1. Effect of Tibolone on Breast Cancer Cell Proliferation in Postmenopausal ER+ Patients: Results from STEM Trial
- Author
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Cornelius C.M. Hageluken, Ernst Kubista, Michail Nechushkin, Mitch Dowsett, Alexey G. Manikhas, Juan V.M. Planellas Gomez, Kamil Pohlodek, Christian F. Singer, Jean-Michel Foidart, Rudolphe Serreyn, and Victor F. Semiglazov
- Subjects
Cancer Research ,medicine.medical_specialty ,HORMONE-REPLACEMENT THERAPY ,Antineoplastic Agents, Hormonal ,Norpregnenes ,medicine.medical_treatment ,Urology ,Placebo-controlled study ,Breast Neoplasms ,HOT FLASHES ,Tibolone ,PLACEBO-CONTROLLED TRIAL ,Placebo ,METABOLITES ,law.invention ,Placebos ,DOUBLE-BLIND ,Breast cancer ,Randomized controlled trial ,law ,medicine ,Humans ,Aged ,Gynecology ,ORG OD14 ,business.industry ,WOMENS HEALTH ,Hormone replacement therapy (menopause) ,IN-VITRO ,Middle Aged ,medicine.disease ,Combined Modality Therapy ,Primary tumor ,PREVALENCE ,Postmenopause ,MENOPAUSAL SYMPTOMS ,Menopause ,Oncology ,Female ,Safety ,business ,Cell Division ,medicine.drug - Abstract
Purpose: Tibolone is a selective tissue estrogenic activity regulator, approved for the treatment of vasomotor symptoms in postmenopausal women. We have done an exploratory, double-blind, randomized, placebo-controlled pilot trial to investigate the tissue-specific effects of 2.5 mg tibolone on breast cancer in postmenopausal women, in particular on tissue proliferation (STEM, Study of Tibolone Effects on Mamma carcinoma tissue). Experimental Design: Postmenopausal women with initially stage I/II, estrogen receptor–positive (ER+) primary breast cancer, were randomly assigned to 14 days of placebo or 2.5 mg/d tibolone. Core biopsies of the primary tumor were obtained before and after treatment. Ki-67 and apoptosis index were analyzed in baseline and corresponding posttreatment specimen. Results: Of 102 enrolled patients, 95 had evaluable data. Baseline characteristics were comparable between both treatment groups. Breast cancer cases are mainly invasive (99%), stage I or II (42% and 50% respectively), and ER+ (99%). Median intratumoral Ki-67 expression at baseline was 13.0% in the tibolone group and 17.8% in the placebo group, and decreased to 12.0% after 14 days of tibolone while increasing to 19.0% in the placebo group. This change from baseline was not significantly different between tibolone and placebo (Wilcoxon test; P = 0.17). A significant difference was observed between the treatment groups when the median change from baseline apoptosis index was compared between the treatment groups (tibolone, 0.0%; placebo, +0.3%; Wilcoxon test; P = 0.031). The incidence of adverse effects was comparable. Conclusions: In ER+ breast tumors, 2.5 mg/d tibolone given for 14 days has no significant effect on tumor cell proliferation.
- Published
- 2007