An insight to the molecular interactions of the FDA approved HIV PR drugs against L38L↑N↑L PR mutant

Zainab K Sanusi; Thavendran Govender; Glenn E M Maguire; Sibusiso B Maseko; Johnson Lin; Hendrik G Kruger; Bahareh Honarparvar

doi:10.1007/s10822-018-0099-9

An insight to the molecular interactions of the FDA approved HIV PR drugs against L38L↑N↑L PR mutant

J Comput Aided Mol Des. 2018 Mar;32(3):459-471. doi: 10.1007/s10822-018-0099-9. Epub 2018 Feb 3.

Authors

Zainab K Sanusi¹, Thavendran Govender¹, Glenn E M Maguire^{1

2}, Sibusiso B Maseko¹, Johnson Lin³, Hendrik G Kruger⁴, Bahareh Honarparvar⁵

Affiliations

¹ Catalysis and Peptide Research Unit, School of Health Sciences, University of KwaZulu-Natal, Durban, 4001, South Africa.
² School of Chemistry and Physics, University of KwaZulu-Natal, Durban, 4001, South Africa.
³ School of Life Sciences, University of KwaZulu-Natal, Durban, 4001, South Africa.
⁴ Catalysis and Peptide Research Unit, School of Health Sciences, University of KwaZulu-Natal, Durban, 4001, South Africa. kruger@ukzn.ac.za.
⁵ Catalysis and Peptide Research Unit, School of Health Sciences, University of KwaZulu-Natal, Durban, 4001, South Africa. Honarparvar@ukzn.ac.za.

PMID: 29397520
DOI: 10.1007/s10822-018-0099-9

Abstract

The aspartate protease of the human immune deficiency type-1 virus (HIV-1) has become a crucial antiviral target in which many useful antiretroviral inhibitors have been developed. However, it seems the emergence of new HIV-1 PR mutations enhances drug resistance, hence, the available FDA approved drugs show less activity towards the protease. A mutation and insertion designated L38L↑N↑L PR was recently reported from subtype of C-SA HIV-1. An integrated two-layered ONIOM (QM:MM) method was employed in this study to examine the binding affinities of the nine HIV PR inhibitors against this mutant. The computed binding free energies as well as experimental data revealed a reduced inhibitory activity towards the L38L↑N↑L PR in comparison with subtype C-SA HIV-1 PR. This observation suggests that the insertion and mutations significantly affect the binding affinities or characteristics of the HIV PIs and/or parent PR. The same trend for the computational binding free energies was observed for eight of the nine inhibitors with respect to the experimental binding free energies. The outcome of this study shows that ONIOM method can be used as a reliable computational approach to rationalize lead compounds against specific targets. The nature of the intermolecular interactions in terms of the host-guest hydrogen bond interactions is discussed using the atoms in molecules (AIM) analysis. Natural bond orbital analysis was also used to determine the extent of charge transfer between the QM region of the L38L↑N↑L PR enzyme and FDA approved drugs. AIM analysis showed that the interaction between the QM region of the L38L↑N↑L PR and FDA approved drugs are electrostatic dominant, the bond stability computed from the NBO analysis supports the results from the AIM application. Future studies will focus on the improvement of the computational model by considering explicit water molecules in the active pocket. We believe that this approach has the potential to provide information that will aid in the design of much improved HIV-1 PR antiviral drugs.

Keywords: Atoms in molecules (AIM); Binding free energies; HIV PR inhibitors; Inhibitor–enzyme interactions; L38L↑N↑L PR; Natural bond orbital (NBO); Our own N-layered Integrated molecular orbital and molecular mechanics (ONIOM).

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Anti-HIV Agents / chemistry*
Drug Approval
Drug Resistance, Viral
HIV Protease / genetics*
HIV Protease Inhibitors / chemistry*
Hydrogen Bonding
Models, Molecular*
Mutation
Protein Binding
Structure-Activity Relationship
Thermodynamics
United States
United States Food and Drug Administration
Water / chemistry

Substances

Anti-HIV Agents
HIV Protease Inhibitors
Water
HIV Protease