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Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions

[Image: see text] The development of ligands for biological targets is critically dependent on the identification of sites on proteins that bind molecules with high affinity. A set of compounds, called FragLites, can identify such sites, along with the interactions required to gain affinity, by X-ra...

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Autores principales: Davison, Gemma, Martin, Mathew P., Turberville, Shannon, Dormen, Selma, Heath, Richard, Heptinstall, Amy B., Lawson, Marie, Miller, Duncan C., Ng, Yi Min, Sanderson, James N., Hope, Ian, Wood, Daniel J., Cano, Céline, Endicott, Jane A., Hardcastle, Ian R., Noble, Martin E. M., Waring, Michael J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2022
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9706561/
https://www.ncbi.nlm.nih.gov/pubmed/36367089
http://dx.doi.org/10.1021/acs.jmedchem.2c01357
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author Davison, Gemma
Martin, Mathew P.
Turberville, Shannon
Dormen, Selma
Heath, Richard
Heptinstall, Amy B.
Lawson, Marie
Miller, Duncan C.
Ng, Yi Min
Sanderson, James N.
Hope, Ian
Wood, Daniel J.
Cano, Céline
Endicott, Jane A.
Hardcastle, Ian R.
Noble, Martin E. M.
Waring, Michael J.
author_facet Davison, Gemma
Martin, Mathew P.
Turberville, Shannon
Dormen, Selma
Heath, Richard
Heptinstall, Amy B.
Lawson, Marie
Miller, Duncan C.
Ng, Yi Min
Sanderson, James N.
Hope, Ian
Wood, Daniel J.
Cano, Céline
Endicott, Jane A.
Hardcastle, Ian R.
Noble, Martin E. M.
Waring, Michael J.
author_sort Davison, Gemma
collection PubMed
description [Image: see text] The development of ligands for biological targets is critically dependent on the identification of sites on proteins that bind molecules with high affinity. A set of compounds, called FragLites, can identify such sites, along with the interactions required to gain affinity, by X-ray crystallography. We demonstrate the utility of FragLites in mapping the binding sites of bromodomain proteins BRD4 and ATAD2 and demonstrate that FragLite mapping is comparable to a full fragment screen in identifying ligand binding sites and key interactions. We extend the FragLite set with analogous compounds derived from amino acids (termed PepLites) that mimic the interactions of peptides. The output of the FragLite maps is shown to enable the development of ligands with leadlike potency. This work establishes the use of FragLite and PepLite screening at an early stage in ligand discovery allowing the rapid assessment of tractability of protein targets and informing downstream hit-finding.
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spelling pubmed-97065612022-11-30 Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions Davison, Gemma Martin, Mathew P. Turberville, Shannon Dormen, Selma Heath, Richard Heptinstall, Amy B. Lawson, Marie Miller, Duncan C. Ng, Yi Min Sanderson, James N. Hope, Ian Wood, Daniel J. Cano, Céline Endicott, Jane A. Hardcastle, Ian R. Noble, Martin E. M. Waring, Michael J. J Med Chem [Image: see text] The development of ligands for biological targets is critically dependent on the identification of sites on proteins that bind molecules with high affinity. A set of compounds, called FragLites, can identify such sites, along with the interactions required to gain affinity, by X-ray crystallography. We demonstrate the utility of FragLites in mapping the binding sites of bromodomain proteins BRD4 and ATAD2 and demonstrate that FragLite mapping is comparable to a full fragment screen in identifying ligand binding sites and key interactions. We extend the FragLite set with analogous compounds derived from amino acids (termed PepLites) that mimic the interactions of peptides. The output of the FragLite maps is shown to enable the development of ligands with leadlike potency. This work establishes the use of FragLite and PepLite screening at an early stage in ligand discovery allowing the rapid assessment of tractability of protein targets and informing downstream hit-finding. American Chemical Society 2022-11-11 2022-11-24 /pmc/articles/PMC9706561/ /pubmed/36367089 http://dx.doi.org/10.1021/acs.jmedchem.2c01357 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by/4.0/Permits the broadest form of re-use including for commercial purposes, provided that author attribution and integrity are maintained (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Davison, Gemma
Martin, Mathew P.
Turberville, Shannon
Dormen, Selma
Heath, Richard
Heptinstall, Amy B.
Lawson, Marie
Miller, Duncan C.
Ng, Yi Min
Sanderson, James N.
Hope, Ian
Wood, Daniel J.
Cano, Céline
Endicott, Jane A.
Hardcastle, Ian R.
Noble, Martin E. M.
Waring, Michael J.
Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions
title Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions
title_full Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions
title_fullStr Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions
title_full_unstemmed Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions
title_short Mapping Ligand Interactions of Bromodomains BRD4 and ATAD2 with FragLites and PepLites—Halogenated Probes of Druglike and Peptide-like Molecular Interactions
title_sort mapping ligand interactions of bromodomains brd4 and atad2 with fraglites and peplites—halogenated probes of druglike and peptide-like molecular interactions
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9706561/
https://www.ncbi.nlm.nih.gov/pubmed/36367089
http://dx.doi.org/10.1021/acs.jmedchem.2c01357
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