Naheed Bushra, Kuiper Jan Herman, Uthman Olalekan A, O'Mahony Fidelma, O'Brien Patrick Michael Shaughn
Institute for Science and Technology in Medicine, Keele University, Thornburrow Drive, Hartshill, Stoke-on-Trent, UK, ST4 7QB UK.
Warwick Centre for Applied Health Research and Delivery (WCAHRD), Division of Health Sciences, Warwick Medical School, The University of Warwick, Coventry, UK, CV4 7AL.
Cochrane Database Syst Rev. 2017 Mar 3;3(3):CD010503. doi: 10.1002/14651858.CD010503.pub2.
Premenstrual syndrome (PMS) is a psychological and somatic disorder of unknown aetiology, with symptoms typically including irritability, depression, mood swings, bloating, breast tenderness and sleep disturbances. About 3% to 10% of women who experience these symptoms may also meet criteria for premenstrual dysphoric disorder (PMDD). PMS symptoms recur during the luteal phase of the menstrual cycle and reduce by the end of menstruation. PMS results from ovulation and may be due to ovarian steroid interactions relating to neurotransmitter dysfunction. Premenstrual disorders have a devastating effect on women, their families and their work.Several treatment options have been suggested for PMS, including pharmacological and surgical interventions. The treatments thought to be most effective tend to fall into one of two categories: suppressing ovulation or correcting a speculated neuroendocrine anomaly.Transdermal oestradiol by patch, gel or implant effectively stops ovulation and the cyclical hormonal changes which produce the cyclical symptoms. These preparations are normally used for hormone therapy and contain lower doses of oestrogen than found in oral contraceptive pills. A shortened seven-day course of a progestogen is required each month for endometrial protection but can reproduce premenstrual syndrome-type symptoms in these women.
To determine the effectiveness and safety of non-contraceptive oestrogen-containing preparations in the management of PMS.
On 14 March 2016, we searched the following databases: the Cochrane Gynaecology and Fertility Group (CGF) Specialised Register; Cochrane Central Register of Studies (CRSO); MEDLINE; Embase; PsycINFO; CINAHL; ClinicalTrials.gov; metaRegister of Controlled trials (mRCT); and the World Health Organization (WHO) International Clinical Trials Registry Platform (ICTRP) Search Portal. In addition, we checked the reference lists of articles retrieved.
We included published and unpublished randomized placebo or active controlled trials on the efficacy of the use of non-contraceptive oestrogen-containing preparations in the management of premenstrual syndrome in women of reproductive age with PMS diagnosed by at least two prospective cycles without current psychiatric disorder.
Two review authors independently selected studies, assessed risk of bias, extracted data on premenstrual symptoms and adverse effects and entered data into Review Manager 5 software. Where possible, intention-to-treat or modified intention-to-treat analysis was used. Studies were pooled using a fixed-effect model, analysing cross-over trials as parallel trials. Standardised mean differences (SMDs) with 95% confidence intervals (CIs) were calculated for premenstrual symptom scores. Risk ratios (RRs) with 95% confidence intervals (CIs) were calculated for dichotomous outcomes. The overall quality of the evidence was assessed using the GRADE working group methods.
The search resulted in 524 potentially relevant articles. Five eligible randomized controlled trials (RCTs) were identified (305 women). Trials using oral tablets, transdermal patches and implants were identified. No trial used gels.One small cross-over trial (11 women, effective sample size 22 women considering cross-over trials) compared oral luteal-phase oestrogen versus placebo. Data were very low quality and unsuitable for analysis, but study authors reported that the intervention was ineffective and might aggravate the symptoms of PMS. They also reported that there were no adverse events.Three studies compared continuous oestrogen with progestogen versus placebo (with or without progestogen). These trials were of reasonable quality, although with a high risk of attrition bias and an unclear risk of bias due to potential carry-over effects in two cross-over trials. Continuous oestrogen had a small to moderate positive effect on global symptom scores (SMD -0.34, 95% CI -0.59 to -0.10, P = 0.005, 3 RCTs, 158 women, effective sample size 267 women, I² = 63%, very low quality evidence). The evidence was too imprecise to determine if the groups differed in withdrawal rates due to adverse effects (RR 0.64, 95% CI 0.26 to 1.58, P = 0.33, 3 RCTs, 196 women, effective sample size 284 women, I² = 0%, very low quality evidence). Similarly, the evidence was very imprecise in measures of specific adverse events, with large uncertainties around the true value of the relative risk. None of the studies reported on long-term risks such as endometrial cancer or breast cancer.One study compared patch dosage (100 vs 200 µg oestrogen, with progestogen in both arms) and had a high risk of performance bias, detection bias and attrition bias. The study did not find evidence that dosage affects global symptoms but there was much uncertainty around the effect estimate (SMD -1.55, 95% CI -8.88 to 5.78, P = 0.68, 1 RCT, 98 women, very low quality evidence). The evidence on rates of withdrawal for adverse events was too imprecise to draw any conclusions (RR 0.70, 95% CI 0.34 to 1.46, P = 0.34, 1 RCT, 107 women, low-quality evidence). However, it appeared that the 100 µg dose might be associated with a lower overall risk of adverse events attributed to oestrogen (RR 0.51, 95% Cl 0.26 to 0.99, P = 0.05, 1 RCT, 107 women, very low quality evidence) with a large uncertainty around the effect estimate.The overall quality of the evidence for all comparisons was very low, mainly due to risk of bias (specifically attrition), imprecision, and statistical and clinical heterogeneity.
AUTHORS' CONCLUSIONS: We found very low quality evidence to support the effectiveness of continuous oestrogen (transdermal patches or subcutaneous implants) plus progestogen, with a small to moderate effect size. We found very low quality evidence from a study based on 11 women to suggest that luteal-phase oral unopposed oestrogen is probably ineffective and possibly detrimental for controlling the symptoms of PMS. A comparison between 200 µg and 100 µg doses of continuous oestrogen was inconclusive with regard to effectiveness, but suggested that the lower dose was less likely to cause side effects. Uncertainty remains regarding safety, as the identified studies were too small to provide definite answers. Moreover, no included trial addressed adverse effects that might occur beyond the typical trial duration of 2-8 months. This suggests the choice of oestrogen dose and mode of administration could be based on an individual woman's preference and modified according to the effectiveness and tolerability of the chosen regimen.
经前综合征(PMS)是一种病因不明的心理和躯体疾病,症状通常包括易怒、抑郁、情绪波动、腹胀、乳房胀痛和睡眠障碍。出现这些症状的女性中,约3%至10%可能符合经前烦躁障碍(PMDD)的标准。PMS症状在月经周期的黄体期复发,并在月经结束时减轻。PMS由排卵引起,可能与卵巢类固醇与神经递质功能障碍的相互作用有关。经前疾病对女性及其家庭和工作都有毁灭性影响。针对PMS提出了几种治疗选择,包括药物和手术干预。被认为最有效的治疗方法往往属于两类之一:抑制排卵或纠正推测的神经内分泌异常。通过贴片、凝胶或植入物的经皮雌二醇可有效阻止排卵以及产生周期性症状的周期性激素变化。这些制剂通常用于激素治疗,其雌激素剂量低于口服避孕药。每月需要一个为期七天的孕激素短疗程以保护子宫内膜,但这可能会在这些女性中重现经前综合征类型的症状。
确定含非避孕雌激素制剂治疗PMS的有效性和安全性。
2016年3月14日,我们检索了以下数据库:Cochrane妇科和生育组(CGF)专业注册库;Cochrane系统评价中心注册库(CRSO);医学期刊数据库(MEDLINE);荷兰医学文摘数据库(Embase);心理学文摘数据库(PsycINFO);护理学与健康领域数据库(CINAHL);临床试验.gov;对照试验元注册库(mRCT);以及世界卫生组织(WHO)国际临床试验注册平台(ICTRP)搜索门户。此外,我们还检查了检索到的文章的参考文献列表。
我们纳入了已发表和未发表的随机安慰剂或活性对照试验,这些试验研究了含非避孕雌激素制剂用于治疗有PMS的育龄期女性经前综合征的疗效,这些女性经至少两个前瞻性周期诊断为PMS,且目前无精神疾病。
两位综述作者独立选择研究、评估偏倚风险、提取经前症状和不良反应的数据,并将数据录入Review Manager 5软件。尽可能采用意向性分析或改良意向性分析。使用固定效应模型对研究进行汇总,将交叉试验作为平行试验进行分析。计算经前症状评分的标准化均数差(SMD)及其95%置信区间(CI)。计算二分结局的风险比(RR)及其95%置信区间(CI)。使用GRADE工作组方法评估证据的整体质量。
检索结果产生了524篇可能相关的文章。确定了5项符合条件的随机对照试验(RCT)(305名女性)。确定了使用口服片剂、经皮贴片和植入物的试验。没有试验使用凝胶。一项小型交叉试验(11名女性,考虑交叉试验后有效样本量为22名女性)比较了口服黄体期雌激素与安慰剂。数据质量非常低,不适合分析,但研究作者报告该干预无效,可能会加重PMS的症状。他们还报告没有不良事件。三项研究比较了连续雌激素加孕激素与安慰剂(有或无孕激素)。这些试验质量尚可,尽管两项交叉试验存在较高失访偏倚风险,且由于潜在的延续效应导致偏倚风险不明确。连续雌激素对总体症状评分有小到中度的积极影响(SMD -0.34,95%CI -0.59至-0.10,P = 0.005,3项RCT,158名女性,有效样本量267名女性,I² = 63%,极低质量证据)。证据过于不精确,无法确定两组因不良反应导致的退出率是否存在差异(RR 0.64,95%CI 0.26至1.58,P = 0.33,3项RCT,196名女性,有效样本量284名女性,I² = 0%,极低质量证据)。同样,在特定不良事件的测量方面,证据也非常不精确,相对风险的真实值存在很大不确定性。没有研究报告子宫内膜癌或乳腺癌等长期风险。一项研究比较了贴片剂量(100 vs 200μg雌激素,两组均有孕激素),存在较高的实施偏倚、检测偏倚和失访偏倚风险。该研究未发现剂量影响总体症状的证据,但效应估计值存在很大不确定性(SMD -1.55,95%CI -8.88至5.78,P = 0.68,1项RCT,98名女性,极低质量证据)。关于因不良事件导致的退出率的证据过于不精确,无法得出任何结论(RR 0.70,95%CI 0.34至1.46,P = 0.34,1项RCT,107名女性,低质量证据)。然而,似乎100μg剂量可能与归因于雌激素的不良事件总体风险较低相关(RR 0.51,95%CI 0.26至0.99,P = 0.05,1项RCT,107名女性,极低质量证据),效应估计值存在很大不确定性。所有比较的证据总体质量都非常低,主要是由于偏倚风险(特别是失访)、不精确性以及统计和临床异质性。
我们发现极低质量的证据支持连续雌激素(经皮贴片或皮下植入物)加孕激素的有效性,效应大小为小到中度。我们从一项基于11名女性的研究中发现极低质量的证据表明,黄体期口服单一雌激素可能对控制PMS症状无效,甚至可能有害。200μg和100μg连续雌激素剂量在有效性方面的比较尚无定论,但表明较低剂量引起副作用的可能性较小。由于已确定的研究规模太小,无法提供明确答案,因此在安全性方面仍存在不确定性。此外,没有纳入的试验涉及典型试验持续时间2至8个月以外可能出现的不良反应。这表明雌激素剂量和给药方式的选择可以基于个体女性的偏好,并根据所选方案的有效性和耐受性进行调整。
