Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies

Kinase-targeted therapies have the potential to improve the survival of patients with cancer. However, the cancer-specific spectrum of kinase alterations exhibits distinct functional properties and requires mutation-oriented drug treatments. Besides post-translational modifications and diverse inter...

Descripción completa

Detalles Bibliográficos
Autores principales: Mayrhofer, Johanna E., Enzler, Florian, Feichtner, Andreas, Röck, Ruth, Fleischmann, Jakob, Raffeiner, Andrea, Tschaikner, Philipp, Ogris, Egon, Huber, Roland G., Hartl, Markus, Schneider, Rainer, Troppmair, Jakob, Torres-Quesada, Omar, Stefan, Eduard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: National Academy of Sciences 2020
Materias:
Biological Sciences
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7733820/
https://www.ncbi.nlm.nih.gov/pubmed/33229534
http://dx.doi.org/10.1073/pnas.2012150117
_version_ 1783622347241029632
author Mayrhofer, Johanna E.
Enzler, Florian
Feichtner, Andreas
Röck, Ruth
Fleischmann, Jakob
Raffeiner, Andrea
Tschaikner, Philipp
Ogris, Egon
Huber, Roland G.
Hartl, Markus
Schneider, Rainer
Troppmair, Jakob
Torres-Quesada, Omar
Stefan, Eduard
author_facet Mayrhofer, Johanna E.
Enzler, Florian
Feichtner, Andreas
Röck, Ruth
Fleischmann, Jakob
Raffeiner, Andrea
Tschaikner, Philipp
Ogris, Egon
Huber, Roland G.
Hartl, Markus
Schneider, Rainer
Troppmair, Jakob
Torres-Quesada, Omar
Stefan, Eduard
author_sort Mayrhofer, Johanna E.
collection PubMed
description Kinase-targeted therapies have the potential to improve the survival of patients with cancer. However, the cancer-specific spectrum of kinase alterations exhibits distinct functional properties and requires mutation-oriented drug treatments. Besides post-translational modifications and diverse intermolecular interactions of kinases, it is the distinct disease mutation which reshapes full-length kinase conformations, affecting their activity. Oncokinase mutation profiles differ between cancer types, as it was shown for BRAF in melanoma and non–small-cell lung cancers. Here, we present the target-oriented application of a kinase conformation (KinCon) reporter platform for live-cell measurements of autoinhibitory kinase activity states. The bioluminescence-based KinCon biosensor allows the tracking of conformation dynamics of full-length kinases in intact cells and real time. We show that the most frequent BRAF cancer mutations affect kinase conformations and thus the engagement and efficacy of V600E-specific BRAF inhibitors (BRAFi). We illustrate that the patient mutation harboring KinCon reporters display differences in the effectiveness of the three clinically approved BRAFi vemurafenib, encorafenib, and dabrafenib and the preclinical paradox breaker PLX8394. We confirmed KinCon-based drug efficacy predictions for BRAF mutations other than V600E in proliferation assays using patient-derived lung cancer cell lines and by analyzing downstream kinase signaling. The systematic implementation of such conformation reporters will allow to accelerate the decision process for the mutation-oriented RAF-kinase cancer therapy. Moreover, we illustrate that the presented kinase reporter concept can be extended to other kinases which harbor patient mutations. Overall, KinCon profiling provides additional mechanistic insights into full-length kinase functions by reporting protein–protein interaction (PPI)-dependent, mutation-specific, and drug-driven changes of kinase activity conformations.
format Online
Article
Text
id pubmed-7733820
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher National Academy of Sciences
record_format MEDLINE/PubMed
spelling pubmed-77338202020-12-21 Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies Mayrhofer, Johanna E. Enzler, Florian Feichtner, Andreas Röck, Ruth Fleischmann, Jakob Raffeiner, Andrea Tschaikner, Philipp Ogris, Egon Huber, Roland G. Hartl, Markus Schneider, Rainer Troppmair, Jakob Torres-Quesada, Omar Stefan, Eduard Proc Natl Acad Sci U S A Biological Sciences Kinase-targeted therapies have the potential to improve the survival of patients with cancer. However, the cancer-specific spectrum of kinase alterations exhibits distinct functional properties and requires mutation-oriented drug treatments. Besides post-translational modifications and diverse intermolecular interactions of kinases, it is the distinct disease mutation which reshapes full-length kinase conformations, affecting their activity. Oncokinase mutation profiles differ between cancer types, as it was shown for BRAF in melanoma and non–small-cell lung cancers. Here, we present the target-oriented application of a kinase conformation (KinCon) reporter platform for live-cell measurements of autoinhibitory kinase activity states. The bioluminescence-based KinCon biosensor allows the tracking of conformation dynamics of full-length kinases in intact cells and real time. We show that the most frequent BRAF cancer mutations affect kinase conformations and thus the engagement and efficacy of V600E-specific BRAF inhibitors (BRAFi). We illustrate that the patient mutation harboring KinCon reporters display differences in the effectiveness of the three clinically approved BRAFi vemurafenib, encorafenib, and dabrafenib and the preclinical paradox breaker PLX8394. We confirmed KinCon-based drug efficacy predictions for BRAF mutations other than V600E in proliferation assays using patient-derived lung cancer cell lines and by analyzing downstream kinase signaling. The systematic implementation of such conformation reporters will allow to accelerate the decision process for the mutation-oriented RAF-kinase cancer therapy. Moreover, we illustrate that the presented kinase reporter concept can be extended to other kinases which harbor patient mutations. Overall, KinCon profiling provides additional mechanistic insights into full-length kinase functions by reporting protein–protein interaction (PPI)-dependent, mutation-specific, and drug-driven changes of kinase activity conformations. National Academy of Sciences 2020-12-08 2020-11-23 /pmc/articles/PMC7733820/ /pubmed/33229534 http://dx.doi.org/10.1073/pnas.2012150117 Text en Copyright © 2020 the Author(s). Published by PNAS. https://creativecommons.org/licenses/by-nc-nd/4.0/ https://creativecommons.org/licenses/by-nc-nd/4.0/This open access article is distributed under Creative Commons Attribution-NonCommercial-NoDerivatives License 4.0 (CC BY-NC-ND) (https://creativecommons.org/licenses/by-nc-nd/4.0/) .
spellingShingle Biological Sciences
Mayrhofer, Johanna E.
Enzler, Florian
Feichtner, Andreas
Röck, Ruth
Fleischmann, Jakob
Raffeiner, Andrea
Tschaikner, Philipp
Ogris, Egon
Huber, Roland G.
Hartl, Markus
Schneider, Rainer
Troppmair, Jakob
Torres-Quesada, Omar
Stefan, Eduard
Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies
title Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies
title_full Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies
title_fullStr Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies
title_full_unstemmed Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies
title_short Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies
title_sort mutation-oriented profiling of autoinhibitory kinase conformations predicts raf inhibitor efficacies
topic Biological Sciences
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7733820/
https://www.ncbi.nlm.nih.gov/pubmed/33229534
http://dx.doi.org/10.1073/pnas.2012150117
work_keys_str_mv AT mayrhoferjohannae mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT enzlerflorian mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT feichtnerandreas mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT rockruth mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT fleischmannjakob mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT raffeinerandrea mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT tschaiknerphilipp mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT ogrisegon mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT huberrolandg mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT hartlmarkus mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT schneiderrainer mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT troppmairjakob mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT torresquesadaomar mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies
AT stefaneduard mutationorientedprofilingofautoinhibitorykinaseconformationspredictsrafinhibitorefficacies

Ejemplares similares