Prospective study on gynaecological effects of two antioestrogens tamoxifen and toremifene in postmenopausal women

Marttunen, Merja B.; Cacciatore, Bruno; Hietanen, Päivi; Pyrhönen, Seppo; Tiitinen, Aila; Wahlström, Torsten; Ylikorkala, Olavi

doi:10.1054/bjoc.2001.1703

Cited by 40 publications

(28 citation statements)

References 37 publications

(37 reference statements)

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“…A 3-year study specifically designed to compare the gynecological effects of toremifene 40 mg and tamoxifen 20 mg in 167 postmenopausal breast cancer patients showed that the incidence of proliferative endometrium was increased to a significantly (P < 0.0001) lesser extent by toremifene (from 20.0% to 32.2%) than by tamoxifen (from 20.4% to 46.8%) [60] .…”

Section: Long Term Safetymentioning

confidence: 99%

Toremifene in the treatment of breast cancer

Mustonen¹

2014

WJCO

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Core tip: Toremifene is safe and effective in the treatment of breast cancer. Toremifene and tamoxifen are equivalently effective in the treatment of breast cancer, although some studies show an advantage for toremifene. Safety and tolerability is also broadly equivalent, although toremifene may cause fewer uterine neoplasms, serious vascular adverse events and has a more beneficial effect on plasma lipids than does tamoxifen.Mustonen MVJ, Pyrhönen S, Kellokumpu-Lehtinen PL. Toremifene in the treatment of breast cancer.

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Section: Long Term Safetymentioning

confidence: 99%

Toremifene in the treatment of breast cancer

Mustonen¹

2014

WJCO

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“…Disappointing efficacy data for both droloxifene and idoxifene when compared with tamoxifen or when used in tamoxifen-resistant disease have led to their development being halted. Toremifene (chloro-tamoxifen), which has similar efficacy but fewer agonist properties compared with tamoxifen (Marttunen et al 1998(Marttunen et al , 2001, remains in clinical development in the breast cancer prevention setting.…”

Section: Introductionmentioning

confidence: 99%

Pure oestrogen antagonists for the treatment of advanced breast cancer

Howell¹

2006

Endocr Relat Cancer

107

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For more than 30 years, tamoxifen has been the drug of choice in treating patients with oestrogen receptor (ER)-positive breast tumours. However, research has endeavoured to develop agents that match and improve the clinical efficacy of tamoxifen, but lack its partial agonist effects. The first 'pure' oestrogen antagonist was developed in 1987; from this, an even more potent derivative was developed for clinical use, known as fulvestrant (ICI 182,780, 'Faslodex'). Mechanistic studies have shown that fulvestrant possesses high ER-binding affinity and has multiple effects on ER signalling: it blocks dimerisation and nuclear localisation of the ER, reduces cellular levels of ER and blocks ER-mediated gene transcription. Unlike anti-oestrogens chemically related to tamoxifen, fulvestrant also helps circumvent resistance to tamoxifen. There are extensive data to support the lack of partial agonist effects of fulvestrant and, importantly, its lack of cross-resistance with tamoxifen. In phase III studies in patients with locally advanced or metastatic breast cancer, fulvestrant was at least as effective as anastrozole in patients with tamoxifen-resistant tumours, was effective in the first-line setting and was also well tolerated. These data are supported by experience from the compassionate use of fulvestrant in more heavily pretreated patients. Further studies are now underway to determine the best strategy for sequencing oestrogen endocrine therapies and to optimise dosing regimens of fulvestrant. At present, and for the foreseeable future, fulvestrant is the only oestrogen antagonist with no agonistic effects licensed for the treatment of advanced breast cancer in postmenopausal women. Other similar oestrogen antagonists are undergoing research and development, with a few currently being evaluated in phase II trials.

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“…MB Marttunen et al suggested that at least in the first 2-3 years, toremifene treatment does not increase the risk of endometrial cancer. 12 According to Ha et al, 8 the majority of uterine cancers developed after more than 1 year of treatment, and the annual hazard rate for endometrial cancer was 1.0 per 1,000 patient treatment years. Adenosarcoma is a very rare uterine malignancy detected in this patient on toremifene therapy who has no risk factors for uterine malignancy other than old age.…”

Section: Discussionmentioning

confidence: 99%

Endometrial mullerian adenosarcoma after toremifene treatment in breast cancer patients: a case report

et al. 2010

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Toremifene is an anti-estrogen which has been shown to be effective in the treatment of breast cancer, and is thought to be a less uterotrophic agent than tamoxifen. The risk assessment concerning endometrial cancer has been inconclusive because of its rare use up to the mid-1990s. We report a case of an adenosarcoma, which is a very rare type of uterine malignancy, after toremifene treatment for 5 years in a breast cancer patient. After 1 year of toremifene use, the patient had a benign Mullerian adenofibroma. After an additional 4 years of toremifene treatment, the endometrial polypoid lesion was transformed into a Mullerian adenosarcoma. Although toremifene is a promising anti-estrogenic agent in the treatment of breast cancer patients, clinicians should not neglect the possibility of a uterine malignancy.

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Prospective study on gynaecological effects of two antioestrogens tamoxifen and toremifene in postmenopausal women

Cited by 40 publications

References 37 publications

Toremifene in the treatment of breast cancer

Toremifene in the treatment of breast cancer

Pure oestrogen antagonists for the treatment of advanced breast cancer

Endometrial mullerian adenosarcoma after toremifene treatment in breast cancer patients: a case report

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