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Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer

Progesterone (Pg) and estrogen (E) receptors (PgRs and ERs) are expressed in normal and neoplastic adrenal cortex, but their role is not fully understood. In literature, Pg demonstrated cytotoxic activity on AdrenoCortical Carcinoma (ACC) cells, while tamoxifen is cytotoxic in NCI-H295R cells. Here,...

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Autores principales: Rossini, Elisa, Tamburello, Mariangela, Abate, Andrea, Beretta, Silvia, Fragni, Martina, Cominelli, Manuela, Cosentini, Deborah, Hantel, Constanze, Bono, Federica, Grisanti, Salvatore, Poliani, Pietro Luigi, Tiberio, Guido A. M., Memo, Maurizio, Sigala, Sandra, Berruti, Alfredo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8108132/
https://www.ncbi.nlm.nih.gov/pubmed/33981288
http://dx.doi.org/10.3389/fendo.2021.669426
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author Rossini, Elisa
Tamburello, Mariangela
Abate, Andrea
Beretta, Silvia
Fragni, Martina
Cominelli, Manuela
Cosentini, Deborah
Hantel, Constanze
Bono, Federica
Grisanti, Salvatore
Poliani, Pietro Luigi
Tiberio, Guido A. M.
Memo, Maurizio
Sigala, Sandra
Berruti, Alfredo
author_facet Rossini, Elisa
Tamburello, Mariangela
Abate, Andrea
Beretta, Silvia
Fragni, Martina
Cominelli, Manuela
Cosentini, Deborah
Hantel, Constanze
Bono, Federica
Grisanti, Salvatore
Poliani, Pietro Luigi
Tiberio, Guido A. M.
Memo, Maurizio
Sigala, Sandra
Berruti, Alfredo
author_sort Rossini, Elisa
collection PubMed
description Progesterone (Pg) and estrogen (E) receptors (PgRs and ERs) are expressed in normal and neoplastic adrenal cortex, but their role is not fully understood. In literature, Pg demonstrated cytotoxic activity on AdrenoCortical Carcinoma (ACC) cells, while tamoxifen is cytotoxic in NCI-H295R cells. Here, we demonstrated that in ACC cell models, ERs were expressed in NCI-H295R cells with a prevalence of ER-β over the ER-α.Metastasis-derived MUC-1 and ACC115m cells displayed a very weak ER-α/β signal, while PgR cells were expressed, although at low level. Accordingly, these latter were resistant to the SERM tamoxifen and scarcely sensitive to Pg, as we observed a lower potency compared to NCI-H295R cells in cytotoxicity (IC(50): MUC-1 cells: 67.58 µM (95%CI: 63.22–73.04), ACC115m cells: 51.76 µM (95%CI: 46.45–57.67) and cell proliferation rate. Exposure of NCI-H295R cells to tamoxifen induced cytotoxicity (IC(50): 5.43 µM (95%CI: 5.18–5.69 µM) mainly involving ER-β, as their nuclear localization increased after tamoxifen: Δ A.U. treated vs untreated: 12 h: +27.04% (p < 0.01); 24 h: +36.46% (p < 0.0001). This effect involved the SF-1 protein reduction: Pg: −36.34 ± 9.26%; tamoxifen: −46.25 ± 15.68% (p < 0.01). Finally, in a cohort of 36 ACC samples, immunohistochemistry showed undetectable/low level of ERs, while PgR demonstrated a higher expression. In conclusion, ACC experimental cell models expressed PgR and low levels of ER in line with data obtained in patient tissues, thus limiting the possibility of a clinical approach targeting ER. Interestingly, Pg exerted cytotoxicity also in metastatic ACC cells, although with low potency.
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spelling pubmed-81081322021-05-11 Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer Rossini, Elisa Tamburello, Mariangela Abate, Andrea Beretta, Silvia Fragni, Martina Cominelli, Manuela Cosentini, Deborah Hantel, Constanze Bono, Federica Grisanti, Salvatore Poliani, Pietro Luigi Tiberio, Guido A. M. Memo, Maurizio Sigala, Sandra Berruti, Alfredo Front Endocrinol (Lausanne) Endocrinology Progesterone (Pg) and estrogen (E) receptors (PgRs and ERs) are expressed in normal and neoplastic adrenal cortex, but their role is not fully understood. In literature, Pg demonstrated cytotoxic activity on AdrenoCortical Carcinoma (ACC) cells, while tamoxifen is cytotoxic in NCI-H295R cells. Here, we demonstrated that in ACC cell models, ERs were expressed in NCI-H295R cells with a prevalence of ER-β over the ER-α.Metastasis-derived MUC-1 and ACC115m cells displayed a very weak ER-α/β signal, while PgR cells were expressed, although at low level. Accordingly, these latter were resistant to the SERM tamoxifen and scarcely sensitive to Pg, as we observed a lower potency compared to NCI-H295R cells in cytotoxicity (IC(50): MUC-1 cells: 67.58 µM (95%CI: 63.22–73.04), ACC115m cells: 51.76 µM (95%CI: 46.45–57.67) and cell proliferation rate. Exposure of NCI-H295R cells to tamoxifen induced cytotoxicity (IC(50): 5.43 µM (95%CI: 5.18–5.69 µM) mainly involving ER-β, as their nuclear localization increased after tamoxifen: Δ A.U. treated vs untreated: 12 h: +27.04% (p < 0.01); 24 h: +36.46% (p < 0.0001). This effect involved the SF-1 protein reduction: Pg: −36.34 ± 9.26%; tamoxifen: −46.25 ± 15.68% (p < 0.01). Finally, in a cohort of 36 ACC samples, immunohistochemistry showed undetectable/low level of ERs, while PgR demonstrated a higher expression. In conclusion, ACC experimental cell models expressed PgR and low levels of ER in line with data obtained in patient tissues, thus limiting the possibility of a clinical approach targeting ER. Interestingly, Pg exerted cytotoxicity also in metastatic ACC cells, although with low potency. Frontiers Media S.A. 2021-04-26 /pmc/articles/PMC8108132/ /pubmed/33981288 http://dx.doi.org/10.3389/fendo.2021.669426 Text en Copyright © 2021 Rossini, Tamburello, Abate, Beretta, Fragni, Cominelli, Cosentini, Hantel, Bono, Grisanti, Poliani, Tiberio, Memo, Sigala and Berruti https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Rossini, Elisa
Tamburello, Mariangela
Abate, Andrea
Beretta, Silvia
Fragni, Martina
Cominelli, Manuela
Cosentini, Deborah
Hantel, Constanze
Bono, Federica
Grisanti, Salvatore
Poliani, Pietro Luigi
Tiberio, Guido A. M.
Memo, Maurizio
Sigala, Sandra
Berruti, Alfredo
Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer
title Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer
title_full Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer
title_fullStr Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer
title_full_unstemmed Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer
title_short Cytotoxic Effect of Progesterone, Tamoxifen and Their Combination in Experimental Cell Models of Human Adrenocortical Cancer
title_sort cytotoxic effect of progesterone, tamoxifen and their combination in experimental cell models of human adrenocortical cancer
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8108132/
https://www.ncbi.nlm.nih.gov/pubmed/33981288
http://dx.doi.org/10.3389/fendo.2021.669426
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