Toward physics-based solubility computation for pharmaceuticals to rival informatics

Daniel J. Fowles; David S. Palmer; Rui Guo; Sarah L. Price; John B. O. Mitchell

doi:10.1021/acs.jctc.1c00130

Toward physics-based solubility computation for pharmaceuticals to rival informatics

Daniel J. Fowles, David S. Palmer, Rui Guo, Sarah L. Price, John B. O. Mitchell

Research output: Contribution to journal › Article › peer-review

Abstract

We demonstrate that physics-based calculations of intrinsic aqueous solubility can rival cheminformatics-based machine learning predictions. A proof-of-concept was developed for a physics-based approach via a sublimation thermodynamic cycle, building upon previous work that relied upon several thermodynamic approximations, notably the 2RT approximation, and limited conformational sampling. Here, we apply improvements to our sublimation free-energy model with the use of crystal phonon mode calculations to capture the contributions of the vibrational modes of the crystal. Including these improvements with lattice energies computed using the model-potential-based Ψ_mol method leads to accurate estimates of sublimation free energy. Combining these with hydration free energies obtained from either molecular dynamics free-energy perturbation simulations or density functional theory calculations, solubilities comparable to both experiment and informatics predictions are obtained. The application to coronene, succinic acid, and the pharmaceutical desloratadine shows how the methods must be adapted for the adoption of different conformations in different phases. The approach has the flexibility to extend to applications that cannot be covered by informatics methods.

Original language	English
Pages (from-to)	3700-3709
Number of pages	10
Journal	Journal of Chemical Theory and Computation
Volume	17
Issue number	6
Early online date	14 May 2021
DOIs	https://doi.org/10.1021/acs.jctc.1c00130
Publication status	Published - 8 Jun 2021

Access to Document

10.1021/acs.jctc.1c00130Licence: CC BY

Fowles_2021_JCTC_Towrds-physics_CC
Copyright © 2021 The Authors. Published by American Chemical Society. This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
Final published version, 4.29 MBLicence: CC BY

Data Underpinning: Toward physics-based solubility computation for pharmaceuticals to rival informatics
Fowles, D. (Creator), Palmer, D. (Creator), Guo, R. (Creator), Price, S. (Creator) & Mitchell, J. B. O. (Creator), University of St Andrews, 2021
DOI: 10.17630/4a3b4fba-1e62-46d5-af7a-6eedfb517c67, https://doi.org/10.1021/acs.jctc.1c00130.s001
Dataset

File

Cite this

@article{118e9be9105c49a28c243cdabe7e8f94,

title = "Toward physics-based solubility computation for pharmaceuticals to rival informatics",

abstract = "We demonstrate that physics-based calculations of intrinsic aqueous solubility can rival cheminformatics-based machine learning predictions. A proof-of-concept was developed for a physics-based approach via a sublimation thermodynamic cycle, building upon previous work that relied upon several thermodynamic approximations, notably the 2RT approximation, and limited conformational sampling. Here, we apply improvements to our sublimation free-energy model with the use of crystal phonon mode calculations to capture the contributions of the vibrational modes of the crystal. Including these improvements with lattice energies computed using the model-potential-based Ψmol method leads to accurate estimates of sublimation free energy. Combining these with hydration free energies obtained from either molecular dynamics free-energy perturbation simulations or density functional theory calculations, solubilities comparable to both experiment and informatics predictions are obtained. The application to coronene, succinic acid, and the pharmaceutical desloratadine shows how the methods must be adapted for the adoption of different conformations in different phases. The approach has the flexibility to extend to applications that cannot be covered by informatics methods.",

author = "Fowles, {Daniel J.} and Palmer, {David S.} and Rui Guo and Price, {Sarah L.} and Mitchell, {John B. O.}",

note = "D.S.P. and D.J.F. thank the EPSRC for funding via Prosperity Partnership EP/S035990/1. D.S.P. and D.J.F. thank the ARCHIE-WeSt High-Performance Computing Centre (www.archie-west.ac.uk) for computational resources. The UCL authors thank Prof. Keith Refson for guidance with the phonon calculations, which used the ARCHER U.K. National Supercomputing Service (http://www.archer.ac.uk) as part of the U.K. HEC Materials Chemistry Consortium, which is funded by the EPSRC (EP/L000202, EP/R029431). R.G. was funded by MagnaPharm, a project funded by the European Union{\textquoteright}s Horizon 2020 Research and Innovation programme under grant agreement number 736899.",

year = "2021",

month = jun,

day = "8",

doi = "10.1021/acs.jctc.1c00130",

language = "English",

volume = "17",

pages = "3700--3709",

journal = "Journal of Chemical Theory and Computation",

issn = "1549-9618",

publisher = "American Chemical Society (ACS)",

number = "6",

}

TY - JOUR

T1 - Toward physics-based solubility computation for pharmaceuticals to rival informatics

AU - Fowles, Daniel J.

AU - Palmer, David S.

AU - Guo, Rui

AU - Price, Sarah L.

AU - Mitchell, John B. O.

N1 - D.S.P. and D.J.F. thank the EPSRC for funding via Prosperity Partnership EP/S035990/1. D.S.P. and D.J.F. thank the ARCHIE-WeSt High-Performance Computing Centre (www.archie-west.ac.uk) for computational resources. The UCL authors thank Prof. Keith Refson for guidance with the phonon calculations, which used the ARCHER U.K. National Supercomputing Service (http://www.archer.ac.uk) as part of the U.K. HEC Materials Chemistry Consortium, which is funded by the EPSRC (EP/L000202, EP/R029431). R.G. was funded by MagnaPharm, a project funded by the European Union’s Horizon 2020 Research and Innovation programme under grant agreement number 736899.

PY - 2021/6/8

Y1 - 2021/6/8

N2 - We demonstrate that physics-based calculations of intrinsic aqueous solubility can rival cheminformatics-based machine learning predictions. A proof-of-concept was developed for a physics-based approach via a sublimation thermodynamic cycle, building upon previous work that relied upon several thermodynamic approximations, notably the 2RT approximation, and limited conformational sampling. Here, we apply improvements to our sublimation free-energy model with the use of crystal phonon mode calculations to capture the contributions of the vibrational modes of the crystal. Including these improvements with lattice energies computed using the model-potential-based Ψmol method leads to accurate estimates of sublimation free energy. Combining these with hydration free energies obtained from either molecular dynamics free-energy perturbation simulations or density functional theory calculations, solubilities comparable to both experiment and informatics predictions are obtained. The application to coronene, succinic acid, and the pharmaceutical desloratadine shows how the methods must be adapted for the adoption of different conformations in different phases. The approach has the flexibility to extend to applications that cannot be covered by informatics methods.

AB - We demonstrate that physics-based calculations of intrinsic aqueous solubility can rival cheminformatics-based machine learning predictions. A proof-of-concept was developed for a physics-based approach via a sublimation thermodynamic cycle, building upon previous work that relied upon several thermodynamic approximations, notably the 2RT approximation, and limited conformational sampling. Here, we apply improvements to our sublimation free-energy model with the use of crystal phonon mode calculations to capture the contributions of the vibrational modes of the crystal. Including these improvements with lattice energies computed using the model-potential-based Ψmol method leads to accurate estimates of sublimation free energy. Combining these with hydration free energies obtained from either molecular dynamics free-energy perturbation simulations or density functional theory calculations, solubilities comparable to both experiment and informatics predictions are obtained. The application to coronene, succinic acid, and the pharmaceutical desloratadine shows how the methods must be adapted for the adoption of different conformations in different phases. The approach has the flexibility to extend to applications that cannot be covered by informatics methods.

U2 - 10.1021/acs.jctc.1c00130

DO - 10.1021/acs.jctc.1c00130

M3 - Article

SN - 1549-9618

VL - 17

SP - 3700

EP - 3709

JO - Journal of Chemical Theory and Computation

JF - Journal of Chemical Theory and Computation

IS - 6

ER -

Toward physics-based solubility computation for pharmaceuticals to rival informatics

Abstract

Access to Document

Fingerprint

Datasets

Data Underpinning: Toward physics-based solubility computation for pharmaceuticals to rival informatics

Cite this