Qgui: A high-throughput interface for automated setup and analysis of free energy calculations and empirical valence bond simulations in biological systems

2015 ◽  
Vol 60 ◽  
pp. 15-23 ◽  
Author(s):  
Geir Villy Isaksen ◽  
Tor Arne Heim Andberg ◽  
Johan Åqvist ◽  
Bjørn Olav Brandsdal
Keyword(s):  
Free Energy ◽  
High Throughput ◽  
Biological Systems ◽  
Valence Bond ◽  
Free Energy Calculations ◽  
Energy Calculations ◽  
Empirical Valence Bond

scholarly journals Q6: A comprehensive toolkit for empirical valence bond and related free energy calculations

SoftwareX ◽  
2018 ◽  
Vol 7 ◽  
pp. 388-395 ◽  
Author(s):  
Paul Bauer ◽  
Alexandre Barrozo ◽  
Miha Purg ◽  
Beat Anton Amrein ◽  
Mauricio Esguerra ◽  
...  
Keyword(s):  
Free Energy ◽  
Valence Bond ◽  
Free Energy Calculations ◽  
Energy Calculations ◽  
Empirical Valence Bond

scholarly journals Implementation of the QUBE Force Field in SOMD for High-Throughput Alchemical Free Energy Calculations

2021 ◽  
Author(s):  
Lauren Nelson ◽  
Sofia Bariami ◽  
Chris Ringrose ◽  
Joshua Horton ◽  
Vadiraj Kurdekar ◽  
...  
Keyword(s):  
Free Energy ◽  
Force Field ◽  
High Throughput ◽  
Free Energy Calculations ◽  
Dynamics Simulation ◽  
Energy Calculation ◽  
Energy Calculations ◽  
Alchemical Free Energy ◽  
Simulation Package ◽  
Alchemical Free Energy Calculations

<div><div><div><p>The quantum mechanical bespoke (QUBE) force field approach has been developed to facilitate the automated derivation of potential energy function parameters for modelling protein-ligand binding. To date the approach has been validated in the context of Monte Carlo simulations of protein-ligand complexes. We describe here the implementation of the QUBE force field in the alchemical free energy calculation molecular dynamics simulation package SOMD. The implementation is validated by demonstrating the reproducibility of absolute hydration free energies computed with the QUBE force field across the SOMD and GROMACS software packages. We further demonstrate, by way of a case study involving two series of non-nucleoside inhibitors of HIV-1 reverse transcriptase, that the availability of QUBE in a modern simulation package that makes efficient use of GPU acceleration will facilitate high-throughput alchemical free energy calculations.</p></div></div></div>

scholarly journals Combining Cloud-Based Free Energy Calculations, Synthetically Aware Enumerations and Goal-Directed Generative Machine Learning for Rapid Large-Scale Chemical Exploration and Optimization

2020 ◽  
Author(s):  
Phani Ghanakota ◽  
Pieter Bos ◽  
Kyle Konze ◽  
Joshua Staker ◽  
Gabriel Marques ◽  
...  
Keyword(s):  
Machine Learning ◽  
Free Energy ◽  
High Throughput ◽  
Large Scale ◽  
Chemical Space ◽  
Free Energy Calculations ◽  
Energy Calculations ◽  
Fold Enrichment ◽  
Property Space ◽  
High Throughput Screens

The hit identification process usually involves the profiling of millions to more recently billions of compounds either via traditional experimental high throughput screens (HTS) or computational virtual high throughput screens (vHTS). We have previously demonstrated that by coupling reaction-based enumeration, active learning and free energy calculations, a similarly large-scale exploration of chemical space can be extended to the hit-to-lead process. In this work, we augment that approach by coupling large scale enumeration and cloud-based FEP profiling with goal-directed generative machine learning, which results in a higher enrichment of potent ideas compared to large scale enumeration alone, while simultaneously staying within the bounds of a predefined drug-like property space. We are able to achieve this by building the molecular distribution for generative machine learning from the PathFinder rules-based enumeration and optimizing for a weighted sum QSAR based multi-parameter optimization function. We examine the utility of this combined approach by designing potent inhibitors of cyclin-dependent kinase 2 (CDK2) and demonstrate a coupled workflow that can: (1) provide a 6.4 fold enrichment improvement in identifying < 10nM compounds over random selection, and a 1.5 fold enrichment in identifying < 10nM compounds over our previous method (2) rapidly explore relevant chemical space outside the bounds of commercial reagents, (3) use generative ML approaches to “learn” the SAR from large scale in silico enumerations and generate novel idea molecules for a flexible receptor site that are both potent and within relevant physicochemical space and (4) produce over 3,000,000 idea molecules and run 2153 FEP simulations, identifying 69 ideas with a predicted IC<sub>50</sub> < 10nM and 358 ideas with a predicted IC<sub>50</sub> <100 nM. The reported data suggest combining both reaction-based and generative machine learning for ideation results in a higher enrichment of potent compounds over previously described approaches, and can rapidly accelerate the discovery of novel chemical matter within a predefined potency and property space.<br>

scholarly journals Combining Cloud-Based Free Energy Calculations, Synthetically Aware Enumerations and Goal-Directed Generative Machine Learning for Rapid Large-Scale Chemical Exploration and Optimization

2020 ◽  
Author(s):  
Phani Ghanakota ◽  
Pieter Bos ◽  
Kyle Konze ◽  
Joshua Staker ◽  
Gabriel Marques ◽  
...  
Keyword(s):  
Machine Learning ◽  
Free Energy ◽  
High Throughput ◽  
Large Scale ◽  
Chemical Space ◽  
Free Energy Calculations ◽  
Energy Calculations ◽  
Fold Enrichment ◽  
Property Space ◽  
High Throughput Screens

The hit identification process usually involves the profiling of millions to more recently billions of compounds either via traditional experimental high throughput screens (HTS) or computational virtual high throughput screens (vHTS). We have previously demonstrated that by coupling reaction-based enumeration, active learning and free energy calculations, a similarly large-scale exploration of chemical space can be extended to the hit-to-lead process. In this work, we augment that approach by coupling large scale enumeration and cloud-based FEP profiling with goal-directed generative machine learning, which results in a higher enrichment of potent ideas compared to large scale enumeration alone, while simultaneously staying within the bounds of a predefined drug-like property space. We are able to achieve this by building the molecular distribution for generative machine learning from the PathFinder rules-based enumeration and optimizing for a weighted sum QSAR based multi-parameter optimization function. We examine the utility of this combined approach by designing potent inhibitors of cyclin-dependent kinase 2 (CDK2) and demonstrate a coupled workflow that can: (1) provide a 6.4 fold enrichment improvement in identifying < 10nM compounds over random selection, and a 1.5 fold enrichment in identifying < 10nM compounds over our previous method (2) rapidly explore relevant chemical space outside the bounds of commercial reagents, (3) use generative ML approaches to “learn” the SAR from large scale in silico enumerations and generate novel idea molecules for a flexible receptor site that are both potent and within relevant physicochemical space and (4) produce over 3,000,000 idea molecules and run 2153 FEP simulations, identifying 69 ideas with a predicted IC<sub>50</sub> < 10nM and 358 ideas with a predicted IC<sub>50</sub> <100 nM. The reported data suggest combining both reaction-based and generative machine learning for ideation results in a higher enrichment of potent compounds over previously described approaches, and can rapidly accelerate the discovery of novel chemical matter within a predefined potency and property space.<br>

Sign in / Sign up

Export Citation Format

Share Document