Behre H M, Baus S, Kliesch S, Keck C, Simoni M, Nieschlag E
Institute of Reproductive Medicine of the University (WHO Collaborating Center for Research in Human Reproduction), Münster, Germany.
J Clin Endocrinol Metab. 1995 Aug;80(8):2394-403. doi: 10.1210/jcem.80.8.7543113.
Suppression of serum LH and FSH, by testosterone (T) alone or in combination with other agents, has proved to be the most promising approach to male contraception. T enanthate, the only androgen preparation tested in male contraceptive efficacy trials so far, must be injected every week due to its short terminal elimination half-life of 4.5 days and leads to supraphysiological T serum levels. A new T ester synthesized under WHO and NIH auspices, testosterone buciclate (TB), showed a favorable pharmacokinetic profile, with a terminal half-life of 29.5 days when tested in hypogonadal men. Here we describe the results of the first clinical trial with TB for male contraception. After two control examinations, normal healthy male volunteers were given a single im injection of 600 mg TB (group I; n = 4) and 1200 mg TB (group II; n = 8) on day 0. Follow-up examinations were performed every 2 weeks up to week 32. In both groups mean serum T levels remained in the normal physiological range throughout the study course. Serum levels of dihydrotestosterone (DHT) showed a dose- and time-dependent increase, with serum levels slightly above the normal range in group II for several weeks and a maximal concentration of 3.8 +/- 0.5 nmol/L (mean +/- SE) in week 6. No suppression of spermatogenesis to oligozoospermia was observed in group I. However, in group II, spermatogenesis was suppressed to azoospermia in three of eight volunteers in week 10 that persisted up to weeks 14, 20, and 22, respectively. In these three men, LH and FSH were suppressed by TB injections to the respective assay detection limits, whereas in the other five subjects, mean serum levels were only decreased to values near the lower normal limit for LH and FSH, respectively. In addition, throughout the study course, a significant difference in serum sex hormone-binding globulin was detected between the responders (mean values, 21.2-26.4 nmol/L) and nonresponders (mean values, 36.2-46.3 nmol/L). Serum levels of LH as well as total and free T at baseline and after TB injection were lower in the responders than in the nonresponders. Both subgroups showed similar increases in serum LH and FSH after GnRH stimulation. In a newly introduced GnRH antagonist suppression test, serum LH and T were decreased to significantly lower levels in the responders. These results indicate a different hormonal equilibrium and probably different susceptibility to feedback regulation of the responders compared to the nonresponders.(ABSTRACT TRUNCATED AT 400 WORDS)
单独使用睾酮(T)或与其他药物联合使用来抑制血清促黄体生成素(LH)和促卵泡生成素(FSH),已被证明是男性避孕最有前景的方法。目前在男性避孕效果试验中测试过的唯一雄激素制剂庚酸睾酮,因其较短的终末消除半衰期4.5天,必须每周注射,并且会导致血清T水平高于生理水平。在世界卫生组织(WHO)和美国国立卫生研究院(NIH)的支持下合成的一种新的睾酮酯,环布氯睾酮(TB),显示出良好的药代动力学特征,在性腺功能减退男性中进行测试时终末半衰期为29.5天。在此,我们描述了TB用于男性避孕的首次临床试验结果。经过两次对照检查后,在第0天,正常健康男性志愿者单次肌肉注射600mg TB(I组;n = 4)和1200mg TB(II组;n = 8)。在第32周之前每2周进行一次随访检查。在整个研究过程中,两组的平均血清T水平均保持在正常生理范围内。双氢睾酮(DHT)的血清水平呈剂量和时间依赖性增加,II组在数周内血清水平略高于正常范围,在第6周时最大浓度为3.8±0.5nmol/L(平均值±标准误)。I组未观察到精子发生抑制至少精子症。然而,在II组中,8名志愿者中有3名在第10周时精子发生被抑制至无精子症,分别持续到第14、20和22周。在这三名男性中,TB注射使LH和FSH被抑制至各自的检测下限,而在其他五名受试者中,平均血清水平仅分别降至LH和FSH正常下限附近的值。此外,在整个研究过程中,应答者(平均值为21.2 - 26.4nmol/L)和非应答者(平均值为36.2 - 46.3nmol/L)之间血清性激素结合球蛋白存在显著差异。应答者在基线和注射TB后的LH以及总T和游离T血清水平均低于非应答者。两个亚组在促性腺激素释放激素(GnRH)刺激后血清LH和FSH的升高相似。在新引入的GnRH拮抗剂抑制试验中,应答者的血清LH和T降至显著更低水平。这些结果表明,与非应答者相比,应答者存在不同的激素平衡,并且可能对反馈调节的敏感性不同。(摘要截断于400字)
