Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping

Structure-guided drug discovery emerged in the 1970s and 1980s, stimulated by the three-dimensional structures of protein targets that became available, mainly through X-ray crystal structure analysis, assisted by the development of synchrotron radiation sources. Structures of known drugs or inhibit...

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Autores principales: Thomas, Sherine E., Collins, Patrick, James, Rory Hennell, Mendes, Vitor, Charoensutthivarakul, Sitthivut, Radoux, Chris, Abell, Chris, Coyne, Anthony G., Floto, R. Andres, von Delft, Frank, Blundell, Tom L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society Publishing 2019
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Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6501894/
https://www.ncbi.nlm.nih.gov/pubmed/31030650
http://dx.doi.org/10.1098/rsta.2018.0422
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author Thomas, Sherine E.
Collins, Patrick
James, Rory Hennell
Mendes, Vitor
Charoensutthivarakul, Sitthivut
Radoux, Chris
Abell, Chris
Coyne, Anthony G.
Floto, R. Andres
von Delft, Frank
Blundell, Tom L.
author_facet Thomas, Sherine E.
Collins, Patrick
James, Rory Hennell
Mendes, Vitor
Charoensutthivarakul, Sitthivut
Radoux, Chris
Abell, Chris
Coyne, Anthony G.
Floto, R. Andres
von Delft, Frank
Blundell, Tom L.
author_sort Thomas, Sherine E.
collection PubMed
description Structure-guided drug discovery emerged in the 1970s and 1980s, stimulated by the three-dimensional structures of protein targets that became available, mainly through X-ray crystal structure analysis, assisted by the development of synchrotron radiation sources. Structures of known drugs or inhibitors were used to guide the development of leads. The growth of high-throughput screening during the late 1980s and the early 1990s in the pharmaceutical industry of chemical libraries of hundreds of thousands of compounds of molecular weight of approximately 500 Da was impressive but still explored only a tiny fraction of the chemical space of the predicted 10(40) drug-like compounds. The use of fragments with molecular weights less than 300 Da in drug discovery not only decreased the chemical space needing exploration but also increased promiscuity in binding targets. Here we discuss advances in X-ray fragment screening and the challenge of identifying sites where fragments not only bind but can be chemically elaborated while retaining their positions and binding modes. We first describe the analysis of fragment binding using conventional X-ray difference Fourier techniques, with Mycobacterium abscessus SAICAR synthetase (PurC) as an example. We observe that all fragments occupy positions predicted by computational hotspot mapping. We compare this with fragment screening at Diamond Synchrotron Light Source XChem facility using PanDDA software, which identifies many more fragment hits, only some of which bind to the predicted hotspots. Many low occupancy sites identified may not support elaboration to give adequate ligand affinity, although they will likely be useful in drug discovery as ‘warm spots’ for guiding elaboration of fragments bound at hotspots. We discuss implications of these observations for fragment screening at the synchrotron sources. This article is part of the theme issue ‘Fifty years of synchrotron science: achievements and opportunities’.
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spelling pubmed-65018942019-05-13 Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping Thomas, Sherine E. Collins, Patrick James, Rory Hennell Mendes, Vitor Charoensutthivarakul, Sitthivut Radoux, Chris Abell, Chris Coyne, Anthony G. Floto, R. Andres von Delft, Frank Blundell, Tom L. Philos Trans A Math Phys Eng Sci Articles Structure-guided drug discovery emerged in the 1970s and 1980s, stimulated by the three-dimensional structures of protein targets that became available, mainly through X-ray crystal structure analysis, assisted by the development of synchrotron radiation sources. Structures of known drugs or inhibitors were used to guide the development of leads. The growth of high-throughput screening during the late 1980s and the early 1990s in the pharmaceutical industry of chemical libraries of hundreds of thousands of compounds of molecular weight of approximately 500 Da was impressive but still explored only a tiny fraction of the chemical space of the predicted 10(40) drug-like compounds. The use of fragments with molecular weights less than 300 Da in drug discovery not only decreased the chemical space needing exploration but also increased promiscuity in binding targets. Here we discuss advances in X-ray fragment screening and the challenge of identifying sites where fragments not only bind but can be chemically elaborated while retaining their positions and binding modes. We first describe the analysis of fragment binding using conventional X-ray difference Fourier techniques, with Mycobacterium abscessus SAICAR synthetase (PurC) as an example. We observe that all fragments occupy positions predicted by computational hotspot mapping. We compare this with fragment screening at Diamond Synchrotron Light Source XChem facility using PanDDA software, which identifies many more fragment hits, only some of which bind to the predicted hotspots. Many low occupancy sites identified may not support elaboration to give adequate ligand affinity, although they will likely be useful in drug discovery as ‘warm spots’ for guiding elaboration of fragments bound at hotspots. We discuss implications of these observations for fragment screening at the synchrotron sources. This article is part of the theme issue ‘Fifty years of synchrotron science: achievements and opportunities’. The Royal Society Publishing 2019-06-17 2019-04-29 /pmc/articles/PMC6501894/ /pubmed/31030650 http://dx.doi.org/10.1098/rsta.2018.0422 Text en © 2019 The Authors. http://creativecommons.org/licenses/by/4.0/ Published by the Royal Society under the terms of the Creative Commons Attribution License http://creativecommons.org/licenses/by/4.0/, which permits unrestricted use, provided the original author and source are credited.
spellingShingle Articles
Thomas, Sherine E.
Collins, Patrick
James, Rory Hennell
Mendes, Vitor
Charoensutthivarakul, Sitthivut
Radoux, Chris
Abell, Chris
Coyne, Anthony G.
Floto, R. Andres
von Delft, Frank
Blundell, Tom L.
Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping
title Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping
title_full Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping
title_fullStr Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping
title_full_unstemmed Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping
title_short Structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping
title_sort structure-guided fragment-based drug discovery at the synchrotron: screening binding sites and correlations with hotspot mapping
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6501894/
https://www.ncbi.nlm.nih.gov/pubmed/31030650
http://dx.doi.org/10.1098/rsta.2018.0422
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