Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model

BRAF(V600E) mutation exerts an essential oncogenic function in many tumors, including papillary thyroid carcinoma (PTC). Although BRAF(V600E) inhibitors are available, lack of response has been frequently observed. To study the mechanism underlying intrinsic resistance to the mutant BRAF(V600E) sele...

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Autores principales: Duquette, Mark, Sadow, Peter M., Husain, Amjad, Sims, Jennifer N., Antonello, Zeus A., Fischer, Andrew H., Song, Chen, Castellanos-Rizaldos, Elena, Makrigiorgos, G. Mike, Kurebayashi, Junichi, Nose, Vania, Van Hummelen, Paul, Bronson, Roderick T., Vinco, Michelle, Giordano, Thomas J., Dias-Santagata, Dora, Pandolfi, Pier Paolo, Nucera, Carmelo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Priority Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4767444/
https://www.ncbi.nlm.nih.gov/pubmed/26636651
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author Duquette, Mark
Sadow, Peter M.
Husain, Amjad
Sims, Jennifer N.
Antonello, Zeus A.
Fischer, Andrew H.
Song, Chen
Castellanos-Rizaldos, Elena
Makrigiorgos, G. Mike
Kurebayashi, Junichi
Nose, Vania
Van Hummelen, Paul
Bronson, Roderick T.
Vinco, Michelle
Giordano, Thomas J.
Dias-Santagata, Dora
Pandolfi, Pier Paolo
Nucera, Carmelo
author_facet Duquette, Mark
Sadow, Peter M.
Husain, Amjad
Sims, Jennifer N.
Antonello, Zeus A.
Fischer, Andrew H.
Song, Chen
Castellanos-Rizaldos, Elena
Makrigiorgos, G. Mike
Kurebayashi, Junichi
Nose, Vania
Van Hummelen, Paul
Bronson, Roderick T.
Vinco, Michelle
Giordano, Thomas J.
Dias-Santagata, Dora
Pandolfi, Pier Paolo
Nucera, Carmelo
author_sort Duquette, Mark
collection PubMed
description BRAF(V600E) mutation exerts an essential oncogenic function in many tumors, including papillary thyroid carcinoma (PTC). Although BRAF(V600E) inhibitors are available, lack of response has been frequently observed. To study the mechanism underlying intrinsic resistance to the mutant BRAF(V600E) selective inhibitor vemurafenib, we established short-term primary cell cultures of human metastatic/recurrent BRAF(V600E)-PTC, intrathyroidal BRAF(V600E)-PTC, and normal thyroid (NT). We also generated an early intervention model of human BRAF(V600E)-PTC orthotopic mouse. We find that metastatic BRAF(V600E)-PTC cells elicit paracrine-signaling which trigger migration of pericytes, blood endothelial cells and lymphatic endothelial cells as compared to BRAF(WT)-PTC cells, and show a higher rate of invasion. We further show that vemurafenib therapy significantly suppresses these aberrant functions in non-metastatic BRAF(V600E)-PTC cells but lesser in metastatic BRAF(V600E)-PTC cells as compared to vehicle treatment. These results concur with similar folds of down-regulation of tumor microenvironment–associated pro-metastatic molecules, with no effects in BRAF(WT)-PTC and NT cells. Our early intervention preclinical trial shows that vemurafenib delays tumor growth in the orthotopic BRAF(WT/V600E)-PTC mice. Importantly, we identify high copy number gain of MCL1 (chromosome 1q) and loss of CDKN2A (P16, chromosome 9p) in metastatic BRAF(V600E)-PTC cells which are associated with resistance to vemurafenib treatment. Critically, we demonstrate that combined vemurafenib therapy with BCL2/MCL1 inhibitor increases metastatic BRAF(V600E)-PTC cell death and ameliorates response to vemurafenib treatment as compared to single agent treatment. In conclusion, short-term PTC and NT cultures offer a predictive model for evaluating therapeutic response in patients with PTC. Our PTC pre-clinical model suggests that combined targeted therapy might be an important therapeutic strategy for metastatic and refractory BRAF(V600E)-positive PTC.
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spelling pubmed-47674442016-03-25 Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model Duquette, Mark Sadow, Peter M. Husain, Amjad Sims, Jennifer N. Antonello, Zeus A. Fischer, Andrew H. Song, Chen Castellanos-Rizaldos, Elena Makrigiorgos, G. Mike Kurebayashi, Junichi Nose, Vania Van Hummelen, Paul Bronson, Roderick T. Vinco, Michelle Giordano, Thomas J. Dias-Santagata, Dora Pandolfi, Pier Paolo Nucera, Carmelo Oncotarget Priority Research Paper BRAF(V600E) mutation exerts an essential oncogenic function in many tumors, including papillary thyroid carcinoma (PTC). Although BRAF(V600E) inhibitors are available, lack of response has been frequently observed. To study the mechanism underlying intrinsic resistance to the mutant BRAF(V600E) selective inhibitor vemurafenib, we established short-term primary cell cultures of human metastatic/recurrent BRAF(V600E)-PTC, intrathyroidal BRAF(V600E)-PTC, and normal thyroid (NT). We also generated an early intervention model of human BRAF(V600E)-PTC orthotopic mouse. We find that metastatic BRAF(V600E)-PTC cells elicit paracrine-signaling which trigger migration of pericytes, blood endothelial cells and lymphatic endothelial cells as compared to BRAF(WT)-PTC cells, and show a higher rate of invasion. We further show that vemurafenib therapy significantly suppresses these aberrant functions in non-metastatic BRAF(V600E)-PTC cells but lesser in metastatic BRAF(V600E)-PTC cells as compared to vehicle treatment. These results concur with similar folds of down-regulation of tumor microenvironment–associated pro-metastatic molecules, with no effects in BRAF(WT)-PTC and NT cells. Our early intervention preclinical trial shows that vemurafenib delays tumor growth in the orthotopic BRAF(WT/V600E)-PTC mice. Importantly, we identify high copy number gain of MCL1 (chromosome 1q) and loss of CDKN2A (P16, chromosome 9p) in metastatic BRAF(V600E)-PTC cells which are associated with resistance to vemurafenib treatment. Critically, we demonstrate that combined vemurafenib therapy with BCL2/MCL1 inhibitor increases metastatic BRAF(V600E)-PTC cell death and ameliorates response to vemurafenib treatment as compared to single agent treatment. In conclusion, short-term PTC and NT cultures offer a predictive model for evaluating therapeutic response in patients with PTC. Our PTC pre-clinical model suggests that combined targeted therapy might be an important therapeutic strategy for metastatic and refractory BRAF(V600E)-positive PTC. Impact Journals LLC 2015-11-30 /pmc/articles/PMC4767444/ /pubmed/26636651 Text en Copyright: © 2015 Duquette 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 Priority Research Paper
Duquette, Mark
Sadow, Peter M.
Husain, Amjad
Sims, Jennifer N.
Antonello, Zeus A.
Fischer, Andrew H.
Song, Chen
Castellanos-Rizaldos, Elena
Makrigiorgos, G. Mike
Kurebayashi, Junichi
Nose, Vania
Van Hummelen, Paul
Bronson, Roderick T.
Vinco, Michelle
Giordano, Thomas J.
Dias-Santagata, Dora
Pandolfi, Pier Paolo
Nucera, Carmelo
Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model
title Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model
title_full Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model
title_fullStr Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model
title_full_unstemmed Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model
title_short Metastasis-associated MCL1 and P16 copy number alterations dictate resistance to vemurafenib in a BRAF(V600E) patient-derived papillary thyroid carcinoma preclinical model
title_sort metastasis-associated mcl1 and p16 copy number alterations dictate resistance to vemurafenib in a braf(v600e) patient-derived papillary thyroid carcinoma preclinical model
topic Priority Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4767444/
https://www.ncbi.nlm.nih.gov/pubmed/26636651
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