Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model

AIM: A model of progressively endocrine-resistant breast cancer was investigated to identify changes that can occur in signaling pathways after endocrine manipulation. METHODS: The MCF7 breast cancer model is sensitive to estrogens and anti-estrogens while variant lines previously derived from wild-...

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Autores principales: Moore, Kate M., Cerqueira, Vera, MacLeod, Kenneth G., Mullen, Peter, Hayward, Richard L., Green, Simon, Harrison, David J., Cameron, David A., Langdon, Simon P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Open Exploration 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7612628/
https://www.ncbi.nlm.nih.gov/pubmed/35441158
http://dx.doi.org/10.37349/etat.2022.00074
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author Moore, Kate M.
Cerqueira, Vera
MacLeod, Kenneth G.
Mullen, Peter
Hayward, Richard L.
Green, Simon
Harrison, David J.
Cameron, David A.
Langdon, Simon P.
author_facet Moore, Kate M.
Cerqueira, Vera
MacLeod, Kenneth G.
Mullen, Peter
Hayward, Richard L.
Green, Simon
Harrison, David J.
Cameron, David A.
Langdon, Simon P.
author_sort Moore, Kate M.
collection PubMed
description AIM: A model of progressively endocrine-resistant breast cancer was investigated to identify changes that can occur in signaling pathways after endocrine manipulation. METHODS: The MCF7 breast cancer model is sensitive to estrogens and anti-estrogens while variant lines previously derived from wild-type MCF7 are either relatively 17β-estradiol (E(2 ))-insensitive (LCC1) or fully resistant to estrogen and anti-estrogens (LCC9). RESULTS: In LCC1 and LCC9 cell lines, loss of estrogen sensitivity was accompanied by loss of growth response to transforming growth factor alpha (TGFα), heregulin-beta and pertuzumab. LCC1 and LCC9 cells had enhanced AKT phosphorylation relative to MCF7 which was reflected in downstream activation of phospho-mechanistic target of rapamycin (mTOR), phospho-S6, and phospho-estrogen receptor alpha Ser167 [ERα(Ser167)]. Both AKT2 and AKT3 were phosphorylated in the resistant cell lines, but small interfering RNA (siRNA) knockdown suggested that all three AKT isoforms contributed to growth response. ERα(Ser118) phosphorylation was increased by E(2) and TGFα in MCF7, by E(2) only in LCC1, but by neither in LCC9 cells. Multiple alterations in E(2)-mediated cell cycle control were identified in the endocrine-resistant cell lines including increased expression of MYC, cyclin A1, cyclin D1, cyclin-dependent kinase 1 (CDK1), CDK2, and hyperphosphorylated retinoblastoma protein (ppRb), whereas p21 and p27 were reduced. Estrogen modulated expression of these regulators in MCF7 and LCC1 cells but not in LCC9 cells. Seliciclib inhibited CDK2 activation in MCF7 cells but not in resistant variants; in all lines, it reduced ppRb, increased p53 associated responses including p21, p53 up-regulated modulator of apoptosis (PUMA), and p53 apoptosis-inducing protein 1 (p53AIP1), inhibited growth, and produced G2/M block and apoptosis. CONCLUSIONS: Multiple changes occur with progression of endocrine resistance in this model with AKT activation contributing to E(2) insensitivity and loss of ERα(Ser118) phosphorylation being associated with full resistance. Cell cycle regulation is modified in endocrine-resistant breast cancer cells, and seliciclib is effective in both endocrine-sensitive and resistant diseases.
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spelling pubmed-76126282022-04-18 Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model Moore, Kate M. Cerqueira, Vera MacLeod, Kenneth G. Mullen, Peter Hayward, Richard L. Green, Simon Harrison, David J. Cameron, David A. Langdon, Simon P. Explor Target Antitumor Ther Original Article AIM: A model of progressively endocrine-resistant breast cancer was investigated to identify changes that can occur in signaling pathways after endocrine manipulation. METHODS: The MCF7 breast cancer model is sensitive to estrogens and anti-estrogens while variant lines previously derived from wild-type MCF7 are either relatively 17β-estradiol (E(2 ))-insensitive (LCC1) or fully resistant to estrogen and anti-estrogens (LCC9). RESULTS: In LCC1 and LCC9 cell lines, loss of estrogen sensitivity was accompanied by loss of growth response to transforming growth factor alpha (TGFα), heregulin-beta and pertuzumab. LCC1 and LCC9 cells had enhanced AKT phosphorylation relative to MCF7 which was reflected in downstream activation of phospho-mechanistic target of rapamycin (mTOR), phospho-S6, and phospho-estrogen receptor alpha Ser167 [ERα(Ser167)]. Both AKT2 and AKT3 were phosphorylated in the resistant cell lines, but small interfering RNA (siRNA) knockdown suggested that all three AKT isoforms contributed to growth response. ERα(Ser118) phosphorylation was increased by E(2) and TGFα in MCF7, by E(2) only in LCC1, but by neither in LCC9 cells. Multiple alterations in E(2)-mediated cell cycle control were identified in the endocrine-resistant cell lines including increased expression of MYC, cyclin A1, cyclin D1, cyclin-dependent kinase 1 (CDK1), CDK2, and hyperphosphorylated retinoblastoma protein (ppRb), whereas p21 and p27 were reduced. Estrogen modulated expression of these regulators in MCF7 and LCC1 cells but not in LCC9 cells. Seliciclib inhibited CDK2 activation in MCF7 cells but not in resistant variants; in all lines, it reduced ppRb, increased p53 associated responses including p21, p53 up-regulated modulator of apoptosis (PUMA), and p53 apoptosis-inducing protein 1 (p53AIP1), inhibited growth, and produced G2/M block and apoptosis. CONCLUSIONS: Multiple changes occur with progression of endocrine resistance in this model with AKT activation contributing to E(2) insensitivity and loss of ERα(Ser118) phosphorylation being associated with full resistance. Cell cycle regulation is modified in endocrine-resistant breast cancer cells, and seliciclib is effective in both endocrine-sensitive and resistant diseases. Open Exploration 2022 2022-02-28 /pmc/articles/PMC7612628/ /pubmed/35441158 http://dx.doi.org/10.37349/etat.2022.00074 Text en © The Author(s) 2022. https://creativecommons.org/licenses/by/4.0/This is an Open Access article licensed under a Creative Commons Attribution 4.0 International License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, sharing, adaptation, distribution and reproduction in any medium or format, for any purpose, even commercially, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Original Article
Moore, Kate M.
Cerqueira, Vera
MacLeod, Kenneth G.
Mullen, Peter
Hayward, Richard L.
Green, Simon
Harrison, David J.
Cameron, David A.
Langdon, Simon P.
Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model
title Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model
title_full Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model
title_fullStr Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model
title_full_unstemmed Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model
title_short Collateral-resistance to estrogen and HER-activated growth is associated with modified AKT, ERα, and cell-cycle signaling in a breast cancer model
title_sort collateral-resistance to estrogen and her-activated growth is associated with modified akt, erα, and cell-cycle signaling in a breast cancer model
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7612628/
https://www.ncbi.nlm.nih.gov/pubmed/35441158
http://dx.doi.org/10.37349/etat.2022.00074
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