Conformational rearrangements required of the V3 loop of HIV‐1 gp120 for proteolytic cleavage and infection

Abstract

HIV gp120 is specifically cleaved at a single site in the V₃ loop between Arg³¹⁵ and Ala³¹⁶ by thrombin. Previous observations by others have indicated that binding to CD4 enhances the rate of V₃ loop cleavage, and that this cleavage is a prerequisite for HIV infection. Other observations also suggest that the cleavage site is in a type II β-turn centered at Pro³¹³-Gly³¹⁴. However, our docking experiments indicate that this conformation cannot dock to thrombin and other trypsin-like serine proteases. Thus, based on the thrombin-bound conformation of peptide substrates, we propose that CD4 binding, at a site remote from the V₃ loop, induces and stabilizes a trans to cis isomerization of the highly conserved residue Pro³¹³, and that this conformational shift is a prerequisite for cleavage by a ‘thrombin-like’ cellular pro tease and subsequent infection.