Estimation of ligand binding free energy using multi-eGO.

03 December 2024, Version 2
This content is a preprint and has not undergone peer review at the time of posting.

Abstract

The computational study of ligand binding to a target protein provides mechanistic insight into the molecular determinants of this process and can improve the success rate of in silico drug design. All-atom molecular dynamics (MD) simulations can be used to evaluate the binding free energy, typically by thermodynamic integration, and to probe binding mechanisms, including the description of protein conformational dynamics. The advantages of MD come at a high computational cost, which limits its use. Such cost could be reduced by using coarse-grained models, but their use is generally associated with an undesirable loss of resolution and accuracy. To address the trade-off between speed and accuracy of MD simulations, we describe the use of the recently introduced multi-eGO atomic model for the estimation of binding free energies. We illustrate this approach in the case of the binding of benzene to lysozyme by both thermodynamic integration and metadynamics, showing multiple binding/unbinding pathways of benzene. We then provide equally accurate results for the binding free en-ergy of dasatinib and PP1 to Src kinase by thermodynamic integration. Finally, we show how we can describe the binding of the small molecule 10074-G5 to Aβ42 by single molecule simulations and by explicit titration of the ligand as a function of concentration. These results demonstrate that multi-eGO has the potential to significantly reduce the cost of accurate binding free energy calculations and can be used to develop and benchmark in silico ligand binding techniques.

Keywords

Ligand binding
binding free energy
thermodynamic integration
molecular dynamics
lysozyme
c-Src kinase
aβ42
multi-eGO

Supplementary materials

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Supporting Information
Description
The supporting information file contains extended convergence plots for all the TI and VMetaD calculations performed, the representation of binding pathways for LYZ:BNZ, the parameters selection details for SRC:DAS, SRC:PP1, and Aβ42:10074-G5; supporting tables with the parameters for all the TI performed on the four systems. Finally, we added 4 movies showing the binding events from multi-eGO simulations in the four complexes.
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