Background: Most licensed antiviral drugs are nucleoside analogs. A recent research focuses on blocking a virus from entering the cells in the viral cell adsorption/entry stage. In this entry mechanism, the glycans present on the viral surface play a fundamental role. Homochiral L-peptides acting this fusion mechanism have shown some inhibition of viral infection. Peptides with regularly alternating enantiomeric sequence (L,D-peptides) can assume structures that are not accessible to the corresponding homochiral molecules. Furthermore, L,D-peptides are less sensitive to enzymatic digestion. Aim: In silico design of an L, D-peptide with a high affinity for the viral surface glycans and consequently able to interfere with its fusion mechanism. Methods: We used a 3α,6α3α,6α-Mannopentaose (3-6MP) molecule to simulate a viral surface glycan. We performed molecular dynamics (MD) simulations of 3-6MP and D,L-peptide in water using the force field AMBER12-GLYCAM06i. We evaluated the binding constant from trajectories. The D,L-peptide molecule was modified over the sequence, the length, the terminals and finally glycosylated to attain a very high binding constant value for 3-6MP. In addition, we studied the specific interaction between T lymphocyte CD4 glycoprotein and HIV envelope glycoprotein gp120 through MD simulations between a D,L-peptide, bounded to a typical CD4 glycan, and a highly conserved HIV gp120 glycan. Results: Concerning the interaction with 3-6MP molecule, the very effective molecule obtained was H-d-Trp-l-Pro-d-Asn-l-Pro-d-Trp-l-Pro-d-Asn-l-Pro-OH where the Asn residues in position 3 and 7 are glycosylated with alpha-D-Mannopyranosyl-(1→31→3)-[alpha-D-mannopyranosyl-(1→61→6)]-alpha-D-mannopyranosyl-(1→41→4)-N-acetyl-beta-D-glucopyranosyl-(1→41→4)-N-acetyl-beta-D-glucopyranosyl-1-OH. As far as the interaction with HIV envelope is considered instead, the very effective molecule obtained, able to antagonize the CD4 glycoprotein, was H-d-Trp-l-Pro-d-Asn-l-Pro-d-Trp-l-Pro-d-Asn-l-Pro-OH where the Asn residue in position 3 is glycosylated with alpha-D-galactopyranosyl-(1→41→4)- N-acetyl-beta-D-glucopyranosyl-(1→21→2)-alpha-D-Mannopyranosyl-(1→31→3)- [alpha-D-galactopyranosyl-(1→41→4)- N-acetyl-beta-D-glucopyranosyl-(1→21→2)- alpha-D-Mannopyranosyl-(1→61→6)]- beta-D-mannopyranosyl-(1→41→4)-N-acetyl-beta-D-glucopyranosyl-(1→41→4)-N-acetyl-beta-D-glucopyranosyl-1-OH Conclusion: The above optimized glycosylated D,L-peptide molecules could be very promising representatives of a new powerful class of antiviral agents.
