Is the conformational flexibility of piperazine derivatives important to inhibit HIV-1 replication?

•The binding mode of piperazine derivatives with HIV-1 gp120 was predicted.•Impact of their conformational flexibility in their anti-HIV activity was inquired.•Results suggested their flexibility is more important than it has been assumed. The conserved binding site of HIV-1 gp120 envelope protein,...

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Bibliographic Details
Published in:Journal of molecular graphics & modelling 2013-07, Vol.44, p.91-103
Main Authors: Teixeira, Cátia, Serradji, Nawal, Amroune, Souad, Storck, Karen, Rogez-Kreuz, Christine, Clayette, Pascal, Barbault, Florent, Maurel, François
Format: Article
Language:English
Subjects:
Anti-HIV Agents - chemistry
Anti-HIV Agents - metabolism
Anti-HIV Agents - pharmacology
Binding Sites
BMS-378806
Conformational flexibility
Docking and molecular dynamics
HIV Envelope Protein gp120 - chemistry
HIV Envelope Protein gp120 - metabolism
HIV-1 - drug effects
HIV-1 gp120
Humans
Models, Molecular
Molecular Conformation
Molecular Docking Simulation
Molecular Dynamics Simulation
Piperazine derivatives
Piperazines - chemistry
Piperazines - metabolism
Piperazines - pharmacology
Protein Binding
Protein Conformation
Virus Replication - drug effects
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Summary:•The binding mode of piperazine derivatives with HIV-1 gp120 was predicted.•Impact of their conformational flexibility in their anti-HIV activity was inquired.•Results suggested their flexibility is more important than it has been assumed. The conserved binding site of HIV-1 gp120 envelope protein, an essential component in the viral entry process, provides an attractive antiviral target. The structural similarities between two piperazine derivatives: PMS-601, showing a dual activity for anti-PAF and anti-HIV activity, and BMS-378806, known to inhibit HIV-1 gp120, motivated us to merge important structural features of the two compounds. Novel piperazine derivatives were synthesized and evaluated in vitro concerning their ability to inhibit HIV-1 replication in in vitro infected lymphocytes. We described an approach that combines molecular docking, molecular dynamics, MM-PBSA calculations and conformational analysis to rationally predict piperazine derivatives binding mode with HIV-1 gp120. We also inquired about the conformational adaptability of the molecules, upon complex formation, and its importance to their respective inhibitory activity. The analysis suggested that the impact of the flexibility of these molecules revealed to be more important, in the context of drug design, than it has generally been assumed. These new insights at the atomic level might be useful to design inhibitors with improved antiviral activity.
ISSN:1093-3263
1873-4243
DOI:10.1016/j.jmgm.2013.05.003