Synapse - Italian randomized trial among women with hysterectomy: Tamoxifen and hormone-dependent breast cancer in high-risk women

Italian randomized trial among women with hysterectomy: Tamoxifen and hormone-dependent breast cancer in high-risk women Journal Article

Authors:	Veronesi, U.; Maisonneuve, P.; Rotmensz, N.; Costa, A.; Sacchini, V.; Travaglini, R.; D'Aiuto, G.; Lovison, F.; Gucciardo, G.; Muraca, M. G.; Pizzichetta, M. A.; Conforti, S.; Decensi, A.; Robertson, C.; Boyle, P.
Article Title:	Italian randomized trial among women with hysterectomy: Tamoxifen and hormone-dependent breast cancer in high-risk women
Abstract:	Tamoxifen improves outcome in women with breast cancer and reduces the incidence of estrogen receptor-positive (ER+) breast tumors in prevention trials. Tamoxifen use is associated with an increased risk of potentially serious adverse events, principally endometrial cancer and venous thromboembolic events and, therefore, detailed knowledge of the effects of tamoxifen is important. With more cases of breast cancer being found as the follow-up time increases, it is now possible to perform more detailed analysis of the Italian Randomized Trial of Tamoxifen. Women with hysterectomy (N = 5408) were randomly assigned to receive 20 mg tamoxifen per day (N = 2700) or placebo (N = 2708). After a median of 81.2 months of follow-up, 79 case subjects (34 in the tamoxifen arm and 45 in the placebo arm) were diagnosed with breast cancer. We were able to identify a group of women at increased risk of ER+ breast cancers (high-risk group) on the basis of baseline as well as reproductive and hormonal characteristics (height, age at menarche, parity, age at first birth, and oophorectomy). Tamoxifen administered to women in the high-risk group showed statistically significantly reduced incidence of breast cancer (tamoxifen, 3 and placebo, 15; P = .003), but no such effect was seen in the low-risk group (tamoxifen, 31 and placebo, 30; P = .89). The positive effect of tamoxifen on breast cancer among high-risk women is most marked for ER+ tumors (tamoxifen, 1 and placebo, 11; P = .002). Chemoprevention of breast cancer with tamoxifen appears to be effective in women at high risk of ER+ tumors but not among women at low risk, who may well be protected naturally by late age at menarche or early first pregnancy, or artificially by removal of the ovaries. Tamoxifen could be offered as a preventive agent to women identified at high-risk of breast cancer because of hormone-related risk factors. Such a strategy would greatly reduce the numbers of women who would need to take tamoxifen to obtain the same absolute reduction in breast cancer. These findings are exploratory and need to be confirmed in other randomized trials.
Keywords:	controlled study; treatment outcome; disease-free survival; middle aged; survival analysis; clinical trial; placebo; cancer risk; drug efficacy; follow up; follow-up studies; cancer incidence; hysterectomy; endometrium cancer; cancer prevention; chemoprophylaxis; controlled clinical trial; breast cancer; randomized controlled trial; ovariectomy; incidence; odds ratio; risk factors; breast neoplasms; risk factor; high risk patient; menarche; age; risk assessment; estrogen replacement therapy; statistical significance; thromboembolism; vein thrombosis; tamoxifen; receptors, estrogen; body height; antineoplastic agents, hormonal; estrogen receptor; hormone; breast carcinogenesis; reproduction; italy; parity; selective estrogen receptor modulators; primigravida; hormonal carcinogenesis; estrogen antagonists; humans; human; female; priority journal; article; birth order
Journal Title:	JNCI: Journal of the National Cancer Institute
Volume:	95
Issue:	2
ISSN:	0027-8874
Publisher:	Oxford University Press
Date Published:	2003-01-15
Start Page:	160
End Page:	165
Language:	English
PUBMED:	12529349
PROVIDER:	scopus
DOI:	10.1093/jnci/95.2.160
DOI/URL:	http://www.scopus.com/inward/record.url?eid=2-s2.0-20244363902&partnerID=40&md5=3bf0cb5f34f55fb085e4ef8c3fd9c195
Notes:	Export Date: 12 September 2014 -- Source: Scopus

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