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Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease

To better understand the genesis of autoimmunity in Graves' disease (GD), it is essential to study the mechanism of apoptosis and cell proliferation in thyroid cells and intrathyroidal lymphocytic infiltrate of GD patients. Methods. A cross sectional, observational study performed by evaluating...

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Autores principales: de Vasconcelos, Jessica Castro, Barreto, Icléia Siqueira, Matos, Patrícia Sabino, Maia, Frederico Fernandes Ribeiro, Tambascia, Marcos Antônio, Parisi, Maria Cândida Ribeiro, Zantut-Wittmann, Denise Engelbrecht
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6029459/
https://www.ncbi.nlm.nih.gov/pubmed/30018638
http://dx.doi.org/10.1155/2018/3171280
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author de Vasconcelos, Jessica Castro
Barreto, Icléia Siqueira
Matos, Patrícia Sabino
Maia, Frederico Fernandes Ribeiro
Tambascia, Marcos Antônio
Parisi, Maria Cândida Ribeiro
Zantut-Wittmann, Denise Engelbrecht
author_facet de Vasconcelos, Jessica Castro
Barreto, Icléia Siqueira
Matos, Patrícia Sabino
Maia, Frederico Fernandes Ribeiro
Tambascia, Marcos Antônio
Parisi, Maria Cândida Ribeiro
Zantut-Wittmann, Denise Engelbrecht
author_sort de Vasconcelos, Jessica Castro
collection PubMed
description To better understand the genesis of autoimmunity in Graves' disease (GD), it is essential to study the mechanism of apoptosis and cell proliferation in thyroid cells and intrathyroidal lymphocytic infiltrate of GD patients. Methods. A cross sectional, observational study performed by evaluating histopathological samples of thyroidectomy products from GD patients using immunohistochemistry. New histological sections were prepared for immunohistochemical analysis with markers of cell proliferation, antiproliferation, apoptosis, and antiapoptosis. Results. Patients with GD who underwent radioiodine therapy (RIT) had a lower lymphocytic expression level of p27Kip1, and those who took beta-blockers had higher expression levels of BID (BH3-interacting domain) and a lower Ki-67 expression level in thyrocytes than those who did not. The association of a shorter diagnostic time with a lower expression level of MCL-1 in thyroid cells suggests that the hyperthyroid state was related to a lower antiapoptotic effect on thyrocytes. In comparison to patients with GD not using antithyroid drugs (ATD), we found a lower expression level of BID in lymphocytes for those who used ATD. Conclusion. In GD, the hyperthyroid state was associated with a lower antiapoptotic effect on thyroid cells. RIT, beta-blockers, and thionamide act by stimulating apoptosis of thyrocytes by intrathyroidal lymphocytes.
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spelling pubmed-60294592018-07-17 Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease de Vasconcelos, Jessica Castro Barreto, Icléia Siqueira Matos, Patrícia Sabino Maia, Frederico Fernandes Ribeiro Tambascia, Marcos Antônio Parisi, Maria Cândida Ribeiro Zantut-Wittmann, Denise Engelbrecht Int J Endocrinol Research Article To better understand the genesis of autoimmunity in Graves' disease (GD), it is essential to study the mechanism of apoptosis and cell proliferation in thyroid cells and intrathyroidal lymphocytic infiltrate of GD patients. Methods. A cross sectional, observational study performed by evaluating histopathological samples of thyroidectomy products from GD patients using immunohistochemistry. New histological sections were prepared for immunohistochemical analysis with markers of cell proliferation, antiproliferation, apoptosis, and antiapoptosis. Results. Patients with GD who underwent radioiodine therapy (RIT) had a lower lymphocytic expression level of p27Kip1, and those who took beta-blockers had higher expression levels of BID (BH3-interacting domain) and a lower Ki-67 expression level in thyrocytes than those who did not. The association of a shorter diagnostic time with a lower expression level of MCL-1 in thyroid cells suggests that the hyperthyroid state was related to a lower antiapoptotic effect on thyrocytes. In comparison to patients with GD not using antithyroid drugs (ATD), we found a lower expression level of BID in lymphocytes for those who used ATD. Conclusion. In GD, the hyperthyroid state was associated with a lower antiapoptotic effect on thyroid cells. RIT, beta-blockers, and thionamide act by stimulating apoptosis of thyrocytes by intrathyroidal lymphocytes. Hindawi 2018-06-19 /pmc/articles/PMC6029459/ /pubmed/30018638 http://dx.doi.org/10.1155/2018/3171280 Text en Copyright © 2018 Jessica Castro de Vasconcelos et al. http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
de Vasconcelos, Jessica Castro
Barreto, Icléia Siqueira
Matos, Patrícia Sabino
Maia, Frederico Fernandes Ribeiro
Tambascia, Marcos Antônio
Parisi, Maria Cândida Ribeiro
Zantut-Wittmann, Denise Engelbrecht
Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease
title Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease
title_full Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease
title_fullStr Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease
title_full_unstemmed Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease
title_short Value of Apoptotic, Antiapoptotic, and Cell Proliferation Markers in the Treatment of Graves' Disease
title_sort value of apoptotic, antiapoptotic, and cell proliferation markers in the treatment of graves' disease
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6029459/
https://www.ncbi.nlm.nih.gov/pubmed/30018638
http://dx.doi.org/10.1155/2018/3171280
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