Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets

BACKGROUND: Dual-specificity phosphatase-5 (DUSP5) plays a central role in vascular development and disease. We present a p-nitrophenol phosphate (pNPP) based enzymatic assay to screen for inhibitors of the phosphatase domain of DUSP5. METHODS: pNPP is a mimic of the phosphorylated tyrosine on the E...

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Autores principales: Neumann, Terrence S., Span, Elise A., Kalous, Kelsey S., Bongard, Robert, Gastonguay, Adam, Lepley, Michael A., Kutty, Raman G., Nayak, Jaladhi, Bohl, Chris, Lange, Rachel G., Sarker, Majher I., Talipov, Marat R., Rathore, Rajendra, Ramchandran, Ramani, Sem, Daniel S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4545774/
https://www.ncbi.nlm.nih.gov/pubmed/26286528
http://dx.doi.org/10.1186/s12858-015-0048-3
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author Neumann, Terrence S.
Span, Elise A.
Kalous, Kelsey S.
Bongard, Robert
Gastonguay, Adam
Lepley, Michael A.
Kutty, Raman G.
Nayak, Jaladhi
Bohl, Chris
Lange, Rachel G.
Sarker, Majher I.
Talipov, Marat R.
Rathore, Rajendra
Ramchandran, Ramani
Sem, Daniel S.
author_facet Neumann, Terrence S.
Span, Elise A.
Kalous, Kelsey S.
Bongard, Robert
Gastonguay, Adam
Lepley, Michael A.
Kutty, Raman G.
Nayak, Jaladhi
Bohl, Chris
Lange, Rachel G.
Sarker, Majher I.
Talipov, Marat R.
Rathore, Rajendra
Ramchandran, Ramani
Sem, Daniel S.
author_sort Neumann, Terrence S.
collection PubMed
description BACKGROUND: Dual-specificity phosphatase-5 (DUSP5) plays a central role in vascular development and disease. We present a p-nitrophenol phosphate (pNPP) based enzymatic assay to screen for inhibitors of the phosphatase domain of DUSP5. METHODS: pNPP is a mimic of the phosphorylated tyrosine on the ERK2 substrate (pERK2) and binds the DUSP5 phosphatase domain with a K(m) of 7.6 ± 0.4 mM. Docking followed by inhibitor verification using the pNPP assay identified a series of polysulfonated aromatic inhibitors that occupy the DUSP5 active site in the region that is likely occupied by the dual-phosphorylated ERK2 substrate tripeptide (pThr-Glu-pTyr). Secondary assays were performed with full length DUSP5 with ERK2 as substrate. RESULTS: The most potent inhibitor has a naphthalene trisulfonate (NTS) core. A search for similar compounds in a drug database identified suramin, a dimerized form of NTS. While suramin appears to be a potent and competitive inhibitor (25 ± 5 μM), binding to the DUSP5 phosphatase domain more tightly than the monomeric ligands of which it is comprised, it also aggregates. Further ligand-based screening, based on a pharmacophore derived from the 7 Å separation of sulfonates on inhibitors and on sulfates present in the DUSP5 crystal structure, identified a disulfonated and phenolic naphthalene inhibitor (CSD(3)_2320) with IC(50) of 33 μM that is similar to NTS and does not aggregate. CONCLUSIONS: The new DUSP5 inhibitors we identify in this study typically have sulfonates 7 Å apart, likely positioning them where the two phosphates of the substrate peptide (pThr-Glu-pTyr) bind, with one inhibitor also positioning a phenolic hydroxyl where the water nucleophile may reside. Polysulfonated aromatic compounds do not commonly appear in drugs and have a tendency to aggregate. One FDA-approved polysulfonated drug, suramin, inhibits DUSP5 and also aggregates. Docking and modeling studies presented herein identify polysulfonated aromatic inhibitors that do not aggregate, and provide insights to guide future design of mimics of the dual-phosphate loops of the ERK substrates for DUSPs. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12858-015-0048-3) contains supplementary material, which is available to authorized users.
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spelling pubmed-45457742015-08-23 Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets Neumann, Terrence S. Span, Elise A. Kalous, Kelsey S. Bongard, Robert Gastonguay, Adam Lepley, Michael A. Kutty, Raman G. Nayak, Jaladhi Bohl, Chris Lange, Rachel G. Sarker, Majher I. Talipov, Marat R. Rathore, Rajendra Ramchandran, Ramani Sem, Daniel S. BMC Biochem Research Article BACKGROUND: Dual-specificity phosphatase-5 (DUSP5) plays a central role in vascular development and disease. We present a p-nitrophenol phosphate (pNPP) based enzymatic assay to screen for inhibitors of the phosphatase domain of DUSP5. METHODS: pNPP is a mimic of the phosphorylated tyrosine on the ERK2 substrate (pERK2) and binds the DUSP5 phosphatase domain with a K(m) of 7.6 ± 0.4 mM. Docking followed by inhibitor verification using the pNPP assay identified a series of polysulfonated aromatic inhibitors that occupy the DUSP5 active site in the region that is likely occupied by the dual-phosphorylated ERK2 substrate tripeptide (pThr-Glu-pTyr). Secondary assays were performed with full length DUSP5 with ERK2 as substrate. RESULTS: The most potent inhibitor has a naphthalene trisulfonate (NTS) core. A search for similar compounds in a drug database identified suramin, a dimerized form of NTS. While suramin appears to be a potent and competitive inhibitor (25 ± 5 μM), binding to the DUSP5 phosphatase domain more tightly than the monomeric ligands of which it is comprised, it also aggregates. Further ligand-based screening, based on a pharmacophore derived from the 7 Å separation of sulfonates on inhibitors and on sulfates present in the DUSP5 crystal structure, identified a disulfonated and phenolic naphthalene inhibitor (CSD(3)_2320) with IC(50) of 33 μM that is similar to NTS and does not aggregate. CONCLUSIONS: The new DUSP5 inhibitors we identify in this study typically have sulfonates 7 Å apart, likely positioning them where the two phosphates of the substrate peptide (pThr-Glu-pTyr) bind, with one inhibitor also positioning a phenolic hydroxyl where the water nucleophile may reside. Polysulfonated aromatic compounds do not commonly appear in drugs and have a tendency to aggregate. One FDA-approved polysulfonated drug, suramin, inhibits DUSP5 and also aggregates. Docking and modeling studies presented herein identify polysulfonated aromatic inhibitors that do not aggregate, and provide insights to guide future design of mimics of the dual-phosphate loops of the ERK substrates for DUSPs. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12858-015-0048-3) contains supplementary material, which is available to authorized users. BioMed Central 2015-08-19 /pmc/articles/PMC4545774/ /pubmed/26286528 http://dx.doi.org/10.1186/s12858-015-0048-3 Text en © Neumann et al. 2015 Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research Article
Neumann, Terrence S.
Span, Elise A.
Kalous, Kelsey S.
Bongard, Robert
Gastonguay, Adam
Lepley, Michael A.
Kutty, Raman G.
Nayak, Jaladhi
Bohl, Chris
Lange, Rachel G.
Sarker, Majher I.
Talipov, Marat R.
Rathore, Rajendra
Ramchandran, Ramani
Sem, Daniel S.
Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets
title Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets
title_full Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets
title_fullStr Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets
title_full_unstemmed Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets
title_short Identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets
title_sort identification of inhibitors that target dual-specificity phosphatase 5 provide new insights into the binding requirements for the two phosphate pockets
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4545774/
https://www.ncbi.nlm.nih.gov/pubmed/26286528
http://dx.doi.org/10.1186/s12858-015-0048-3
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