Author:
Agrawal Nikhil,Parisini Emilio
Abstract
AbstractPAP248-286 is a fusogenic peptide derived from prostatic acid phosphatase, commonly found in human semen, and is known to mediate HIV fusion with cell membranes. In this study, we performed 120 independent coarse-grained molecular dynamics simulations to investigate the spontaneous binding of PAP248-286 monomers, considering both charged and neutral histidine (His) residues, to membrane bilayers composed of different lipid compositions: 100% POPC, 70% POPC-30% POPG, and 50% POPC-50% POPG. Our simulations revealed that PAP248-286 displayed spontaneous binding to the membrane, with increased binding observed in the presence of anionic lipid POPG. Specifically, in systems containing 30% and 50% POPG lipids, monomer residues, particularly in the systems containing charged histidine (His) residues, exhibited prolonged binding with the membrane. Furthermore, our simulations indicated that PAP248-286 adopted a parallel orientation with the membrane, exposing its positively charged residues to the lipid bilayer. Interestingly, systems containing charged His residues showed higher lipid occupancy around the peptide. These findings are consistent with previous experimental data, suggesting that PAP248-286 binding is enhanced in membranes with charged His residues, resembling the conditions found in the acidic vaginal pH environment. The results of our study provide further insights into the molecular mechanisms underlying the membrane binding of PAP248-286, contributing to our understanding of its potential role in HIV fusion and infection.
Publisher
Cold Spring Harbor Laboratory
Reference44 articles.
1. Organization, W. H. , Regional action plans for ending AIDS and the epidemics of viral hepatitis and sexually transmitted infections 2022–2030. 2023.
2. From a Deadly Disease to a Manageable Chronic Disease, HIV/AIDS Remains a Challenge for Mankind;LWW,2023
3. Viral tropism for the testis and sexual transmission;Frontiers in Immunology,2022
4. The role of semen in sexual transmission of HIV: beyond a carrier for virus particles
5. Semen-Derived Amyloid Fibrils Drastically Enhance HIV Infection