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The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes
In comparison to other human cancer types, malignant melanoma exhibits the greatest amount of heterogeneity. After DNA-based detection of the BRAF V600E mutation in melanoma patients, targeted inhibitor treatment is the current recommendation. This approach, however, does not take the abundance of t...
Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
MDPI
2019
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6966659/ https://www.ncbi.nlm.nih.gov/pubmed/31835364 http://dx.doi.org/10.3390/cancers11121981 |
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author | Betancourt, Lazaro Hiram Szasz, A. Marcell Kuras, Magdalena Rodriguez Murillo, Jimmy Sugihara, Yutaka Pla, Indira Horvath, Zsolt Pawłowski, Krzysztof Rezeli, Melinda Miharada, Kenichi Gil, Jeovanis Eriksson, Jonatan Appelqvist, Roger Miliotis, Tasso Baldetorp, Bo Ingvar, Christian Olsson, Håkan Lundgren, Lotta Horvatovich, Peter Welinder, Charlotte Wieslander, Elisabet Kwon, Ho Jeong Malm, Johan Nemeth, Istvan Balazs Jönsson, Göran Fenyö, David Sanchez, Aniel Marko-Varga, György |
author_facet | Betancourt, Lazaro Hiram Szasz, A. Marcell Kuras, Magdalena Rodriguez Murillo, Jimmy Sugihara, Yutaka Pla, Indira Horvath, Zsolt Pawłowski, Krzysztof Rezeli, Melinda Miharada, Kenichi Gil, Jeovanis Eriksson, Jonatan Appelqvist, Roger Miliotis, Tasso Baldetorp, Bo Ingvar, Christian Olsson, Håkan Lundgren, Lotta Horvatovich, Peter Welinder, Charlotte Wieslander, Elisabet Kwon, Ho Jeong Malm, Johan Nemeth, Istvan Balazs Jönsson, Göran Fenyö, David Sanchez, Aniel Marko-Varga, György |
author_sort | Betancourt, Lazaro Hiram |
collection | PubMed |
description | In comparison to other human cancer types, malignant melanoma exhibits the greatest amount of heterogeneity. After DNA-based detection of the BRAF V600E mutation in melanoma patients, targeted inhibitor treatment is the current recommendation. This approach, however, does not take the abundance of the therapeutic target, i.e., the B-raf V600E protein, into consideration. As shown by immunohistochemistry, the protein expression profiles of metastatic melanomas clearly reveal the existence of inter- and intra-tumor variability. Nevertheless, the technique is only semi-quantitative. To quantitate the mutant protein there is a fundamental need for more precise techniques that are aimed at defining the currently non-existent link between the levels of the target protein and subsequent drug efficacy. Using cutting-edge mass spectrometry combined with DNA and mRNA sequencing, the mutated B-raf protein within metastatic tumors was quantitated for the first time. B-raf V600E protein analysis revealed a subjacent layer of heterogeneity for mutation-positive metastatic melanomas. These were characterized into two distinct groups with different tumor morphologies, protein profiles and patient clinical outcomes. This study provides evidence that a higher level of expression in the mutated protein is associated with a more aggressive tumor progression. Our study design, comprised of surgical isolation of tumors, histopathological characterization, tissue biobanking, and protein analysis, may enable the eventual delineation of patient responders/non-responders and subsequent therapy for malignant melanoma. |
format | Online Article Text |
id | pubmed-6966659 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2019 |
publisher | MDPI |
record_format | MEDLINE/PubMed |
spelling | pubmed-69666592020-02-04 The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes Betancourt, Lazaro Hiram Szasz, A. Marcell Kuras, Magdalena Rodriguez Murillo, Jimmy Sugihara, Yutaka Pla, Indira Horvath, Zsolt Pawłowski, Krzysztof Rezeli, Melinda Miharada, Kenichi Gil, Jeovanis Eriksson, Jonatan Appelqvist, Roger Miliotis, Tasso Baldetorp, Bo Ingvar, Christian Olsson, Håkan Lundgren, Lotta Horvatovich, Peter Welinder, Charlotte Wieslander, Elisabet Kwon, Ho Jeong Malm, Johan Nemeth, Istvan Balazs Jönsson, Göran Fenyö, David Sanchez, Aniel Marko-Varga, György Cancers (Basel) Article In comparison to other human cancer types, malignant melanoma exhibits the greatest amount of heterogeneity. After DNA-based detection of the BRAF V600E mutation in melanoma patients, targeted inhibitor treatment is the current recommendation. This approach, however, does not take the abundance of the therapeutic target, i.e., the B-raf V600E protein, into consideration. As shown by immunohistochemistry, the protein expression profiles of metastatic melanomas clearly reveal the existence of inter- and intra-tumor variability. Nevertheless, the technique is only semi-quantitative. To quantitate the mutant protein there is a fundamental need for more precise techniques that are aimed at defining the currently non-existent link between the levels of the target protein and subsequent drug efficacy. Using cutting-edge mass spectrometry combined with DNA and mRNA sequencing, the mutated B-raf protein within metastatic tumors was quantitated for the first time. B-raf V600E protein analysis revealed a subjacent layer of heterogeneity for mutation-positive metastatic melanomas. These were characterized into two distinct groups with different tumor morphologies, protein profiles and patient clinical outcomes. This study provides evidence that a higher level of expression in the mutated protein is associated with a more aggressive tumor progression. Our study design, comprised of surgical isolation of tumors, histopathological characterization, tissue biobanking, and protein analysis, may enable the eventual delineation of patient responders/non-responders and subsequent therapy for malignant melanoma. MDPI 2019-12-09 /pmc/articles/PMC6966659/ /pubmed/31835364 http://dx.doi.org/10.3390/cancers11121981 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/). |
spellingShingle | Article Betancourt, Lazaro Hiram Szasz, A. Marcell Kuras, Magdalena Rodriguez Murillo, Jimmy Sugihara, Yutaka Pla, Indira Horvath, Zsolt Pawłowski, Krzysztof Rezeli, Melinda Miharada, Kenichi Gil, Jeovanis Eriksson, Jonatan Appelqvist, Roger Miliotis, Tasso Baldetorp, Bo Ingvar, Christian Olsson, Håkan Lundgren, Lotta Horvatovich, Peter Welinder, Charlotte Wieslander, Elisabet Kwon, Ho Jeong Malm, Johan Nemeth, Istvan Balazs Jönsson, Göran Fenyö, David Sanchez, Aniel Marko-Varga, György The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes |
title | The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes |
title_full | The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes |
title_fullStr | The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes |
title_full_unstemmed | The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes |
title_short | The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma—Association with Clinical Outcome and Tumor Phenotypes |
title_sort | hidden story of heterogeneous b-raf v600e mutation quantitative protein expression in metastatic melanoma—association with clinical outcome and tumor phenotypes |
topic | Article |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6966659/ https://www.ncbi.nlm.nih.gov/pubmed/31835364 http://dx.doi.org/10.3390/cancers11121981 |
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