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绝经后激素治疗——也包括使用雌二醇加左炔诺孕酮宫内节育系统——与原发性输卵管癌风险增加相关。

Postmenopausal hormone therapy-also use of estradiol plus levonorgestrel-intrauterine system is associated with an increased risk of primary fallopian tube carcinoma.

作者信息

Koskela-Niska Virpi, Pukkala Eero, Lyytinen Heli, Ylikorkala Olavi, Dyba Tadeusz

机构信息

Department of Obstetrics and Gynecology, Helsinki University Hospital, FI-00029 HUS, Finland.

Finnish Cancer Registry, Institute for Statistical and Epidemiological Cancer Research, Unioninkatu 20, Helsinki, FI-00130, Finland.

出版信息

Int J Cancer. 2015 Oct 15;137(8):1947-52. doi: 10.1002/ijc.29549. Epub 2015 Apr 21.

Abstract

Data on the possible impact of postmenopausal hormone therapy (HT) on the incidence of rare primary fallopian tube carcinoma (PFTC) are scarce. Therefore, we conducted a nationwide case-control study analyzing the association between the use of different HTs and PFTC. All women aged 50 years or older with an incident PFTC (n = 360) during 1995-2007 were identified from the Finnish Cancer Registry. For each case of PFTC, ten age- and place of residence-matched controls were selected from the Finnish National Population Register, which also provided information on parity. Data on HT purchases were received from the Prescription Register, and data on hysterectomies and sterilizations from the National Care Register. Controls with a salpingectomy before the PFTC diagnosis of the respective case were excluded. The PFTC risk in relation to different HTs was estimated with a conditional logistic regression model, adjusted for parity, age at last delivery, hysterectomy and sterilization. The use for five years or more of estradiol combined with levonorgestrel-releasing-intrauterine system (odds ratio 2.84, 95% confidence interval 1.10-7.38) and sequential estradiol-progestin therapy (EPT; 3.37; 2.23-5.08) were both linked with increases in the risk of PFTC, while the risk with use of estradiol-only therapy or continuous EPT was not statistically significantly increased. The OR for the use of tibolone for one year or more was 1.56 (0.55-4.41). The use of HT is related to an increased risk of PFTC, particularly when a progestin component is intrauterine or systemic progestin is given in sequential manner.

摘要

关于绝经后激素治疗(HT)对罕见原发性输卵管癌(PFTC)发病率可能产生的影响的数据很少。因此,我们进行了一项全国性病例对照研究,分析不同HT的使用与PFTC之间的关联。从芬兰癌症登记处识别出1995 - 2007年期间所有年龄在50岁及以上且患有新发PFTC(n = 360)的女性。对于每例PFTC病例,从芬兰国家人口登记处选取10名年龄和居住地点匹配的对照,该登记处还提供了生育史信息。HT购买数据来自处方登记处,子宫切除术和绝育数据来自国家护理登记处。排除在相应病例的PFTC诊断之前进行过输卵管切除术的对照。使用条件逻辑回归模型估计不同HT相关的PFTC风险,并对生育史、末次分娩年龄、子宫切除术和绝育进行了调整。使用雌二醇联合左炔诺孕酮宫内节育系统五年或更长时间(比值比2.84,95%置信区间1.10 - 7.38)以及序贯雌二醇 - 孕激素治疗(EPT;3.37;2.23 - 5.08)均与PFTC风险增加有关,而仅使用雌二醇治疗或连续EPT的风险没有统计学上的显著增加。使用替勃龙一年或更长时间的OR为1.56(0.55 - 4.41)。HT的使用与PFTC风险增加有关,特别是当孕激素成分是宫内使用或采用序贯方式给予全身性孕激素时。

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