Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use

Frequent genetic alterations discovered in FGFRs and evidence implicating some as drivers in diverse tumors has been accompanied by rapid progress in targeting FGFRs for anticancer treatments. Wider assessment of the impact of genetic changes on the activation state and drug responses is needed to b...

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Autores principales: Patani, Harshnira, Bunney, Tom D., Thiyagarajan, Nethaji, Norman, Richard A., Ogg, Derek, Breed, Jason, Ashford, Paul, Potterton, Andrew, Edwards, Mina, Williams, Sarah V., Thomson, Gary S., Pang, Camilla S.M., Knowles, Margaret A., Breeze, Alexander L., Orengo, Christine, Phillips, Chris, Katan, Matilda
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5029699/
https://www.ncbi.nlm.nih.gov/pubmed/26992226
http://dx.doi.org/10.18632/oncotarget.8132
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author Patani, Harshnira
Bunney, Tom D.
Thiyagarajan, Nethaji
Norman, Richard A.
Ogg, Derek
Breed, Jason
Ashford, Paul
Potterton, Andrew
Edwards, Mina
Williams, Sarah V.
Thomson, Gary S.
Pang, Camilla S.M.
Knowles, Margaret A.
Breeze, Alexander L.
Orengo, Christine
Phillips, Chris
Katan, Matilda
author_facet Patani, Harshnira
Bunney, Tom D.
Thiyagarajan, Nethaji
Norman, Richard A.
Ogg, Derek
Breed, Jason
Ashford, Paul
Potterton, Andrew
Edwards, Mina
Williams, Sarah V.
Thomson, Gary S.
Pang, Camilla S.M.
Knowles, Margaret A.
Breeze, Alexander L.
Orengo, Christine
Phillips, Chris
Katan, Matilda
author_sort Patani, Harshnira
collection PubMed
description Frequent genetic alterations discovered in FGFRs and evidence implicating some as drivers in diverse tumors has been accompanied by rapid progress in targeting FGFRs for anticancer treatments. Wider assessment of the impact of genetic changes on the activation state and drug responses is needed to better link the genomic data and treatment options. We here apply a direct comparative and comprehensive analysis of FGFR3 kinase domain variants representing the diversity of point-mutations reported in this domain. We reinforce the importance of N540K and K650E and establish that not all highly activating mutations (for example R669G) occur at high-frequency and conversely, that some “hotspots” may not be linked to activation. Further structural characterization consolidates a mechanistic view of FGFR kinase activation and extends insights into drug binding. Importantly, using several inhibitors of particular clinical interest (AZD4547, BGJ-398, TKI258, JNJ42756493 and AP24534), we find that some activating mutations (including different replacements of the same residue) result in distinct changes in their efficacy. Considering that there is no approved inhibitor for anticancer treatments based on FGFR-targeting, this information will be immediately translatable to ongoing clinical trials.
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spelling pubmed-50296992016-09-29 Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use Patani, Harshnira Bunney, Tom D. Thiyagarajan, Nethaji Norman, Richard A. Ogg, Derek Breed, Jason Ashford, Paul Potterton, Andrew Edwards, Mina Williams, Sarah V. Thomson, Gary S. Pang, Camilla S.M. Knowles, Margaret A. Breeze, Alexander L. Orengo, Christine Phillips, Chris Katan, Matilda Oncotarget Research Paper Frequent genetic alterations discovered in FGFRs and evidence implicating some as drivers in diverse tumors has been accompanied by rapid progress in targeting FGFRs for anticancer treatments. Wider assessment of the impact of genetic changes on the activation state and drug responses is needed to better link the genomic data and treatment options. We here apply a direct comparative and comprehensive analysis of FGFR3 kinase domain variants representing the diversity of point-mutations reported in this domain. We reinforce the importance of N540K and K650E and establish that not all highly activating mutations (for example R669G) occur at high-frequency and conversely, that some “hotspots” may not be linked to activation. Further structural characterization consolidates a mechanistic view of FGFR kinase activation and extends insights into drug binding. Importantly, using several inhibitors of particular clinical interest (AZD4547, BGJ-398, TKI258, JNJ42756493 and AP24534), we find that some activating mutations (including different replacements of the same residue) result in distinct changes in their efficacy. Considering that there is no approved inhibitor for anticancer treatments based on FGFR-targeting, this information will be immediately translatable to ongoing clinical trials. Impact Journals LLC 2016-03-16 /pmc/articles/PMC5029699/ /pubmed/26992226 http://dx.doi.org/10.18632/oncotarget.8132 Text en Copyright: © 2016 Patani et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
Patani, Harshnira
Bunney, Tom D.
Thiyagarajan, Nethaji
Norman, Richard A.
Ogg, Derek
Breed, Jason
Ashford, Paul
Potterton, Andrew
Edwards, Mina
Williams, Sarah V.
Thomson, Gary S.
Pang, Camilla S.M.
Knowles, Margaret A.
Breeze, Alexander L.
Orengo, Christine
Phillips, Chris
Katan, Matilda
Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use
title Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use
title_full Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use
title_fullStr Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use
title_full_unstemmed Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use
title_short Landscape of activating cancer mutations in FGFR kinases and their differential responses to inhibitors in clinical use
title_sort landscape of activating cancer mutations in fgfr kinases and their differential responses to inhibitors in clinical use
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5029699/
https://www.ncbi.nlm.nih.gov/pubmed/26992226
http://dx.doi.org/10.18632/oncotarget.8132
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