Molecular changes in premenopausal oestrogen receptor-positive primary breast cancer in Vietnamese women after oophorectomy

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Ben P. Haynes
Ophira Ginsburg
Qiong Gao
Elizabeth Folkerd
Maria Afentakis
Le Hong Quang
Pham Thi Han
Pham Hong Khoa
Nguyen Van Dinh
Ta Van To
Mark Clemons
Ian E. Smith
Mitch Dowsett
机构
[1] Royal Marsden Hospital,The Ralph Lauren Centre for Breast Cancer Research
[2] University of Toronto,Department of Medicine
[3] NYU Langone Medical Center,Department of Population Health, NYU School of Medicine/Laura and Isaac Perlmutter Cancer Center
[4] The Institute of Cancer Research,The Breast Cancer Now Toby Robins Research Centre
[5] National Cancer Hospital,Department of Breast Surgery
[6] National Cancer Hospital,Department of Pathology
[7] The Ottawa Hospital and University of Ottawa,Department of Medicine, Division of Medical Oncology
[8] Royal Marsden Hospital,The Breast Unit, Department of Medicine
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For premenopausal women with primary ER + breast cancer, oophorectomy (OvX) is an evidence-based cost-effective option and is standard treatment in many countries. However, there is virtually no data describing the effects of OvX on breast tumour biology. We therefore, characterised the endocrine and genome-wide transcriptional impact of OvX in 56 premenopausal women with ER + breast cancer for 2 weeks prior to mastectomy. Plasma estradiol concentrations decreased from 406 ± 41 to 20.7 ± 2.6 pmol/l (mean ± sem) 24 h after OvX, and to 8.1 ± 0.8 pmol/l 2 weeks later at mastectomy. Ki67 decreased in 33/36 (91.7%) tumours. The expression of 655 genes changed significantly (FDR < 1%) with an absolute mean fold-change (FC) ≥ 1.25 (257 up, 398 down). Archetypal oestrogen-regulated genes (TFF1, GREB1, PGR and PDZK1) showed large decreases in expression (FC = 0.20–0.69; p < 1e-6-1e-7). Proliferation-associated genes (e.g. TOP2A, AURKA and UBE2C) were also strongly downregulated (FC = 0.38–0.56; p < 1e-7) along with putative progesterone-regulated genes (e.g. FKBP4, MYB; FC = 0.64–0.68; p < 1e-4-1e-7). The gene expression changes did not differ according to HER2 status and correlated strongly with the changes reported previously after aromatase inhibitor (AI) treatment in postmenopausal women (rho = 0.55, p < 1e-04). However, after OvX the mean FC was significantly higher compared to AI (p < 1e-04). In conclusion, changes in tumoural gene expression after OvX were largely similar, but of a greater magnitude to those observed after AI in postmenopausal patients; however, OvX appeared to have a greater effect on progesterone-regulated genes than AI.
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