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用于患有多囊卵巢综合征、月经过少和生育力低下的女性的胰岛素增敏药物(二甲双胍、罗格列酮、吡格列酮、D-手性肌醇)。

Insulin-sensitising drugs (metformin, rosiglitazone, pioglitazone, D-chiro-inositol) for women with polycystic ovary syndrome, oligo amenorrhoea and subfertility.

作者信息

Morley Lara C, Tang Thomas, Yasmin Ephia, Norman Robert J, Balen Adam H

机构信息

Department of Obstetrics and Gynaecology, The General Infirmary of Leeds, United Leeds Teaching Hospitals NHS Trust, Belmont Grove, Leeds, UK, LS2 9NS.

出版信息

Cochrane Database Syst Rev. 2017 Nov 29;11(11):CD003053. doi: 10.1002/14651858.CD003053.pub6.

Abstract

BACKGROUND

Polycystic ovary syndrome (PCOS) is characterised by infrequent or absent ovulation, and high levels of androgens and insulin (hyperinsulinaemia). Hyperinsulinaemia occurs secondary to insulin resistance and is associated with increased risk of cardiovascular disease and diabetes mellitus. Insulin-sensitising agents such as metformin may be effective in treating PCOS-related anovulation.

OBJECTIVES

To evaluate the effectiveness and safety of insulin-sensitising drugs in improving reproductive and metabolic outcomes for women with PCOS undergoing ovulation induction.

SEARCH METHODS

We searched the following databases from inception to January 2017: Cochrane Gynaecology and Fertility Group Specialised Register, CENTRAL, MEDLINE, Embase, PsycINFO and CINAHL. We searched registers of ongoing trials and reference lists from relevant studies.

SELECTION CRITERIA

We included randomised controlled trials of insulin-sensitising drugs compared with placebo, no treatment, or an ovulation-induction agent for women with oligo and anovulatory PCOS.

DATA COLLECTION AND ANALYSIS

Two review authors independently assessed studies for eligibility and bias. Primary outcomes were live birth rate and gastrointestinal adverse effects. Secondary outcomes included other pregnancy outcomes, menstrual frequency and metabolic effects. We combined data to calculate pooled odds ratios (ORs) and 95% confidence intervals (CIs). We assessed statistical heterogeneity using the I statistic and reported quality of the evidence for primary outcomes using GRADE methodology.

MAIN RESULTS

We assessed the interventions metformin, clomiphene citrate, metformin plus clomiphene citrate, D-chiro-inositol, rosiglitazone and pioglitazone. We compared these with each other, placebo or no treatment. We included 48 studies (4451 women), 42 of which investigated metformin (4024 women). Evidence quality ranged from very low to moderate. Limitations were risk of bias (poor reporting of methodology and incomplete outcome data), imprecision and inconsistency. Metformin versus placebo or no treatmentThe evidence suggests that metformin may improve live birth rates compared with placebo (OR 1.59, 95% CI 1.00 to 2.51, 4 studies, 435 women, I = 0%, low-quality evidence). The metformin group experienced more gastrointestinal side effects (OR 4.76, 95% CI 3.06 to 7.41, 7 studies, 670 women, I = 61%, moderate-quality evidence) but had higher rates of clinical pregnancy (OR 1.93, 95% CI 1.42 to 2.64, 9 studies, 1027 women, I = 43%, moderate-quality evidence), ovulation (OR 2.55, 95% CI 1.81 to 3.59, 14 studies, 701 women, I = 58%, moderate-quality evidence) and menstrual frequency (OR 1.72, 95% CI 1.14 to 2.61, 7 studies, 427 women, I = 54%, low-quality evidence). There was no clear evidence of a difference in miscarriage rates (OR 1.08, 95% CI 0.50 to 2.35, 4 studies, 748 women, I = 0%, low-quality evidence). Metformin plus clomiphene citrate versus clomiphene citrate alone There was no conclusive evidence of a difference between the groups in live birth rates (OR 1.21, 95% CI 0.92 to 1.59, 9 studies, 1079 women, I = 20%, low-quality evidence), but gastrointestinal side effects were more common with combined therapy (OR 3.97, 95% CI 2.59 to 6.08, 3 studies, 591 women, I = 47%, moderate-quality evidence). However, the combined therapy group had higher rates of clinical pregnancy (OR 1.59, 95% CI 1.27 to 1.99, 16 studies, 1529 women, I = 33%, moderate-quality evidence) and ovulation (OR 1.57, 95% CI 1.28 to 1.92, 21 studies, 1624 women, I = 64%, moderate-quality evidence). There was a statistically significant difference in miscarriage rate per woman, with higher rates in the combined therapy group (OR 1.59, 95% CI 1.03 to 2.46, 9 studies, 1096 women, I = 0%, low-quality evidence) but this is of uncertain clinical significance due to low-quality evidence, and no clear difference between groups when we analysed miscarriage per pregnancy (OR 1.30, 95% CI 0.80 to 2.12, 8 studies; 400 pregnancies, I = 0%, low-quality evidence). Metformin versus clomiphene citrateWhen all studies were combined, findings for live birth were inconclusive and inconsistent (OR 0.71, 95% CI 0.49 to 1.01, 5 studies, 741 women, I = 86%, very low-quality evidence). In subgroup analysis by obesity status, obese women had a lower birth rate in the metformin group (OR 0.30, 95% CI 0.17 to 0.52, 2 studies, 500 women, I = 0%, very low-quality evidence), while data from the non-obese group showed a possible benefit from metformin, with high heterogeneity (OR 1.71, 95% CI 1.00 to 2.94, 3 studies, 241 women, I = 78%, very low-quality evidence). Similarly, among obese women taking metformin there were lower rates of clinical pregnancy (OR 0.34, 95% CI 0.21 to 0.55, 2 studies, 500 women, I = 0%, very low-quality evidence) and ovulation (OR 0.29, 95% CI 0.20 to 0.43 2 studies, 500 women, I = 0%, low-quality evidence) while among non-obese women, the metformin group had more pregnancies (OR 1.56, 95% CI 1.05 to 2.33, 5 studies, 490 women, I = 41%, very low-quality evidence) and no clear difference in ovulation rates (OR 0.81, 95% CI 0.51 to 1.28, 4 studies, 312 women, low-quality evidence, I=0%). There was no clear evidence of a difference in miscarriage rates (overall: OR 0.92, 95% CI 0.50 to 1.67, 5 studies, 741 women, I = 52%, very low-quality evidence). D-chiro-inositol (2 studies), rosiglitazone (1 study) or pioglitazone (1 study) versus placebo or no treatmentWe were unable to draw conclusions regarding other insulin-sensitising drugs as no studies reported primary outcomes.

AUTHORS' CONCLUSIONS: Our updated review suggests that metformin alone may be beneficial over placebo for live birth, although the evidence quality was low. When metformin was compared with clomiphene citrate, data for live birth were inconclusive, and our findings were limited by lack of evidence. Results differed by body mass index (BMI), emphasising the importance of stratifying results by BMI. An improvement in clinical pregnancy and ovulation suggests that clomiphene citrate remains preferable to metformin for ovulation induction in obese women with PCOS.An improved clinical pregnancy and ovulation rate with metformin and clomiphene citrate versus clomiphene citrate alone suggests that combined therapy may be useful although we do not know whether this translates into increased live births. Women taking metformin alone or with combined therapy should be advised that there is no evidence of increased miscarriages, but gastrointestinal side effects are more likely.

摘要

背景

多囊卵巢综合征(PCOS)的特征是排卵稀少或无排卵,以及雄激素和胰岛素水平升高(高胰岛素血症)。高胰岛素血症继发于胰岛素抵抗,与心血管疾病和糖尿病风险增加相关。二甲双胍等胰岛素增敏剂可能有效治疗PCOS相关的无排卵。

目的

评估胰岛素增敏药物在改善接受促排卵治疗的PCOS女性生殖和代谢结局方面的有效性和安全性。

检索方法

我们检索了以下数据库,从创建至2017年1月:Cochrane妇科与生育组专业注册库、CENTRAL、MEDLINE、Embase、PsycINFO和CINAHL。我们检索了正在进行的试验注册库以及相关研究的参考文献列表。

选择标准

我们纳入了将胰岛素增敏药物与安慰剂、不治疗或促排卵药物进行比较的随机对照试验,受试对象为患有少排卵和无排卵PCOS的女性。

数据收集与分析

两位综述作者独立评估研究的合格性和偏倚。主要结局为活产率和胃肠道不良反应。次要结局包括其他妊娠结局、月经频率和代谢效应。我们合并数据以计算合并比值比(OR)和95%置信区间(CI)。我们使用I²统计量评估统计异质性,并使用GRADE方法报告主要结局的证据质量。

主要结果

我们评估了二甲双胍、枸橼酸氯米芬、二甲双胍加枸橼酸氯米芬、D-手性肌醇、罗格列酮和吡格列酮这些干预措施。我们将它们相互比较,以及与安慰剂或不治疗进行比较。我们纳入了48项研究(4451名女性),其中42项研究了二甲双胍(4024名女性)。证据质量从极低到中等不等。局限性包括偏倚风险(方法报告不佳和结局数据不完整)、不精确性和不一致性。二甲双胍与安慰剂或不治疗相比:证据表明,与安慰剂相比,二甲双胍可能提高活产率(OR 1.59,95%CI 1.00至2.51,4项研究,435名女性,I² = 0%,低质量证据)。二甲双胍组胃肠道副作用更多(OR 4.76,95%CI 3.06至7.41,7项研究,670名女性,I² = 61%,中等质量证据),但临床妊娠率更高(OR 1.93,95%CI 1.42至2.64,9项研究,1027名女性,I² = 43%,中等质量证据)、排卵率更高(OR 2.55,95%CI 1.81至3.59,14项研究,701名女性,I² = 58%,中等质量证据)和月经频率更高(OR 1.72,95%CI 1.14至2.61,7项研究,427名女性,I² = 54%,低质量证据)。没有明确证据表明流产率存在差异(OR 1.08,95%CI 0.50至2.35,4项研究,748名女性,I² = 0%,低质量证据)。二甲双胍加枸橼酸氯米芬与单独使用枸橼酸氯米芬相比:两组活产率没有确凿证据表明存在差异(OR 1.21,95%CI 0.92至1.59,9项研究,1079名女性,I² = 20%,低质量证据)但联合治疗胃肠道副作用更常见(OR 3.97,95%CI 2.59至6.08,3项研究,591名女性,I² = 47%,中等质量证据)。然而,联合治疗组临床妊娠率更高(OR 1.59,95%CI 1.27至1.99,16项研究,1529名女性,I² = 33%,中等质量证据)和排卵率更高(OR 1.57,95%CI 1.28至1.92,21项研究,1624名女性,I² = 64%,中等质量证据)。每名女性的流产率存在统计学显著差异,联合治疗组更高(OR 1.59,95%CI 1.03至2.46,9项研究,1096名女性,I² = 0%,低质量证据),但由于证据质量低,其临床意义不确定,且我们分析每次妊娠的流产情况时,两组之间没有明显差异(OR 1.30,95%CI 0.80至2.12,8项研究;400次妊娠,I² = 0%,低质量证据)。二甲双胍与枸橼酸氯米芬相比:当所有研究合并时,活产的结果尚无定论且不一致(OR 0.71,95%CI 0.49至1.01,5项研究,741名女性,I² = 86%,极低质量证据)。在按肥胖状态进行的亚组分析中,肥胖女性在二甲双胍组的出生率较低(OR 0.30,95%CI 0.17至0.52,2项研究,500名女性,I² = 0%,极低质量证据),而非肥胖组的数据显示二甲双胍可能有益,但异质性高(OR 1.71,95%CI 1.00至2.94,3项研究,241名女性,I² = 78%,极低质量证据)。同样,在服用二甲双胍的肥胖女性中,临床妊娠率(OR 0.34,95%CI 0.21至0.55,2项研究,500名女性,I² = 0%,极低质量证据)和排卵率(OR 0.29,95%CI 0.20至0.43,2项研究,500名女性,I² = 0%,低质量证据)较低,而非肥胖女性中,二甲双胍组妊娠更多(OR 1.56,95%CI 1.05至2.33,5项研究,490名女性,I² = 41%,极低质量证据),排卵率无明显差异(OR 0.81,95%CI 0.51至1.28,4项研究,312名女性,低质量证据,I² = 0%)。没有明确证据表明流产率存在差异(总体:OR 0.92,95%CI 0.50至1.67,5项研究,741名女性,I² = 52%,极低质量证据)。D-手性肌醇(2项研究)、罗格列酮(1项研究)或吡格列酮(1项研究)与安慰剂或不治疗相比:由于没有研究报告主要结局,我们无法就其他胰岛素增敏药物得出结论。

作者结论

我们的更新综述表明,单独使用二甲双胍在活产方面可能比安慰剂更有益,尽管证据质量较低。当二甲双胍与枸橼酸氯米芬比较时,活产数据尚无定论,我们的研究结果因缺乏证据而受限。结果因体重指数(BMI)而异,强调了按BMI分层结果的重要性。临床妊娠和排卵的改善表明,对于肥胖的PCOS女性,枸橼酸氯米芬在促排卵方面仍优于二甲双胍。二甲双胍和枸橼酸氯米芬联合使用与单独使用枸橼酸氯米芬相比,临床妊娠和排卵率有所提高,这表明联合治疗可能有用,尽管我们不知道这是否会转化为活产增加。应告知单独服用二甲双胍或联合治疗的女性,没有证据表明流产增加,但胃肠道副作用更有可能发生。

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