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辅助生殖中用于垂体抑制的促性腺激素释放激素激动剂方案。

Gonadotrophin-releasing hormone agonist protocols for pituitary suppression in assisted reproduction.

作者信息

Maheshwari Abha, Gibreel Ahmed, Siristatidis Charalambos S, Bhattacharya Siladitya

机构信息

Division of Applied Health Sciences, University of Aberdeen, Aberdeen, UK, AB25 2ZL.

出版信息

Cochrane Database Syst Rev. 2011 Aug 10(8):CD006919. doi: 10.1002/14651858.CD006919.pub3.

DOI:10.1002/14651858.CD006919.pub3
PMID:21833958
Abstract

BACKGROUND

Gonadotrophin-releasing hormone agonists (GnRHa) are used in assisted reproduction technology (ART) cycles to prevent a luteinizing hormone surge. Various protocols have been described in the literature, such as long protocols (continuous and stop or reduce dose, long luteal, or long follicular protocol); short protocols and ultrashort protocols.

OBJECTIVES

To determine the most effective GnRHa protocol as an adjuvant to gonadotrophins in ART cycles.

SEARCH STRATEGY

We searched the Cochrane Menstrual Disorders and Subfertility Group Specialised Register, Cochrane Central Register of Controlled Trials (CENTRAL) (The Cochrane Library), MEDLINE, EMBASE, CINHAHL and PsycINFO. Reference lists of relevant articles were also searched. All the searches were updated to August 2010.

SELECTION CRITERIA

Only randomised controlled trials comparing any two protocols of GnRHa in in vitro fertilization (IVF) or intra-cytoplasmic sperm injection (ICSI) cycles were included.

DATA COLLECTION AND ANALYSIS

The primary outcome measure was live births per women. Secondary outcome measures were pregnancy rate, ongoing pregnancy rate, number of oocytes retrieved and amount of gonadotrophins used. Data were independently extracted in 2 x 2 tables by two authors. Odds ratios (OR) with 95% confidence intervals (CI) were calculated after verifying the presence of homogeneity of treatment effect across all trials. For continuous variables mean differences (MD) were calculated.

MAIN RESULTS

Of 29 included studies, 17 compared long with short protocols; two compared long with ultrashort protocols; four compared a follicular versus luteal start of GnRHa; three compared continuation versus stopping the GnRHa at the start of stimulation; three compared continuation of the same dose versus reduced dose of GnRHa and one compared a short versus short stop protocol.There was no evidence of a difference in the live birth rate but this outcome was only reported by three studies.There was evidence of a significant increase in clinical pregnancy rate (OR 1.50, 95% CI 1.16 to 1.93) in a long protocol when compared to a short protocol. That is there is a 50% increase in chance of achieving pregnancy if a long protocol is used as compared to a short protocol, although this difference could range from 16% to 93% increased chance of pregnancy. This difference did not persist when the meta-analysis was done only on the studies with adequate randomisation (OR 1.38, 95% CI 0.93 to 2.05).There was evidence of an increased number of oocytes (MD 1.61, 95% CI 0.18 to 3.04) obtained when a long protocol was used as compared to a short protocol. That is there is a 60% increase in the number of oocytes retrieved when a long protocol is used as compared to a short protocol, although this difference could range from 18% to 304% more oocytes.There was evidence of an increase (MD 12.90, 95% CI 3.29 to 22.51) in the requirement for gonadotrophins in long as compared to short protocols. That is approximately 12.9 more ampoules of gonadotrophins were consumed when a long protocol was used as compared to a short protocol. This difference could range from 3.29 to 22.51 more gonadotrophin ampoules.There was no evidence of a difference in any of the outcome measures for luteal versus follicular start of GnRHa and stopping versus continuation of GnRHa at the start of stimulation.

AUTHORS' CONCLUSIONS: The pregnancy rate was found to be higher when GnRHa was used in a long protocol as compared to a short or ultrashort protocol. There was no evidence of a difference in live birth rate, but this outcome was only reported by three studies. There was no evidence of a difference in the outcomes amongst various long protocols; nor that stopping or reducing GnRHa at the start of stimulation was associated with a reduced pregnancy rate. For all comparison, except a long versus short protocol, there was a lack of power.

摘要

背景

促性腺激素释放激素激动剂(GnRHa)用于辅助生殖技术(ART)周期,以防止促黄体生成素激增。文献中描述了各种方案,如长方案(持续及停药或减量、长黄体期或长卵泡期方案);短方案和超短方案。

目的

确定在ART周期中作为促性腺激素辅助药物的最有效GnRHa方案。

检索策略

我们检索了Cochrane月经紊乱与亚生育专业注册库、Cochrane对照试验中心注册库(CENTRAL)(Cochrane图书馆)、MEDLINE、EMBASE、CINAHL和PsycINFO。还检索了相关文章的参考文献列表。所有检索更新至2010年8月。

入选标准

仅纳入比较体外受精(IVF)或卵胞浆内单精子注射(ICSI)周期中任何两种GnRHa方案的随机对照试验。

数据收集与分析

主要结局指标是每位女性的活产数。次要结局指标是妊娠率、持续妊娠率、获卵数及促性腺激素用量。数据由两位作者独立提取到2×2表格中。在核实所有试验治疗效果的同质性后,计算95%置信区间(CI)的比值比(OR)。对于连续变量,计算平均差(MD)。

主要结果

纳入的29项研究中,17项比较了长方案与短方案;2项比较了长方案与超短方案;4项比较了GnRHa的卵泡期起始与黄体期起始;3项比较了刺激开始时继续使用GnRHa与停止使用GnRHa;3项比较了相同剂量继续使用GnRHa与减量使用GnRHa,1项比较了短方案与短停药方案。没有证据表明活产率存在差异,但只有三项研究报告了该结局。有证据表明,与短方案相比,长方案的临床妊娠率显著增加(OR 1.50,95%CI 1.16至1.93)。即与短方案相比,使用长方案时妊娠机会增加50%,尽管这种差异可能导致妊娠机会增加16%至93%。仅对随机化充分的研究进行Meta分析时,这种差异不再存在(OR 1.38,95%CI 0.93至2.05)。有证据表明,与短方案相比,使用长方案时获得的卵母细胞数量增加(MD 1.61,95%CI 0.18至3.04)。即与短方案相比,使用长方案时获卵数增加60%,尽管这种差异可能导致卵母细胞数量增加18%至304%。有证据表明,与短方案相比,长方案中促性腺激素的需求量增加(MD 12.90,95%CI 3.29至22.51)。即与短方案相比,使用长方案时大约多消耗12.9支促性腺激素安瓿。这种差异可能导致多消耗3.29至22.51支促性腺激素安瓿。没有证据表明GnRHa的黄体期起始与卵泡期起始以及刺激开始时停止使用与继续使用GnRHa在任何结局指标上存在差异。

作者结论

与短方案或超短方案相比,GnRHa用于长方案时妊娠率更高。没有证据表明活产率存在差异,但只有三项研究报告了该结局。没有证据表明各种长方案之间的结局存在差异;也没有证据表明刺激开始时停止或减少GnRHa与妊娠率降低有关。对于所有比较,除了长方案与短方案外,均缺乏检验效能。

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