Molecular Dynamics Simulations and Kinetic Measurements to Estimate and Predict Protein-Ligand Residence Times.

Authors :: Mollica L
Theret I
Antoine M
Perron-Sierra F
Charton Y
Fourquez JM
Wierzbicki M
Boutin JA
Ferry G
Decherchi S
Bottegoni G
Ducrot P
Cavalli A
Source :: Journal of medicinal chemistry [J Med Chem] 2016 Aug 11; Vol. 59 (15), pp. 7167-76. Date of Electronic Publication: 2016 Jul 22.
Publication Year :: 2016
Abstract: Ligand-target residence time is emerging as a key drug discovery parameter because it can reliably predict drug efficacy in vivo. Experimental approaches to binding and unbinding kinetics are nowadays available, but we still lack reliable computational tools for predicting kinetics and residence time. Most attempts have been based on brute-force molecular dynamics (MD) simulations, which are CPU-demanding and not yet particularly accurate. We recently reported a new scaled-MD-based protocol, which showed potential for residence time prediction in drug discovery. Here, we further challenged our procedure's predictive ability by applying our methodology to a series of glucokinase activators that could be useful for treating type 2 diabetes mellitus. We combined scaled MD with experimental kinetics measurements and X-ray crystallography, promptly checking the protocol's reliability by directly comparing computational predictions and experimental measures. The good agreement highlights the potential of our scaled-MD-based approach as an innovative method for computationally estimating and predicting drug residence times.

Subjects :: Crystallography, X-Ray
Diabetes Mellitus, Type 2 drug therapy
Diabetes Mellitus, Type 2 metabolism
Glucokinase antagonists & inhibitors
Glucokinase metabolism
Humans
Isoenzymes antagonists & inhibitors
Isoenzymes chemistry
Isoenzymes metabolism
Kinetics
Ligands
Models, Molecular
Molecular Structure
Structure-Activity Relationship
Time Factors
Glucokinase chemistry
Molecular Dynamics Simulation

Full Text Access

Tools