sciences, University of KwaZulu-Natal, Westville Campus, Durban 4001, South Africa
Abstract
Background:
The recent Nipah virus (NiV) outbreak in India has caused a state of chaos, with potential
to become the next international pandemic. There is still a great deal to learn about NiV for the development
of a potent treatment against it. The NiV non-structural proteins play important roles in the lifecycle of the virus,
with the RNA-dependent RNA-polymerase (RdRp) being a vital component in viral replication. In this study, we
not only provide a comprehensive overview of all the literature concerning NiV, we also propose a model of the
NiV RdRp and screen for potential inhibitors of the viral enzyme.
Objectives:
In this study, computational tools were utilized in the design of a NiV RdRp homology model. The
active site of RdRp was then identified and potential inhibitors of the protein were discovered with the use of
pharmacophore-based screening.
Methods:
In this study, computational tools were utilized in the design of a NiV RdRp homology model. The
active site of RdRp was then identified and potential inhibitors of the protein were discovered with the use of
pharmacophore-based screening.
Results:
Ramachandran plot analysis revealed a favourable model. Upon binding of nucleoside analog, 4’-
Azidocytidine, active site residues Trp1714 and Ser1713 took part in stabilizing hydrogen bonds, while Thr1716,
Ser1478, Ser1476 and Glu1465 contributed to hydrophobic interactions. Pharmacophore based screening yielded
18 hits, of which ZINC00085930 demonstrated the most optimal binding energy (-8.1 kcal/mol), validating its use
for further analysis as an inhibitor of NiV.
Conclusion:
In this study we provide a critical guide, elucidating on the in silico requirements of the drug design
and discovery process against NiV. This material lays a foundation for future research into the design and development
of drugs that inhibit NiV.
Publisher
Bentham Science Publishers Ltd.
Subject
Drug Discovery,Pharmacology
Cited by
1 articles.
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