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Abiraterone shows alternate activity in models of endocrine resistant and sensitive disease
by
Nikitorowicz-Buniak, Joanna
, Johnston, Stephen R
, Dowsett, Mitch
, Ribas, Ricardo
, Folkerd, Elizabeth
, Martin, Lesley-Ann
, Liccardi, Gianmaria
, Pancholi, Sunil
, Simigdala, Nikiana
in
Androgen receptors
/ Aromatase
/ Breast cancer
/ Cell death
/ Cell proliferation
/ Cytochrome P450
/ Disease resistance
/ Endocrine therapy
/ ESR1 protein
/ Ligands
/ Metastases
/ Proteasomes
/ Tumor cell lines
2018
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Abiraterone shows alternate activity in models of endocrine resistant and sensitive disease
by
Nikitorowicz-Buniak, Joanna
, Johnston, Stephen R
, Dowsett, Mitch
, Ribas, Ricardo
, Folkerd, Elizabeth
, Martin, Lesley-Ann
, Liccardi, Gianmaria
, Pancholi, Sunil
, Simigdala, Nikiana
in
Androgen receptors
/ Aromatase
/ Breast cancer
/ Cell death
/ Cell proliferation
/ Cytochrome P450
/ Disease resistance
/ Endocrine therapy
/ ESR1 protein
/ Ligands
/ Metastases
/ Proteasomes
/ Tumor cell lines
2018
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Abiraterone shows alternate activity in models of endocrine resistant and sensitive disease
by
Nikitorowicz-Buniak, Joanna
, Johnston, Stephen R
, Dowsett, Mitch
, Ribas, Ricardo
, Folkerd, Elizabeth
, Martin, Lesley-Ann
, Liccardi, Gianmaria
, Pancholi, Sunil
, Simigdala, Nikiana
in
Androgen receptors
/ Aromatase
/ Breast cancer
/ Cell death
/ Cell proliferation
/ Cytochrome P450
/ Disease resistance
/ Endocrine therapy
/ ESR1 protein
/ Ligands
/ Metastases
/ Proteasomes
/ Tumor cell lines
2018
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Abiraterone shows alternate activity in models of endocrine resistant and sensitive disease
Journal Article
Abiraterone shows alternate activity in models of endocrine resistant and sensitive disease
2018
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Overview
BackgroundResistance to endocrine therapy remains a major clinical problem in the treatment of oestrogen-receptor positive (ER+) breast cancer. Studies show androgen-receptor (AR) remains present in 80–90% of metastatic breast cancers providing support for blockade of AR-signalling. However, clinical studies with abiraterone, which blocks cytochrome P450 17A1 (CYP17A1) showed limited benefit.MethodsIn order to address this, we assessed the impact of abiraterone on cell-viability, cell-death, ER-mediated transactivation and recruitment to target promoters. together with ligand-binding assays in a panel of ER+ breast cancer cell lines that were either oestrogen-dependent, modelling endocrine-sensitive disease, or oestrogen-independent modelling relapse on an aromatase inhibitor. The latter, harboured wild-type (wt) or naturally occurring ESR1 mutations.ResultsSimilar to oestrogen, abiraterone showed paradoxical impact on proliferation by stimulating cell growth or death, depending on whether the cells are hormone-dependent or have undergone prolonged oestrogen-deprivation, respectively. Abiraterone increased ER-turnover, induced ER-mediated transactivation and ER-degradation via the proteasome.ConclusionsOur study confirms the oestrogenic activity of abiraterone and highlights its differential impact on cells dependent on oestrogen for their proliferation vs. those that are ligand-independent and harbour wt or mutant ESR1. These properties could impact the clinical efficacy of abiraterone in breast cancer.
Publisher
Nature Publishing Group
Subject
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