Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics

[Image: see text] The cyclooxygenase enzymes (COX-1 and COX-2) are the therapeutic targets of nonsteroidal anti-inflammatory drugs (NSAIDs). Neutralization of the carboxylic acid moiety of the NSAID indomethacin to an ester or amide functionality confers COX-2 selectivity, but the molecular basis fo...

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Autores principales: Konkle, Mary E., Blobaum, Anna L., Moth, Christopher W., Prusakiewicz, Jeffery J., Xu, Shu, Ghebreselasie, Kebreab, Akingbade, Dapo, Jacobs, Aaron T., Rouzer, Carol A., Lybrand, Terry P., Marnett, Lawrence J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2015
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4721528/
https://www.ncbi.nlm.nih.gov/pubmed/26704937
http://dx.doi.org/10.1021/acs.biochem.5b01222
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author Konkle, Mary E.
Blobaum, Anna L.
Moth, Christopher W.
Prusakiewicz, Jeffery J.
Xu, Shu
Ghebreselasie, Kebreab
Akingbade, Dapo
Jacobs, Aaron T.
Rouzer, Carol A.
Lybrand, Terry P.
Marnett, Lawrence J.
author_facet Konkle, Mary E.
Blobaum, Anna L.
Moth, Christopher W.
Prusakiewicz, Jeffery J.
Xu, Shu
Ghebreselasie, Kebreab
Akingbade, Dapo
Jacobs, Aaron T.
Rouzer, Carol A.
Lybrand, Terry P.
Marnett, Lawrence J.
author_sort Konkle, Mary E.
collection PubMed
description [Image: see text] The cyclooxygenase enzymes (COX-1 and COX-2) are the therapeutic targets of nonsteroidal anti-inflammatory drugs (NSAIDs). Neutralization of the carboxylic acid moiety of the NSAID indomethacin to an ester or amide functionality confers COX-2 selectivity, but the molecular basis for this selectivity has not been completely revealed through mutagenesis studies and/or X-ray crystallographic attempts. We expressed and assayed a number of divergent secondary shell COX-2 active site mutants and found that a COX-2 to COX-1 change at position 472 (Leu in COX-2, Met in COX-1) reduced the potency of enzyme inhibition by a series of COX-2-selective indomethacin amides and esters. In contrast, the potencies of indomethacin, arylacetic acid, propionic acid, and COX-2-selective diarylheterocycle inhibitors were either unaffected or only mildly affected by this mutation. Molecular dynamics simulations revealed identical equilibrium enzyme structures around residue 472; however, calculations indicated that the L472M mutation impacted local low-frequency dynamical COX constriction site motions by stabilizing the active site entrance and slowing constriction site dynamics. Kinetic analysis of inhibitor binding is consistent with the computational findings.
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spelling pubmed-47215282016-12-24 Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics Konkle, Mary E. Blobaum, Anna L. Moth, Christopher W. Prusakiewicz, Jeffery J. Xu, Shu Ghebreselasie, Kebreab Akingbade, Dapo Jacobs, Aaron T. Rouzer, Carol A. Lybrand, Terry P. Marnett, Lawrence J. Biochemistry [Image: see text] The cyclooxygenase enzymes (COX-1 and COX-2) are the therapeutic targets of nonsteroidal anti-inflammatory drugs (NSAIDs). Neutralization of the carboxylic acid moiety of the NSAID indomethacin to an ester or amide functionality confers COX-2 selectivity, but the molecular basis for this selectivity has not been completely revealed through mutagenesis studies and/or X-ray crystallographic attempts. We expressed and assayed a number of divergent secondary shell COX-2 active site mutants and found that a COX-2 to COX-1 change at position 472 (Leu in COX-2, Met in COX-1) reduced the potency of enzyme inhibition by a series of COX-2-selective indomethacin amides and esters. In contrast, the potencies of indomethacin, arylacetic acid, propionic acid, and COX-2-selective diarylheterocycle inhibitors were either unaffected or only mildly affected by this mutation. Molecular dynamics simulations revealed identical equilibrium enzyme structures around residue 472; however, calculations indicated that the L472M mutation impacted local low-frequency dynamical COX constriction site motions by stabilizing the active site entrance and slowing constriction site dynamics. Kinetic analysis of inhibitor binding is consistent with the computational findings. American Chemical Society 2015-12-24 2016-01-19 /pmc/articles/PMC4721528/ /pubmed/26704937 http://dx.doi.org/10.1021/acs.biochem.5b01222 Text en Copyright © 2015 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Konkle, Mary E.
Blobaum, Anna L.
Moth, Christopher W.
Prusakiewicz, Jeffery J.
Xu, Shu
Ghebreselasie, Kebreab
Akingbade, Dapo
Jacobs, Aaron T.
Rouzer, Carol A.
Lybrand, Terry P.
Marnett, Lawrence J.
Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics
title Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics
title_full Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics
title_fullStr Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics
title_full_unstemmed Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics
title_short Conservative Secondary Shell Substitution In Cyclooxygenase-2 Reduces Inhibition by Indomethacin Amides and Esters via Altered Enzyme Dynamics
title_sort conservative secondary shell substitution in cyclooxygenase-2 reduces inhibition by indomethacin amides and esters via altered enzyme dynamics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4721528/
https://www.ncbi.nlm.nih.gov/pubmed/26704937
http://dx.doi.org/10.1021/acs.biochem.5b01222
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