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Progress towards a public chemogenomic set for protein kinases and a call for contributions

Protein kinases are highly tractable targets for drug discovery. However, the biological function and therapeutic potential of the majority of the 500+ human protein kinases remains unknown. We have developed physical and virtual collections of small molecule inhibitors, which we call chemogenomic s...

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Autores principales: Drewry, David H., Wells, Carrow I., Andrews, David M., Angell, Richard, Al-Ali, Hassan, Axtman, Alison D., Capuzzi, Stephen J., Elkins, Jonathan M., Ettmayer, Peter, Frederiksen, Mathias, Gileadi, Opher, Gray, Nathanael, Hooper, Alice, Knapp, Stefan, Laufer, Stefan, Luecking, Ulrich, Michaelides, Michael, Müller, Susanne, Muratov, Eugene, Denny, R. Aldrin, Saikatendu, Kumar S., Treiber, Daniel K., Zuercher, William J., Willson, Timothy M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5540273/
https://www.ncbi.nlm.nih.gov/pubmed/28767711
http://dx.doi.org/10.1371/journal.pone.0181585
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author Drewry, David H.
Wells, Carrow I.
Andrews, David M.
Angell, Richard
Al-Ali, Hassan
Axtman, Alison D.
Capuzzi, Stephen J.
Elkins, Jonathan M.
Ettmayer, Peter
Frederiksen, Mathias
Gileadi, Opher
Gray, Nathanael
Hooper, Alice
Knapp, Stefan
Laufer, Stefan
Luecking, Ulrich
Michaelides, Michael
Müller, Susanne
Muratov, Eugene
Denny, R. Aldrin
Saikatendu, Kumar S.
Treiber, Daniel K.
Zuercher, William J.
Willson, Timothy M.
author_facet Drewry, David H.
Wells, Carrow I.
Andrews, David M.
Angell, Richard
Al-Ali, Hassan
Axtman, Alison D.
Capuzzi, Stephen J.
Elkins, Jonathan M.
Ettmayer, Peter
Frederiksen, Mathias
Gileadi, Opher
Gray, Nathanael
Hooper, Alice
Knapp, Stefan
Laufer, Stefan
Luecking, Ulrich
Michaelides, Michael
Müller, Susanne
Muratov, Eugene
Denny, R. Aldrin
Saikatendu, Kumar S.
Treiber, Daniel K.
Zuercher, William J.
Willson, Timothy M.
author_sort Drewry, David H.
collection PubMed
description Protein kinases are highly tractable targets for drug discovery. However, the biological function and therapeutic potential of the majority of the 500+ human protein kinases remains unknown. We have developed physical and virtual collections of small molecule inhibitors, which we call chemogenomic sets, that are designed to inhibit the catalytic function of almost half the human protein kinases. In this manuscript we share our progress towards generation of a comprehensive kinase chemogenomic set (KCGS), release kinome profiling data of a large inhibitor set (Published Kinase Inhibitor Set 2 (PKIS2)), and outline a process through which the community can openly collaborate to create a KCGS that probes the full complement of human protein kinases.
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spelling pubmed-55402732017-08-12 Progress towards a public chemogenomic set for protein kinases and a call for contributions Drewry, David H. Wells, Carrow I. Andrews, David M. Angell, Richard Al-Ali, Hassan Axtman, Alison D. Capuzzi, Stephen J. Elkins, Jonathan M. Ettmayer, Peter Frederiksen, Mathias Gileadi, Opher Gray, Nathanael Hooper, Alice Knapp, Stefan Laufer, Stefan Luecking, Ulrich Michaelides, Michael Müller, Susanne Muratov, Eugene Denny, R. Aldrin Saikatendu, Kumar S. Treiber, Daniel K. Zuercher, William J. Willson, Timothy M. PLoS One Research Article Protein kinases are highly tractable targets for drug discovery. However, the biological function and therapeutic potential of the majority of the 500+ human protein kinases remains unknown. We have developed physical and virtual collections of small molecule inhibitors, which we call chemogenomic sets, that are designed to inhibit the catalytic function of almost half the human protein kinases. In this manuscript we share our progress towards generation of a comprehensive kinase chemogenomic set (KCGS), release kinome profiling data of a large inhibitor set (Published Kinase Inhibitor Set 2 (PKIS2)), and outline a process through which the community can openly collaborate to create a KCGS that probes the full complement of human protein kinases. Public Library of Science 2017-08-02 /pmc/articles/PMC5540273/ /pubmed/28767711 http://dx.doi.org/10.1371/journal.pone.0181585 Text en © 2017 Drewry 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Drewry, David H.
Wells, Carrow I.
Andrews, David M.
Angell, Richard
Al-Ali, Hassan
Axtman, Alison D.
Capuzzi, Stephen J.
Elkins, Jonathan M.
Ettmayer, Peter
Frederiksen, Mathias
Gileadi, Opher
Gray, Nathanael
Hooper, Alice
Knapp, Stefan
Laufer, Stefan
Luecking, Ulrich
Michaelides, Michael
Müller, Susanne
Muratov, Eugene
Denny, R. Aldrin
Saikatendu, Kumar S.
Treiber, Daniel K.
Zuercher, William J.
Willson, Timothy M.
Progress towards a public chemogenomic set for protein kinases and a call for contributions
title Progress towards a public chemogenomic set for protein kinases and a call for contributions
title_full Progress towards a public chemogenomic set for protein kinases and a call for contributions
title_fullStr Progress towards a public chemogenomic set for protein kinases and a call for contributions
title_full_unstemmed Progress towards a public chemogenomic set for protein kinases and a call for contributions
title_short Progress towards a public chemogenomic set for protein kinases and a call for contributions
title_sort progress towards a public chemogenomic set for protein kinases and a call for contributions
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5540273/
https://www.ncbi.nlm.nih.gov/pubmed/28767711
http://dx.doi.org/10.1371/journal.pone.0181585
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