Dengue fever has been a global health concern. Mitigation is a challenging problem due to non-availability of workable treatments. The most difficult objective is to design a perfect anti-dengue agent capable of inhibiting infections caused by all four serotypes. Various tactics have been employed in the past to discover dengue antivirals, including screening of chemical compounds against dengue virus enzymes. The objective of the current study is to investigate phytocompounds as anti-dengue remedies that target the non-structural 2B and non-structural 3 protease (NS2B-NS3(pro)), a possible therapeutic target for dengue fever. Initially, 300â+âantiviral phytocompounds were collected from Duke's phytochemical and ethnobotanical database and 30 phytocompounds with anti-dengue properties were identified from previously reported studies, which were virtually screened against NS2B-NS3(pro) using molecular docking and toxicity evaluation. The top five most screened ligands were naringin, hesperidin, gossypol, maslinic acid and rhodiolin with binding affinities ofâ-â8.7Â kcal/mol,â-â8.5Â kcal/mol,â-â8.5Â kcal/mol,â-â8.5Â kcal/mol andâ-â8.1Â kcal/mol, respectively. The finest docked compounds complexed with NS2B-NS3(pro) were subjected for molecular dynamics (MD) simulations and binding free energy estimations through molecular mechanics generalized born surface area-based calculations. The results of the study are intriguing in the context of computer-aided screening and the binding affinities of the phytocompounds, proposing maslinic acid (MAS) as a potent bioactive antiviral for the development of phytocompound-based anti-dengue agent.
Targeting the DENV NS2B-NS3 protease with active antiviral phytocompounds: structure-based virtual screening, molecular docking and molecular dynamics simulation studies.
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作者:Purohit Priyanka, Sahoo Sthitaprajna, Panda Madhusmita, Sahoo Partha Sarathi, Meher Biswa Ranjan
| 期刊: | Journal of Molecular Modeling | 影响因子: | 2.500 |
| 时间: | 2022 | 起止号: | 2022 Oct 24; 28(11):365 |
| doi: | 10.1007/s00894-022-05355-w | ||
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