Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.

Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.

Estrogen receptors (ER), namely ERα and ERβ, are hormone-activated transcription factors with an important role in carcinogenesis. In the present study, we aimed at elucidating the implication of ERα in skin cancer, using chemically-induced mouse skin tumours, as well as cell lines representing dist...

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Autores principales: Stella Logotheti, Dimitra Papaevangeliou, Ioannis Michalopoulos, Maria Sideridou, Katerina Tsimaratou, Ioannis Christodoulou, Katerina Pyrillou, Vassilis Gorgoulis, Spiros Vlahopoulos, Vassilis Zoumpourlis
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Publicado: Public Library of Science (PLoS) 2012
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spelling oai:doaj.org-article:866cb55984d54136a886fcc3e806aa392021-11-18T07:09:51ZProgression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.1932-620310.1371/journal.pone.0041957https://doaj.org/article/866cb55984d54136a886fcc3e806aa392012-01-01T00:00:00Zhttps://www.ncbi.nlm.nih.gov/pmc/articles/pmid/22870269/pdf/?tool=EBIhttps://doaj.org/toc/1932-6203Estrogen receptors (ER), namely ERα and ERβ, are hormone-activated transcription factors with an important role in carcinogenesis. In the present study, we aimed at elucidating the implication of ERα in skin cancer, using chemically-induced mouse skin tumours, as well as cell lines representing distinct stages of mouse skin oncogenesis. First, using immunohistochemical staining we showed that ERα is markedly increased in aggressive mouse skin tumours in vivo as compared to the papilloma tumours, whereas ERβ levels are low and become even lower in the aggressive spindle tumours of carcinogen-treated mice. Then, using the multistage mouse skin carcinogenesis model, we showed that ERα gradually increases during promotion and progression stages of mouse skin carcinogenesis, peaking at the most aggressive stage, whereas ERβ levels only slightly change throughout skin carcinogenesis. Stable transfection of the aggressive, spindle CarB cells with a dominant negative form of ERα (dnERα) resulted in reduced ERα levels and reduced binding to estrogen responsive elements (ERE)-containing sequences. We characterized two highly conserved EREs on the mouse ERα promoter through which dnERα decreased endogenous ERα levels. The dnERα-transfected CarB cells presented altered protein levels of cytoskeletal and cell adhesion molecules, slower growth rate and impaired anchorage-independent growth in vitro, whereas they gave smaller tumours with extended latency period of tumour onset in vivo. Our findings suggest an implication of ERα in the aggressiveness of spindle mouse skin cancer cells, possibly through regulation of genes affecting cell shape and adhesion, and they also provide hints for the effective targeting of spindle cancer cells by dnERα.Stella LogothetiDimitra PapaevangeliouIoannis MichalopoulosMaria SideridouKaterina TsimaratouIoannis ChristodoulouKaterina PyrillouVassilis GorgoulisSpiros VlahopoulosVassilis ZoumpourlisPublic Library of Science (PLoS)articleMedicineRScienceQENPLoS ONE, Vol 7, Iss 8, p e41957 (2012)
institution DOAJ
collection DOAJ
language EN
topic Medicine
R
Science
Q
spellingShingle Medicine
R
Science
Q
Stella Logotheti
Dimitra Papaevangeliou
Ioannis Michalopoulos
Maria Sideridou
Katerina Tsimaratou
Ioannis Christodoulou
Katerina Pyrillou
Vassilis Gorgoulis
Spiros Vlahopoulos
Vassilis Zoumpourlis
Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.
description Estrogen receptors (ER), namely ERα and ERβ, are hormone-activated transcription factors with an important role in carcinogenesis. In the present study, we aimed at elucidating the implication of ERα in skin cancer, using chemically-induced mouse skin tumours, as well as cell lines representing distinct stages of mouse skin oncogenesis. First, using immunohistochemical staining we showed that ERα is markedly increased in aggressive mouse skin tumours in vivo as compared to the papilloma tumours, whereas ERβ levels are low and become even lower in the aggressive spindle tumours of carcinogen-treated mice. Then, using the multistage mouse skin carcinogenesis model, we showed that ERα gradually increases during promotion and progression stages of mouse skin carcinogenesis, peaking at the most aggressive stage, whereas ERβ levels only slightly change throughout skin carcinogenesis. Stable transfection of the aggressive, spindle CarB cells with a dominant negative form of ERα (dnERα) resulted in reduced ERα levels and reduced binding to estrogen responsive elements (ERE)-containing sequences. We characterized two highly conserved EREs on the mouse ERα promoter through which dnERα decreased endogenous ERα levels. The dnERα-transfected CarB cells presented altered protein levels of cytoskeletal and cell adhesion molecules, slower growth rate and impaired anchorage-independent growth in vitro, whereas they gave smaller tumours with extended latency period of tumour onset in vivo. Our findings suggest an implication of ERα in the aggressiveness of spindle mouse skin cancer cells, possibly through regulation of genes affecting cell shape and adhesion, and they also provide hints for the effective targeting of spindle cancer cells by dnERα.
format article
author Stella Logotheti
Dimitra Papaevangeliou
Ioannis Michalopoulos
Maria Sideridou
Katerina Tsimaratou
Ioannis Christodoulou
Katerina Pyrillou
Vassilis Gorgoulis
Spiros Vlahopoulos
Vassilis Zoumpourlis
author_facet Stella Logotheti
Dimitra Papaevangeliou
Ioannis Michalopoulos
Maria Sideridou
Katerina Tsimaratou
Ioannis Christodoulou
Katerina Pyrillou
Vassilis Gorgoulis
Spiros Vlahopoulos
Vassilis Zoumpourlis
author_sort Stella Logotheti
title Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.
title_short Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.
title_full Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.
title_fullStr Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.
title_full_unstemmed Progression of mouse skin carcinogenesis is associated with increased ERα levels and is repressed by a dominant negative form of ERα.
title_sort progression of mouse skin carcinogenesis is associated with increased erα levels and is repressed by a dominant negative form of erα.
publisher Public Library of Science (PLoS)
publishDate 2012
url https://doaj.org/article/866cb55984d54136a886fcc3e806aa39
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