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Effects of ospemifene, a novel selective estrogen-receptor modulator, on human breast tissue ex vivo.

Menopause (New York, N.Y.) 2016 Vol.23(7) p. 719-30

Eigeliene N, Kangas L, Hellmer C, Kauko T, Erkkola R, Härkönen P

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[OBJECTIVE] Ospemifene (Osp) is a novel selective estrogen-receptor modulator (SERM) accepted for the treatment of dyspareunia, a symptom of postmenopausal vulvovaginal atrophy.

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  • p-value P < 0.01
  • p-value P < 0.001

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BibTeX ↓ RIS ↓
APA Eigeliene N, Kangas L, et al. (2016). Effects of ospemifene, a novel selective estrogen-receptor modulator, on human breast tissue ex vivo.. Menopause (New York, N.Y.), 23(7), 719-30. https://doi.org/10.1097/GME.0000000000000624
MLA Eigeliene N, et al.. "Effects of ospemifene, a novel selective estrogen-receptor modulator, on human breast tissue ex vivo.." Menopause (New York, N.Y.), vol. 23, no. 7, 2016, pp. 719-30.
PMID 27163517

Abstract

[OBJECTIVE] Ospemifene (Osp) is a novel selective estrogen-receptor modulator (SERM) accepted for the treatment of dyspareunia, a symptom of postmenopausal vulvovaginal atrophy. We aimed to analyze the effects of Osp on human breast tissue (HBT), in comparison with the clinically established SERMs raloxifene (Ral) and tamoxifen (Tam), using ex vivo explant cultures.

[METHODS] HBT samples were obtained from postmenopausal women undergoing mammoplasty and cultured with or without Osp, Ral, Tam, or 17β-estradiol (E2) for 7 and 14 days, and studied for morphology, proliferation, and apoptosis. The expression of epithelial markers, the estrogen-receptor alpha (ERα), the androgen receptor (AR), TFF1, and apolipoprotein D was evaluated using immunohistochemistry and quantitative reverse transcription-polymerase chain reaction. The PvuII polymorphism of ERS1 was determined.

[RESULTS] Osp, similar to Ral and Tam, decreased the number of proliferating cells in a concentration-dependent manner (at 100 nM, P < 0.01) and strongly opposed 10 nM E2-stimulated proliferation (P < 0.001). Corresponding effects were observed in the proportions of cells expressing ERα and TFF1 (P < 0.001). At 14 days apoptosis was increased by 100 nM SERMs (P < 0.01), but, notably, decreased by 1 nM Osp and Ral at day 7 (P < 0.05). The SERMs exerted ER-agonist effects on AR-positive cell populations at 1 nM (P < 0.05), but not at 100 nM concentrations. The effects on proliferation and ERα expressing cell numbers were associated with the ERS1 PvuII genotype.

[CONCLUSIONS] In summary, Osp inhibited proliferation and opposed E2 stimulation in normal HBT in an efficacious, but less potent way than Ral and Tam. The ESR1 PvuII polymorphisms may influence the responsiveness of HBT to E2 and SERMs.

추출된 의학 개체 (NER)

유형영어 표현한국어 / 풀이UMLS CUI출처등장
해부 breast 유방 dict 2
시술 mammoplasty 유방성형술 dict 1
해부 Osp → Ospemifene scispacy 1
해부 explant cultures scispacy 1
해부 epithelial scispacy 1
해부 cells scispacy 1
해부 ERα scispacy 1
해부 cell scispacy 1
합병증 postmenopausal vulvovaginal scispacy 1
약물 ospemifene C1313616
ospemifene
scispacy 1
약물 HBT → human breast tissue scispacy 1
약물 raloxifene C0244404
raloxifene
scispacy 1
약물 tamoxifen C0039286
tamoxifen
scispacy 1
약물 Tam → tamoxifen C0039286
tamoxifen
scispacy 1
약물 SERMs C0732611
Selective Estrogen Receptor Modulators
scispacy 1
약물 [OBJECTIVE] Ospemifene scispacy 1
약물 Osp → Ospemifene scispacy 1
약물 apolipoprotein D scispacy 1
약물 ER-agonist scispacy 1
질환 dyspareunia C0013394
Dyspareunia (female)
scispacy 1
질환 vulvovaginal atrophy C0857741
Vulvovaginal atrophy
scispacy 1
질환 AR-positive cell populations scispacy 1
기타 estrogen-receptor scispacy 1
기타 human breast tissue scispacy 1
기타 SERM → selective estrogen-receptor modulator scispacy 1
기타 SERMs raloxifene scispacy 1
기타 Ral → raloxifene scispacy 1
기타 women scispacy 1
기타 Tam → tamoxifen scispacy 1
기타 estrogen-receptor alpha scispacy 1
기타 androgen receptor scispacy 1
기타 TFF1 scispacy 1
기타 PvuII scispacy 1
기타 ERS1 scispacy 1
기타 SERMs scispacy 1
기타 Osp → Ospemifene scispacy 1
기타 ERS1 PvuII scispacy 1
기타 ESR1 PvuII scispacy 1

MeSH Terms

Aged; Apolipoproteins D; Apoptosis; Breast; Cell Proliferation; Estrogen Receptor alpha; Female; Humans; Middle Aged; Polymorphism, Genetic; Postmenopause; Raloxifene Hydrochloride; Receptors, Androgen; Selective Estrogen Receptor Modulators; Tamoxifen; Trefoil Factor-1

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