Grimes D, Gallo M, Grigorieva V, Nanda K, Schulz K
Family Health International, P. O. Box 13950, Research Triangle Park, North Carolina 27709, USA.
Cochrane Database Syst Rev. 2004(3):CD004316. doi: 10.1002/14651858.CD004316.pub2.
Male hormonal contraception has been an elusive goal. Administration of sex steroids to men can shut off sperm production through effects on the pituitary and hypothalamus. However, this approach also decreases production of testosterone, so "add-back" therapy is needed.
To summarize all randomized controlled trials of male hormonal contraception.
We searched the computerized databases Cochrane Central Register of Controlled Trials (CENTRAL), MEDLINE, EMBASE, Popline, and LILACS (each from inception to February, 2003) for randomized controlled trials of hormonal contraception in men. We wrote to authors of identified trials to seek unpublished or published trials that we might have missed.
We included all randomized controlled trials in any language that compared a steroid hormone with another contraceptive. We excluded non-steroidal male contraceptives, such as gossypol. We included both placebo and active-regimen control groups. All trials identified included only healthy men with normal semen analyses.
Azoospermia (absence of spermatozoa on semen examination) was the primary outcome measure. Data were insufficient to examine pregnancy rates and side effects.
The proportion of men who achieved azoospermia varied widely in reports to date. Few significant differences emerged from these trials. Levonorgestrel implants combined with injectable testosterone enanthate (100 mg IM) was significantly more effective than was levonorgestrel 125 mcg by mouth daily combined with testosterone patches (10 mg/d) (OR for azoospermia with the oral levonorgestrel regimen 0.03; 95%CI 0.00-0.29). The addition of levonorgestrel 500 mcg by mouth daily improved the effectiveness of testosterone enanthate 100 mg IM weekly by itself (OR for azoospermia with the combined regimen 4.0; 95%CI 1.00-15.99). Several regimens, including testosterone alone and GnRH agonists and antagonists, had disappointing results.
REVIEWERS' CONCLUSIONS: No male hormonal contraceptive is ready for clinical use. All trials published to date have been small exploratory studies. As a result, their power to detect important differences has been limited and their results imprecise. In addition, the definition of oligospermia has been imprecise or inconsistent in many reports. To avoid bias, future trials need more attention to the methodological requirements for randomized controlled trials. Trials with adequate power would also be helpful.
男性激素避孕一直是一个难以实现的目标。对男性施用性类固醇可通过影响垂体和下丘脑来抑制精子生成。然而,这种方法也会降低睾酮的生成,因此需要“补充”疗法。
总结所有男性激素避孕的随机对照试验。
我们检索了计算机化数据库Cochrane对照试验中心注册库(CENTRAL)、医学索引(MEDLINE)、荷兰医学文摘数据库(EMBASE)、人口信息数据库(Popline)和拉丁美洲及加勒比卫生科学数据库(LILACS)(均从建库至2003年2月),以查找男性激素避孕的随机对照试验。我们致函已识别试验的作者,以寻找我们可能遗漏的未发表或已发表的试验。
我们纳入了所有语言的随机对照试验,这些试验比较了一种类固醇激素与另一种避孕方法。我们排除了非甾体类男性避孕药,如棉酚。我们纳入了安慰剂和活性方案对照组。所有已识别的试验仅纳入精液分析正常的健康男性。
无精子症(精液检查中无精子)是主要结局指标。数据不足以检查妊娠率和副作用。
迄今为止的报告中,实现无精子症的男性比例差异很大。这些试验中几乎没有出现显著差异。左炔诺孕酮植入剂联合注射用庚酸睾酮(100 mg,肌内注射)比每日口服125 mcg左炔诺孕酮联合睾酮贴片(10 mg/d)显著更有效(口服左炔诺孕酮方案的无精子症比值比为0.03;95%可信区间为0.00 - 0.29)。每日口服500 mcg左炔诺孕酮可提高每周单独注射100 mg庚酸睾酮的有效性(联合方案的无精子症比值比为4.0;95%可信区间为1.00 - 15.99)。包括单独使用睾酮以及促性腺激素释放激素(GnRH)激动剂和拮抗剂在内的几种方案,结果令人失望。
尚无男性激素避孕药可用于临床。迄今为止发表的所有试验均为小型探索性研究。因此,它们检测重要差异的能力有限,结果也不精确。此外,在许多报告中,少精子症的定义不精确或不一致。为避免偏倚,未来的试验需要更多关注随机对照试验的方法学要求。有足够检验效能的试验也会有所帮助。
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