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使用雌二醇-孕激素疗法的绝经后女性子宫内膜癌

Endometrial cancer in postmenopausal women using estradiol-progestin therapy.

作者信息

Jaakkola Susanna, Lyytinen Heli, Pukkala Eero, Ylikorkala Olavi

机构信息

From the Department of Obstetrics and Gynecology, Helsinki University Central Hospital, Helsinki; Finnish Cancer Registry, Institute for Statistical and Epidemiological Cancer Research, Helsinki; and Tempere School of Public Health, University of Tempere, Tempere, Finland.

出版信息

Obstet Gynecol. 2009 Dec;114(6):1197-1204. doi: 10.1097/AOG.0b013e3181bea950.

Abstract

OBJECTIVE

To estimate the risk of endometrial cancer in all Finnish postmenopausal women using various forms of estradiol-progestin therapy.

METHODS

All Finnish women (aged more than 50 years) who had used estradiol-progestin therapy in 1994-2006 for at least 6 months (n=224,015) were identified from the national medical Reimbursement Registry and linked to the Finnish Cancer Registry. A total of 1,364 type I and 38 type II endometrial cancers were recorded by the end of 2006. The incidence of endometrial cancer in estradiol-progestin therapy users was compared with that in the general population in this cohort study.

RESULTS

The use of a continuous estradiol-progestin therapy regimen for 3 years or more was associated with a 76% reduction of the risk for type 1 cancer (95% confidence interval [CI] 6-60%). In contrast, the use of a sequential estradiol-progestin therapy regimen for at least 5 years was accompanied with a 69% elevation (95% CI 43-96%) if the progestin was added monthly, and with a significantly higher, 276% risk elevation (95% CI 190-379%) if progestin was added at 3-month intervals. Sequential regimens containing norethisterone acetate, medroxyprogesterone acetate or dydrogesterone administered orally showed no significant differences in the endometrial safety. Oral and transdermal norethisterone acetate were associated with similar risk elevations. Women using a monthly sequential estradiol-progestin regimen tended to be diagnosed with endometrial cancer in an earlier stage than the background population.

CONCLUSION

Use of a continuous rather than a sequential estradiol-progestin regimen decreases the risk of endometrial cancer, whereas the route of administration or type of progestin does not differ in terms of endometrial cancer risk.

LEVEL OF EVIDENCE

II.

摘要

目的

评估使用各种形式雌二醇 - 孕激素疗法的所有芬兰绝经后女性患子宫内膜癌的风险。

方法

从国家医疗报销登记处识别出1994年至2006年期间使用雌二醇 - 孕激素疗法至少6个月的所有芬兰女性(年龄超过50岁,n = 224,015),并与芬兰癌症登记处建立关联。到2006年底,共记录了1364例I型和38例II型子宫内膜癌。在这项队列研究中,将接受雌二醇 - 孕激素疗法的女性子宫内膜癌发病率与普通人群进行了比较。

结果

连续使用雌二醇 - 孕激素疗法3年或更长时间与I型癌症风险降低76%相关(95%置信区间[CI] 6 - 60%)。相比之下,如果每月添加孕激素,连续使用雌二醇 - 孕激素序贯疗法至少5年,风险升高69%(95% CI 43 - 96%);如果每3个月添加一次孕激素,则风险显著升高276%(95% CI 190 - 379%)。口服含有醋酸炔诺酮、醋酸甲羟孕酮或地屈孕酮的序贯疗法在子宫内膜安全性方面无显著差异。口服和经皮给予醋酸炔诺酮的风险升高相似。使用每月一次雌二醇 - 孕激素序贯疗法的女性往往比普通人群更早被诊断出子宫内膜癌。

结论

使用连续而非序贯的雌二醇 - 孕激素疗法可降低子宫内膜癌风险,而给药途径或孕激素类型在子宫内膜癌风险方面并无差异。

证据级别

II级

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