Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models

[Image: see text] The first kinase inhibitor drug approval in 2001 initiated a remarkable decade of tyrosine kinase inhibitor drugs for oncology indications, but a void exists for serine/threonine protein kinase inhibitor drugs and central nervous system indications. Stress kinases are of special in...

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Autores principales: Roy, Saktimayee M., Grum-Tokars, Valerie L., Schavocky, James P., Saeed, Faisal, Staniszewski, Agnieszka, Teich, Andrew F., Arancio, Ottavio, Bachstetter, Adam D., Webster, Scott J., Van Eldik, Linda J., Minasov, George, Anderson, Wayne F., Pelletier, Jeffrey C., Watterson, D. Martin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2015
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4404319/
https://www.ncbi.nlm.nih.gov/pubmed/25676389
http://dx.doi.org/10.1021/acschemneuro.5b00002
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author Roy, Saktimayee M.
Grum-Tokars, Valerie L.
Schavocky, James P.
Saeed, Faisal
Staniszewski, Agnieszka
Teich, Andrew F.
Arancio, Ottavio
Bachstetter, Adam D.
Webster, Scott J.
Van Eldik, Linda J.
Minasov, George
Anderson, Wayne F.
Pelletier, Jeffrey C.
Watterson, D. Martin
author_facet Roy, Saktimayee M.
Grum-Tokars, Valerie L.
Schavocky, James P.
Saeed, Faisal
Staniszewski, Agnieszka
Teich, Andrew F.
Arancio, Ottavio
Bachstetter, Adam D.
Webster, Scott J.
Van Eldik, Linda J.
Minasov, George
Anderson, Wayne F.
Pelletier, Jeffrey C.
Watterson, D. Martin
author_sort Roy, Saktimayee M.
collection PubMed
description [Image: see text] The first kinase inhibitor drug approval in 2001 initiated a remarkable decade of tyrosine kinase inhibitor drugs for oncology indications, but a void exists for serine/threonine protein kinase inhibitor drugs and central nervous system indications. Stress kinases are of special interest in neurological and neuropsychiatric disorders due to their involvement in synaptic dysfunction and complex disease susceptibility. Clinical and preclinical evidence implicates the stress related kinase p38αMAPK as a potential neurotherapeutic target, but isoform selective p38αMAPK inhibitor candidates are lacking and the mixed kinase inhibitor drugs that are promising in peripheral tissue disease indications have limitations for neurologic indications. Therefore, pursuit of the neurotherapeutic hypothesis requires kinase isoform selective inhibitors with appropriate neuropharmacology features. Synaptic dysfunction disorders offer a potential for enhanced pharmacological efficacy due to stress-induced activation of p38αMAPK in both neurons and glia, the interacting cellular components of the synaptic pathophysiological axis, to be modulated. We report a novel isoform selective p38αMAPK inhibitor, MW01-18-150SRM (=MW150), that is efficacious in suppression of hippocampal-dependent associative and spatial memory deficits in two distinct synaptic dysfunction mouse models. A synthetic scheme for biocompatible product and positive outcomes from pharmacological screens are presented. The high-resolution crystallographic structure of the p38αMAPK/MW150 complex documents active site binding, reveals a potential low energy conformation of the bound inhibitor, and suggests a structural explanation for MW150’s exquisite target selectivity. As far as we are aware, MW150 is without precedent as an isoform selective p38MAPK inhibitor or as a kinase inhibitor capable of modulating in vivo stress related behavior.
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spelling pubmed-44043192015-04-21 Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models Roy, Saktimayee M. Grum-Tokars, Valerie L. Schavocky, James P. Saeed, Faisal Staniszewski, Agnieszka Teich, Andrew F. Arancio, Ottavio Bachstetter, Adam D. Webster, Scott J. Van Eldik, Linda J. Minasov, George Anderson, Wayne F. Pelletier, Jeffrey C. Watterson, D. Martin ACS Chem Neurosci [Image: see text] The first kinase inhibitor drug approval in 2001 initiated a remarkable decade of tyrosine kinase inhibitor drugs for oncology indications, but a void exists for serine/threonine protein kinase inhibitor drugs and central nervous system indications. Stress kinases are of special interest in neurological and neuropsychiatric disorders due to their involvement in synaptic dysfunction and complex disease susceptibility. Clinical and preclinical evidence implicates the stress related kinase p38αMAPK as a potential neurotherapeutic target, but isoform selective p38αMAPK inhibitor candidates are lacking and the mixed kinase inhibitor drugs that are promising in peripheral tissue disease indications have limitations for neurologic indications. Therefore, pursuit of the neurotherapeutic hypothesis requires kinase isoform selective inhibitors with appropriate neuropharmacology features. Synaptic dysfunction disorders offer a potential for enhanced pharmacological efficacy due to stress-induced activation of p38αMAPK in both neurons and glia, the interacting cellular components of the synaptic pathophysiological axis, to be modulated. We report a novel isoform selective p38αMAPK inhibitor, MW01-18-150SRM (=MW150), that is efficacious in suppression of hippocampal-dependent associative and spatial memory deficits in two distinct synaptic dysfunction mouse models. A synthetic scheme for biocompatible product and positive outcomes from pharmacological screens are presented. The high-resolution crystallographic structure of the p38αMAPK/MW150 complex documents active site binding, reveals a potential low energy conformation of the bound inhibitor, and suggests a structural explanation for MW150’s exquisite target selectivity. As far as we are aware, MW150 is without precedent as an isoform selective p38MAPK inhibitor or as a kinase inhibitor capable of modulating in vivo stress related behavior. American Chemical Society 2015-02-13 /pmc/articles/PMC4404319/ /pubmed/25676389 http://dx.doi.org/10.1021/acschemneuro.5b00002 Text en Copyright © 2015 American Chemical Society This is an open access article published under a Creative Commons Attribution (CC-BY) License (http://pubs.acs.org/page/policy/authorchoice_ccby_termsofuse.html) , which permits unrestricted use, distribution and reproduction in any medium, provided the author and source are cited.
spellingShingle Roy, Saktimayee M.
Grum-Tokars, Valerie L.
Schavocky, James P.
Saeed, Faisal
Staniszewski, Agnieszka
Teich, Andrew F.
Arancio, Ottavio
Bachstetter, Adam D.
Webster, Scott J.
Van Eldik, Linda J.
Minasov, George
Anderson, Wayne F.
Pelletier, Jeffrey C.
Watterson, D. Martin
Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models
title Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models
title_full Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models
title_fullStr Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models
title_full_unstemmed Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models
title_short Targeting Human Central Nervous System Protein Kinases: An Isoform Selective p38αMAPK Inhibitor That Attenuates Disease Progression in Alzheimer’s Disease Mouse Models
title_sort targeting human central nervous system protein kinases: an isoform selective p38αmapk inhibitor that attenuates disease progression in alzheimer’s disease mouse models
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4404319/
https://www.ncbi.nlm.nih.gov/pubmed/25676389
http://dx.doi.org/10.1021/acschemneuro.5b00002
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