他莫昔芬和托瑞米芬两种抗雌激素药物对绝经后妇女妇科影响的前瞻性研究。
Prospective study on gynaecological effects of two antioestrogens tamoxifen and toremifene in postmenopausal women.
作者信息
Marttunen M B, Cacciatore B, Hietanen P, Pyrhönen S, Tiitinen A, Wahlström T, Ylikorkala O
机构信息
Department of Obstetrics, Helsinki University Central Hospital, P.O. Box 140, FIN-00029 HYKS, Finland.
出版信息
Br J Cancer. 2001 Apr 6;84(7):897-902. doi: 10.1054/bjoc.2001.1703.
To assess and compare the gynaecological consequences of the use of 2 antioestrogens we examined 167 postmenopausal breast cancer patients before and during the use of either tamoxifen (20 mg/day, n = 84) or toremifene (40 mg/day, n = 83) as an adjuvant treatment of stage II-III breast cancer. Detailed interview concerning menopausal symptoms, pelvic examination including transvaginal sonography (TVS) and collection of endometrial sample were performed at baseline and at 6, 12, 24 and 36 months of treatment. In a subgroup of 30 women (15 using tamoxifen and 15 toremifene) pulsatility index (PI) in an uterine artery was measured before and at 6 and 12 months of treatment. The mean (+/-SD) follow-up time was 2.3 +/- 0.8 years. 35% of the patients complained of vasomotor symptoms before the start of the trial. This rate increased to 60.0% during the first year of the trial, being similar among patients using tamoxifen (57.1%) and toremifene (62.7%). Vaginal dryness, which was present in 6.0% at baseline, increased during the use of tamoxifen (26.2%) and toremifene (24.1%). Endometrial thickness increased from baseline (3.9 +/- 2.7 mm) to 6.8 +/- 4.2 mm at 6 months (P< 0.001), and no difference emerged between the 2 regimens in this regard. Before the start of the antioestrogen regimen, the endometrium was atrophic in 71 (75.5%) and proliferative in 19 of 94 (20.2%) samples; 4 patients had benign endometrial polyps. During the use of antioestrogen altogether 339 endometrial samples were taken (159 in tamoxifen group, 180 in toremifene group). The endometrium was proliferative more often in the tamoxifen group (47.8%) than in the toremifene group (32.2%) (P< 0.0001). 20 patients had a total of 24 polyps (17 in tamoxifen and 9 in toremifene group, P< 0.05) during the use of antioestrogens. One patient in the toremifene group developed endometrial adenocarcinoma at 12 months, and one patient had breast cancer metastasis on the endometrium. Tamoxifen failed to affect the PI in the uterine artery, but toremifene reduced it by 15.0% (P< 0.05) by 12 months. In conclusion, tamoxifen and toremifene cause similarly vasomotor and vaginal symptoms. Neither regimen led to the development of premalignant endometrial changes. Our data suggest that so close endometrial surveillance as used in our study may not be mandatory during the first 3 years of use of antioestrogen treatment.
为评估和比较两种抗雌激素药物的妇科影响,我们对167例绝经后乳腺癌患者在使用他莫昔芬(20毫克/天,n = 84)或托瑞米芬(40毫克/天,n = 83)作为II - III期乳腺癌辅助治疗之前及期间进行了检查。在基线以及治疗的6、12、24和36个月时,就绝经症状进行了详细访谈,进行了包括经阴道超声检查(TVS)的盆腔检查并采集了子宫内膜样本。在30名女性亚组(15名使用他莫昔芬,15名使用托瑞米芬)中,在治疗前以及治疗的6个月和12个月时测量了子宫动脉搏动指数(PI)。平均(±标准差)随访时间为2.3±0.8年。35%的患者在试验开始前抱怨有血管舒缩症状。在试验的第一年,这一比例增至60.0%,在使用他莫昔芬(57.1%)和托瑞米芬(62.7%)的患者中相似。阴道干燥在基线时为6.0%,在使用他莫昔芬(26.2%)和托瑞米芬(24.1%)期间增加。子宫内膜厚度从基线时的(3.9±2.7毫米)在6个月时增加至6.8±4.2毫米(P<0.001),在这方面两种治疗方案之间未出现差异。在抗雌激素治疗方案开始前,94份样本中71份(75.5%)子宫内膜萎缩,19份(20.2%)呈增殖状态;4例患者有良性子宫内膜息肉。在使用抗雌激素期间共采集了339份子宫内膜样本(他莫昔芬组159份,托瑞米芬组180份)。他莫昔芬组子宫内膜呈增殖状态更为常见(47.8%),高于托瑞米芬组(32.2%)(P<0.0001)。在使用抗雌激素期间,20例患者共有24个息肉(他莫昔芬组17个,托瑞米芬组9个,P<0.05)。托瑞米芬组1例患者在12个月时发生子宫内膜腺癌,1例患者子宫内膜有乳腺癌转移。他莫昔芬未影响子宫动脉PI,但托瑞米芬在12个月时使其降低了15.0%(P<0.05)。总之,他莫昔芬和托瑞米芬引起的血管舒缩和阴道症状相似。两种治疗方案均未导致癌前子宫内膜变化的发生。我们的数据表明,在抗雌激素治疗的前3年,像我们研究中那样密切的子宫内膜监测可能并非必需。
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