Pathway Specific Unbinding Free Energy Profiles of Ritonavir Dissociation From HIV-1 Protease

Abstract: Investigation of protein-drug recognition is key in understanding drug selectivity and binding affinity. In combination, binding/unbinding free energy landscape and intermolecular interactions can be used to understand the drug binding/unbinding mechanisms. This information is vital for the development of drugs with improved efficacy and explanation of mutation effects. This study investigated the dissociation processes of ritonavir unbinding from HIV protease (HIVp). Analyzing unbinding trajectories modeled b… Show more