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Bioinformatics
Using a drug repurposing strategy to virtually screen potential HIV-1 entry inhibitors that block the NHR domain of the viral envelope protein gp41
A. M. Andrianova, Ya. V. Laykovb, A. V. Tuzikovb a Institute of Bioorganic Chemistry, National Academy of Sciences of Belarus, Minsk, Belarus
b United Institute of Informatics Problems, National Academy of Sciences of Belarus, Minsk, Belarus
Abstract:
Using a drug repurposing strategy, virtual screening of potential inhibitors of the NHR domain of the HIV-1 gp41 protein, a conserved region critical for the virus-cell membrane fusion and viral infectivity, was carried out. The used computational approach included: (1) molecular docking of this functionally significant region of the HIV-1 envelope with compounds from a library of bioactive molecules containing clinically approved drugs, experimental drugs, and investigational drug candidates; (2) assessing the binding affinity of these compounds to the therapeutic target; (3) molecular dynamics simulations of ligand/NHR-gp41 complexes; (4) calculations of the binding free energy followed by the analysis of molecular dynamics trajectories and selection of compounds promising to test for anti-HIV-1 activity. As a result, six compounds that exhibited the high binding affinity to the NHR domain of the HIV-1 gp41 protein and showed acceptable pharmacological properties were identified. The predicted compounds are assumed to form a promising basis for the development of new, effective and safe broad-spectrum antiviral agents able to inhibit the HIV-1 entry into the host cell.
Key words:
HIV-1, protein gp41, domain NHR, virtual screening, molecular docking, molecular dynamics, anti-HIV drugs.
Received 01.02.2024, 26.03.2024, Published 02.04.2024
Citation:
A. M. Andrianov, Ya. V. Laykov, A. V. Tuzikov, “Using a drug repurposing strategy to virtually screen potential HIV-1 entry inhibitors that block the NHR domain of the viral envelope protein gp41”, Mat. Biolog. Bioinform., 19:1 (2024), 77–95
Linking options:
https://www.mathnet.ru/eng/mbb549 https://www.mathnet.ru/eng/mbb/v19/i1/p77
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Abstract page: | 34 | Full-text PDF : | 21 | References: | 1 |
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