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Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice

Thyroid cancer comprises different clinical and histological entities. Whereas differentiated (DTCs) malignancies are sensitive to radioiodine therapy, anaplastic (ATCs) and medullary (MTCs) tumors do not uptake radioactive iodine and display aggressive features associated with a poor prognosis. Mor...

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Autores principales: Tirrò, Elena, Martorana, Federica, Romano, Chiara, Vitale, Silvia Rita, Motta, Gianmarco, Di Gregorio, Sandra, Massimino, Michele, Pennisi, Maria Stella, Stella, Stefania, Puma, Adriana, Gianì, Fiorenza, Russo, Marco, Manzella, Livia, Vigneri, Paolo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6771012/
https://www.ncbi.nlm.nih.gov/pubmed/31540307
http://dx.doi.org/10.3390/genes10090709
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author Tirrò, Elena
Martorana, Federica
Romano, Chiara
Vitale, Silvia Rita
Motta, Gianmarco
Di Gregorio, Sandra
Massimino, Michele
Pennisi, Maria Stella
Stella, Stefania
Puma, Adriana
Gianì, Fiorenza
Russo, Marco
Manzella, Livia
Vigneri, Paolo
author_facet Tirrò, Elena
Martorana, Federica
Romano, Chiara
Vitale, Silvia Rita
Motta, Gianmarco
Di Gregorio, Sandra
Massimino, Michele
Pennisi, Maria Stella
Stella, Stefania
Puma, Adriana
Gianì, Fiorenza
Russo, Marco
Manzella, Livia
Vigneri, Paolo
author_sort Tirrò, Elena
collection PubMed
description Thyroid cancer comprises different clinical and histological entities. Whereas differentiated (DTCs) malignancies are sensitive to radioiodine therapy, anaplastic (ATCs) and medullary (MTCs) tumors do not uptake radioactive iodine and display aggressive features associated with a poor prognosis. Moreover, in a majority of DTCs, disease evolution leads to the progressive loss of iodine sensitivity. Hence, iodine-refractory DTCs, along with ATCs and MTCs, require alternative treatments reflective of their different tumor biology. In the last decade, the molecular mechanisms promoting thyroid cancer development and progression have been extensively studied. This has led to a better understanding of the genomic landscape, displayed by thyroid malignancies, and to the identification of novel therapeutic targets. Indeed, several pharmacological compounds have been developed for iodine-refractory tumors, with four multi-target tyrosine kinase inhibitors already available for DTCs (sorafenib and lenvatinib) and MTCs (cabozantib and vandetanib), and a plethora of drugs currently being evaluated in clinical trials. In this review, we will describe the genomic alterations and biological processes intertwined with thyroid cancer development, also providing a thorough overview of targeted drugs already tested or under investigation for these tumors. Furthermore, given the existing preclinical evidence, we will briefly discuss the potential role of immunotherapy as an additional therapeutic strategy for the treatment of thyroid cancer.
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spelling pubmed-67710122019-10-30 Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice Tirrò, Elena Martorana, Federica Romano, Chiara Vitale, Silvia Rita Motta, Gianmarco Di Gregorio, Sandra Massimino, Michele Pennisi, Maria Stella Stella, Stefania Puma, Adriana Gianì, Fiorenza Russo, Marco Manzella, Livia Vigneri, Paolo Genes (Basel) Review Thyroid cancer comprises different clinical and histological entities. Whereas differentiated (DTCs) malignancies are sensitive to radioiodine therapy, anaplastic (ATCs) and medullary (MTCs) tumors do not uptake radioactive iodine and display aggressive features associated with a poor prognosis. Moreover, in a majority of DTCs, disease evolution leads to the progressive loss of iodine sensitivity. Hence, iodine-refractory DTCs, along with ATCs and MTCs, require alternative treatments reflective of their different tumor biology. In the last decade, the molecular mechanisms promoting thyroid cancer development and progression have been extensively studied. This has led to a better understanding of the genomic landscape, displayed by thyroid malignancies, and to the identification of novel therapeutic targets. Indeed, several pharmacological compounds have been developed for iodine-refractory tumors, with four multi-target tyrosine kinase inhibitors already available for DTCs (sorafenib and lenvatinib) and MTCs (cabozantib and vandetanib), and a plethora of drugs currently being evaluated in clinical trials. In this review, we will describe the genomic alterations and biological processes intertwined with thyroid cancer development, also providing a thorough overview of targeted drugs already tested or under investigation for these tumors. Furthermore, given the existing preclinical evidence, we will briefly discuss the potential role of immunotherapy as an additional therapeutic strategy for the treatment of thyroid cancer. MDPI 2019-09-13 /pmc/articles/PMC6771012/ /pubmed/31540307 http://dx.doi.org/10.3390/genes10090709 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 Review
Tirrò, Elena
Martorana, Federica
Romano, Chiara
Vitale, Silvia Rita
Motta, Gianmarco
Di Gregorio, Sandra
Massimino, Michele
Pennisi, Maria Stella
Stella, Stefania
Puma, Adriana
Gianì, Fiorenza
Russo, Marco
Manzella, Livia
Vigneri, Paolo
Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice
title Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice
title_full Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice
title_fullStr Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice
title_full_unstemmed Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice
title_short Molecular Alterations in Thyroid Cancer: From Bench to Clinical Practice
title_sort molecular alterations in thyroid cancer: from bench to clinical practice
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6771012/
https://www.ncbi.nlm.nih.gov/pubmed/31540307
http://dx.doi.org/10.3390/genes10090709
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