Anderson R A, Wallace A M, Wu F C
Medical Research Council Reproductive Biology Unit, Center for Reproductive Biology, Edinburgh, Scotland.
J Clin Endocrinol Metab. 1996 Mar;81(3):902-8. doi: 10.1210/jcem.81.3.8772548.
The administration of exogenous testosterone (T) to eugonadal men causes suppression of gonadotropin secretion and thus of spermatogenesis. This is currently being investigated as a possible method of hormonal male contraceptive, but complete suppression of spermatogenesis to azoospermia is induced in only 50-70% of Caucasian men; the remainder maintain a low rate of spermatogenesis. The basis for this polymorphism in response is unclear. The enzyme 5 alpha-reductase (5 alpha R) converts T to dihydrotestosterone (DHT) and is important in determining the magnitude of the androgen stimulus in some tissues. We investigated whether the maintenance of spermatogenesis in men remaining oligozoospermic while receiving suppressive doses of T is associated with evidence of increased 5 alpha R activity. Thirty-three normal men were given 200 mg T enanthate (TE), im, weekly in a clinical trial of hormonal male contraception. The MCR of T (MCRT) and the conversion ratio of T to DHT (CRT-DHT) were measured by infusion of [3H]T, plasma levels of DHT and androstanediol glucuronide (AdiolG) were measured by RIA, and 24-h urinary steroid metabolites were measured by capillary column gas chromatography. Sperm density decreased in all men; 18 achieved azoospermia by 20 weeks of treatment, and the remainder had a mean sperm density of 2.0 +/- 0.8 x 10(5)/mL at that time. This treatment caused increases in plasma T levels and MCRT, but with no differences between azoospermic and oligozoospermic responders. There were no differences in CRT-DHT plasma DHT, or AdiolG before treatment, but after 16 weeks, CRT-DHT had increased in the oligozoospermic responders, but not in the azoospermic responders. TE treatment increased plasma DHT and AdiolG levels in both groups, but the increases in both 5 alpha R metabolites were significantly greater in the oligozoospermic responders. Urinary excretion of etiocholanolone and androsterone was increased after 16 weeks of TE treatment, but did not differ between the two groups, andetiocholanolone/androsterone ratios did not differ greatly from unity. There was no change in urinary excretion of tetrahydrocortisol, allo-tetrahydrocortisol, or cortisone after 16 weeks of TE treatment in either group. These results suggest that after TE administration there is a selective increase in 5 alpha R activity in those men who remain oligozoospermic, but not in those becoming azoospermic. This difference in the androgenic milieu may underlie the incomplete suppression in the oligozoospermic responders, in whom a low rate of spermatogenesis is maintained despite the apparent absence of gonadotropins.
给性腺功能正常的男性外源性注射睾酮(T)会抑制促性腺激素分泌,进而抑制精子发生。目前正在研究这作为一种激素男性避孕的可能方法,但仅50 - 70%的白人男性会出现精子发生完全抑制至无精子症;其余男性维持低水平的精子发生。这种反应多态性的基础尚不清楚。5α - 还原酶(5αR)将T转化为二氢睾酮(DHT),在确定某些组织中雄激素刺激的程度方面很重要。我们研究了在接受抑制剂量T时仍保持少精子症的男性中精子发生的维持是否与5αR活性增加的证据相关。在一项激素男性避孕临床试验中,33名正常男性每周肌肉注射200mg庚酸睾酮(TE)。通过输注[3H]T测量T的代谢清除率(MCRT)以及T向DHT的转化比率(CRT - DHT),通过放射免疫分析法测量DHT和雄甾二醇葡萄糖醛酸苷(AdiolG)的血浆水平,并通过毛细管柱气相色谱法测量24小时尿甾体代谢物。所有男性的精子密度均下降;18名男性在治疗20周时达到无精子症,其余男性此时的平均精子密度为2.0±0.8×10⁵/mL。这种治疗导致血浆T水平和MCRT升高,但无精子症和少精子症反应者之间无差异。治疗前CRT - DHT、血浆DHT或AdiolG无差异,但16周后,少精子症反应者的CRT - DHT升高,而无精子症反应者未升高。TE治疗使两组的血浆DHT和AdiolG水平均升高,但少精子症反应者中这两种5αR代谢物的升高均显著更大。TE治疗16周后,尿中本胆烷醇酮和雄酮的排泄增加,但两组之间无差异,且本胆烷醇酮/雄酮比率与1无太大差异。两组在TE治疗16周后,尿中四氢皮质醇、别 - 四氢皮质醇或可的松的排泄均无变化。这些结果表明,在给予TE后,仍保持少精子症的男性中5αR活性有选择性增加,而变为无精子症的男性中则没有。雄激素环境的这种差异可能是少精子症反应者抑制不完全的基础,尽管明显缺乏促性腺激素,但这些男性仍维持低水平的精子发生。
