Paper Info
Title
Structural Basis for Species Selectivity in the HIV-1 gp120-CD4 Interaction: Restoring Affinity to gp120 in Murine CD4 Mimetic Peptides.
Abstract
The first step of HIV-1 infection involves interaction between the viral glycoprotein gp120 and the human cellular receptor CD4. Inhibition of the gp120-CD4 interaction represents an attractive strategy to block HIV-1 infection. In an attempt to explore the known lack of affinity of murine CD4 to gp120, we have investigated peptides presenting the putative gp120-binding site of murine CD4 (mCD4). Molecular modeling indicates that mCD4 protein cannot bind gp120 due to steric clashes, while the larger conformational flexibility of mCD4 peptides allows an interaction. This finding is confirmed by experimental binding assays, which also evidenced specificity of the peptide-gp120 interaction. Molecular dynamics simulations indicate that the mCD4-peptide stably interacts with gp120 via an intermolecular β-sheet, while an important salt-bridge formed by a C-terminal lysine is lost. Fixation of the C-terminus by introducing a disulfide bridge between the N- and C-termini of the peptide significantly enhanced the affinity to gp120.
Year
DOI
Venue
2011
10.1155/2011/736593
Adv. Bioinformatics
Keywords
Field
DocType
bioinformatics
Biology,Disulfide bond,Peptide,Steric effects,Receptor,Molecular dynamics,Lysine,Bioinformatics,Molecular model,Selectivity
Journal
Volume
ISSN
Citations 
2011
1687-8035
0
PageRank 
References 
Authors
0.34
4
4
Name
Order
Citations
PageRank
Kristin Kassler100.34
Julia Meier200.34
Jutta Eichler300.34
Heinrich Sticht4514.49