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Ligand unbinding mechanisms and kinetics for T4 lysozyme mutants from τRAMD simulations

Ariane Nunes-Alves, Daria B. Kokh, Rebecca C. Wade

2021Current Research in Structural Biology64 citationsDOIOpen Access PDF

Abstract

The protein-ligand residence time, τ, influences molecular function in biological networks and has been recognized as an important determinant of drug efficacy. To predict τ, computational methods must overcome the problem that τ often exceeds the timescales accessible to conventional molecular dynamics (MD) simulation. Here, we apply the τ-Random Acceleration Molecular Dynamics (τRAMD) method to a set of kinetically characterized complexes of T4 lysozyme mutants with small, engineered binding cavities. τRAMD yields relative ligand dissociation rates in good accordance with experiments across this diverse set of complexes that differ with regard to measurement temperature, ligand identity, protein mutation and binding cavity. τRAMD thereby allows a comprehensive characterization of the ligand egress routes and determinants of τ. Although ligand dissociation by multiple egress routes is observed, we find that egress via the predominant route determines the value of τ. We also find that the presence of a greater number of metastable states along egress pathways leads to slower protein-ligand dissociation. These physical insights could be exploited in the rational optimization of the kinetic properties of drug candidates.

Topics & Concepts

ChemistryMolecular dynamicsLigand (biochemistry)KineticsDissociation (chemistry)LysozymeBiophysicsMutantMetastabilityProtein ligandFunction (biology)Plasma protein bindingStereochemistryComputational chemistryDocking (animal)Receptor–ligand kineticsChemical physicsAllosteric regulationProtein structureMoleculeDrug discoveryComputational biologyProtein Structure and DynamicsAdvanced Fluorescence Microscopy TechniquesComputational Drug Discovery Methods
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