Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use

The anti-proliferative activities of all twenty-five targeted kinase inhibitor drugs that are in clinical use were measured in two large assay panels: (1) a panel of proliferation assays of forty-four human cancer cell lines from diverse tumour tissue origins; and (2) a panel of more than 300 kinase...

Descripción completa

Detalles Bibliográficos
Autores principales: Uitdehaag, Joost C. M., de Roos, Jeroen A. D. M., van Doornmalen, Antoon M., Prinsen, Martine B. W., de Man, Jos, Tanizawa, Yoshinori, Kawase, Yusuke, Yoshino, Kohichiro, Buijsman, Rogier C., Zaman, Guido J. R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3961306/
https://www.ncbi.nlm.nih.gov/pubmed/24651269
http://dx.doi.org/10.1371/journal.pone.0092146
_version_ 1782308274136154112
author Uitdehaag, Joost C. M.
de Roos, Jeroen A. D. M.
van Doornmalen, Antoon M.
Prinsen, Martine B. W.
de Man, Jos
Tanizawa, Yoshinori
Kawase, Yusuke
Yoshino, Kohichiro
Buijsman, Rogier C.
Zaman, Guido J. R.
author_facet Uitdehaag, Joost C. M.
de Roos, Jeroen A. D. M.
van Doornmalen, Antoon M.
Prinsen, Martine B. W.
de Man, Jos
Tanizawa, Yoshinori
Kawase, Yusuke
Yoshino, Kohichiro
Buijsman, Rogier C.
Zaman, Guido J. R.
author_sort Uitdehaag, Joost C. M.
collection PubMed
description The anti-proliferative activities of all twenty-five targeted kinase inhibitor drugs that are in clinical use were measured in two large assay panels: (1) a panel of proliferation assays of forty-four human cancer cell lines from diverse tumour tissue origins; and (2) a panel of more than 300 kinase enzyme activity assays. This study provides a head-on comparison of all kinase inhibitor drugs in use (status Nov. 2013), and for six of these drugs, the first kinome profiling data in the public domain. Correlation of drug activities with cancer gene mutations revealed novel drug sensitivity markers, suggesting that cancers dependent on mutant CTNNB1 will respond to trametinib and other MEK inhibitors, and cancers dependent on SMAD4 to small molecule EGFR inhibitor drugs. Comparison of cellular targeting efficacies reveals the most targeted inhibitors for EGFR, ABL1 and BRAF(V600E)-driven cell growth, and demonstrates that the best targeted agents combine high biochemical potency with good selectivity. For ABL1 inhibitors, we computationally deduce optimized kinase profiles for use in a next generation of drugs. Our study shows the power of combining biochemical and cellular profiling data in the evaluation of kinase inhibitor drug action.
format Online
Article
Text
id pubmed-3961306
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-39613062014-03-27 Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use Uitdehaag, Joost C. M. de Roos, Jeroen A. D. M. van Doornmalen, Antoon M. Prinsen, Martine B. W. de Man, Jos Tanizawa, Yoshinori Kawase, Yusuke Yoshino, Kohichiro Buijsman, Rogier C. Zaman, Guido J. R. PLoS One Research Article The anti-proliferative activities of all twenty-five targeted kinase inhibitor drugs that are in clinical use were measured in two large assay panels: (1) a panel of proliferation assays of forty-four human cancer cell lines from diverse tumour tissue origins; and (2) a panel of more than 300 kinase enzyme activity assays. This study provides a head-on comparison of all kinase inhibitor drugs in use (status Nov. 2013), and for six of these drugs, the first kinome profiling data in the public domain. Correlation of drug activities with cancer gene mutations revealed novel drug sensitivity markers, suggesting that cancers dependent on mutant CTNNB1 will respond to trametinib and other MEK inhibitors, and cancers dependent on SMAD4 to small molecule EGFR inhibitor drugs. Comparison of cellular targeting efficacies reveals the most targeted inhibitors for EGFR, ABL1 and BRAF(V600E)-driven cell growth, and demonstrates that the best targeted agents combine high biochemical potency with good selectivity. For ABL1 inhibitors, we computationally deduce optimized kinase profiles for use in a next generation of drugs. Our study shows the power of combining biochemical and cellular profiling data in the evaluation of kinase inhibitor drug action. Public Library of Science 2014-03-20 /pmc/articles/PMC3961306/ /pubmed/24651269 http://dx.doi.org/10.1371/journal.pone.0092146 Text en © 2014 Uitdehaag 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
Uitdehaag, Joost C. M.
de Roos, Jeroen A. D. M.
van Doornmalen, Antoon M.
Prinsen, Martine B. W.
de Man, Jos
Tanizawa, Yoshinori
Kawase, Yusuke
Yoshino, Kohichiro
Buijsman, Rogier C.
Zaman, Guido J. R.
Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use
title Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use
title_full Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use
title_fullStr Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use
title_full_unstemmed Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use
title_short Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use
title_sort comparison of the cancer gene targeting and biochemical selectivities of all targeted kinase inhibitors approved for clinical use
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3961306/
https://www.ncbi.nlm.nih.gov/pubmed/24651269
http://dx.doi.org/10.1371/journal.pone.0092146
work_keys_str_mv AT uitdehaagjoostcm comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT deroosjeroenadm comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT vandoornmalenantoonm comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT prinsenmartinebw comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT demanjos comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT tanizawayoshinori comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT kawaseyusuke comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT yoshinokohichiro comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT buijsmanrogierc comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse
AT zamanguidojr comparisonofthecancergenetargetingandbiochemicalselectivitiesofalltargetedkinaseinhibitorsapprovedforclinicaluse

Ejemplares similares