Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays

BACKGROUND: Their large scaffold diversity and properties, such as structural complexity and drug similarity, form the basis of claims that natural products are ideal starting points for drug design and development. Consequently, there has been great interest in determining whether such molecules sh...

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Autores principales: Sala, Esther, Guasch, Laura, Iwaszkiewicz, Justyna, Mulero, Miquel, Salvadó, Maria-Josepa, Pinent, Montserrat, Zoete, Vincent, Grosdidier, Aurélien, Garcia-Vallvé, Santiago, Michielin, Olivier, Pujadas, Gerard
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3044726/
https://www.ncbi.nlm.nih.gov/pubmed/21390216
http://dx.doi.org/10.1371/journal.pone.0016903
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author Sala, Esther
Guasch, Laura
Iwaszkiewicz, Justyna
Mulero, Miquel
Salvadó, Maria-Josepa
Pinent, Montserrat
Zoete, Vincent
Grosdidier, Aurélien
Garcia-Vallvé, Santiago
Michielin, Olivier
Pujadas, Gerard
author_facet Sala, Esther
Guasch, Laura
Iwaszkiewicz, Justyna
Mulero, Miquel
Salvadó, Maria-Josepa
Pinent, Montserrat
Zoete, Vincent
Grosdidier, Aurélien
Garcia-Vallvé, Santiago
Michielin, Olivier
Pujadas, Gerard
author_sort Sala, Esther
collection PubMed
description BACKGROUND: Their large scaffold diversity and properties, such as structural complexity and drug similarity, form the basis of claims that natural products are ideal starting points for drug design and development. Consequently, there has been great interest in determining whether such molecules show biological activity toward protein targets of pharmacological relevance. One target of particular interest is hIKK-2, a serine-threonine protein kinase belonging to the IKK complex that is the primary component responsible for activating NF-κB in response to various inflammatory stimuli. Indeed, this has led to the development of synthetic ATP-competitive inhibitors for hIKK-2. Therefore, the main goals of this study were (a) to use virtual screening to identify potential hIKK-2 inhibitors of natural origin that compete with ATP and (b) to evaluate the reliability of our virtual-screening protocol by experimentally testing the in vitro activity of selected natural-product hits. METHODOLOGY/PRINCIPAL FINDINGS: We thus predicted that 1,061 out of the 89,425 natural products present in the studied database would inhibit hIKK-2 with good ADMET properties. Notably, when these 1,061 molecules were merged with the 98 synthetic hIKK-2 inhibitors used in this study and the resulting set was classified into ten clusters according to chemical similarity, there were three clusters that contained only natural products. Five molecules from these three clusters (for which no anti-inflammatory activity has been previously described) were then selected for in vitro activity testing, in which three out of the five molecules were shown to inhibit hIKK-2. CONCLUSIONS/SIGNIFICANCE: We demonstrated that our virtual-screening protocol was successful in identifying lead compounds for developing new inhibitors for hIKK-2, a target of great interest in medicinal chemistry. Additionally, all the tools developed during the current study (i.e., the homology model for the hIKK-2 kinase domain and the pharmacophore) will be made available to interested readers upon request.
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spelling pubmed-30447262011-03-09 Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays Sala, Esther Guasch, Laura Iwaszkiewicz, Justyna Mulero, Miquel Salvadó, Maria-Josepa Pinent, Montserrat Zoete, Vincent Grosdidier, Aurélien Garcia-Vallvé, Santiago Michielin, Olivier Pujadas, Gerard PLoS One Research Article BACKGROUND: Their large scaffold diversity and properties, such as structural complexity and drug similarity, form the basis of claims that natural products are ideal starting points for drug design and development. Consequently, there has been great interest in determining whether such molecules show biological activity toward protein targets of pharmacological relevance. One target of particular interest is hIKK-2, a serine-threonine protein kinase belonging to the IKK complex that is the primary component responsible for activating NF-κB in response to various inflammatory stimuli. Indeed, this has led to the development of synthetic ATP-competitive inhibitors for hIKK-2. Therefore, the main goals of this study were (a) to use virtual screening to identify potential hIKK-2 inhibitors of natural origin that compete with ATP and (b) to evaluate the reliability of our virtual-screening protocol by experimentally testing the in vitro activity of selected natural-product hits. METHODOLOGY/PRINCIPAL FINDINGS: We thus predicted that 1,061 out of the 89,425 natural products present in the studied database would inhibit hIKK-2 with good ADMET properties. Notably, when these 1,061 molecules were merged with the 98 synthetic hIKK-2 inhibitors used in this study and the resulting set was classified into ten clusters according to chemical similarity, there were three clusters that contained only natural products. Five molecules from these three clusters (for which no anti-inflammatory activity has been previously described) were then selected for in vitro activity testing, in which three out of the five molecules were shown to inhibit hIKK-2. CONCLUSIONS/SIGNIFICANCE: We demonstrated that our virtual-screening protocol was successful in identifying lead compounds for developing new inhibitors for hIKK-2, a target of great interest in medicinal chemistry. Additionally, all the tools developed during the current study (i.e., the homology model for the hIKK-2 kinase domain and the pharmacophore) will be made available to interested readers upon request. Public Library of Science 2011-02-24 /pmc/articles/PMC3044726/ /pubmed/21390216 http://dx.doi.org/10.1371/journal.pone.0016903 Text en Sala et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Sala, Esther
Guasch, Laura
Iwaszkiewicz, Justyna
Mulero, Miquel
Salvadó, Maria-Josepa
Pinent, Montserrat
Zoete, Vincent
Grosdidier, Aurélien
Garcia-Vallvé, Santiago
Michielin, Olivier
Pujadas, Gerard
Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays
title Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays
title_full Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays
title_fullStr Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays
title_full_unstemmed Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays
title_short Identification of Human IKK-2 Inhibitors of Natural Origin (Part I): Modeling of the IKK-2 Kinase Domain, Virtual Screening and Activity Assays
title_sort identification of human ikk-2 inhibitors of natural origin (part i): modeling of the ikk-2 kinase domain, virtual screening and activity assays
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3044726/
https://www.ncbi.nlm.nih.gov/pubmed/21390216
http://dx.doi.org/10.1371/journal.pone.0016903
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