Jockenhövel F, Vogel E, Kreutzer M, Reinhardt W, Lederbogen S, Reinwein D
Abteilung für Endokrinologie, Zentrum für Innere Medizin, Universitätsklinik Essen, Germany.
Clin Endocrinol (Oxf). 1996 Jul;45(1):61-71. doi: 10.1111/j.1365-2265.1996.tb02061.x.
There are advantages and disadvantages with all of the presently available types of testosterone replacement for hypogonadal men. We performed this investigation to establish detailed data about the pharmacokinetics, pharmacodynamics, feasibility and side-effects of subcutaneously implanted testosterone (T) pellets.
In a single-dose, open-label, non-randomized study, 6 T-pellets, each containing 200 mg of fused crystalline T, were implanted in the subdermal fat tissue of the lower abdominal wall of 14 hypogonadal men. Blood samples for determination of T, LH, FSH, 5 alpha-dihydrotestosterone (DHT), sex hormone binding globulin (SHBG) and oestradiol (E2) were obtained at 0, 0.5, 1, 2, 4, 8, 12, 24, 36, 48 hours and on day 21 after implantation and then every 3 weeks until day 189, and on days 246 and 300 during follow-up. In another 36 hypogonadal men the feasibility and side-effects of T-pellets were evaluated.
Fourteen patients participated in the detailed pharmacokinetic study and another 36 patients in the assessment of feasibility and side-effects. All patients (age range 18-61 years) suffered from primary or secondary hypogonadism (T < 3.6 nmol/l).
The pharmacokinetic study in 14 hypogonadal men revealed an initial short-lived burst release of T with a peak concentration of 49.0 +/- 3.7 nmol/l at 0.5 +/- 0.13 days which was followed by a stable plateau lasting until day 63 (day 2, 35.2 +/- 2.3; day 63, 34.8 +/- 2.6 nmol/l). Thereafter serum T gradually declined and was close to baseline concentrations on day 300. Apparent terminal elimination half-life (t1/2) was 70.8 +/- 10.7 days and apparent mean residence time 87.0 +/- 4.5 days. On average, serum T was below 10 nmol/l after 180 days. Absorption of T followed a zero-order release kinetic with an absorption half-time of 74.7 days (95% confidence interval: 71.1-78.5) and was almost complete by day 189 (95.9 +/- 0.84%). Serum DHT and E2 were significantly elevated from day 21 to day 105 and correlated significantly with T (DHT, r = 0.65, P < 0.0001, E2, r = 0.67, P < 0.0001). SHBG was significantly decreased from day 21 to day 168. In 6 men with primary hypogonadism T suppressed LH and FSH to the eugonadal range from day 21 to 126 and 42 to 105, respectively, with nadirs occurring at day 84 (LH) and day 63 (FSH). LH and FSH were highly inversely correlated with T (r = -0.47 and -0.57). The only side-effect observed during 112 implantations in the total group of 50 men were 6 local infections (5.4%) leading to extrusion of 5 pellets in 3 men. When given the choice, all patients except one preferred T-pellets to their previous T medication for permanent substitution therapy.
T-pellets are the androgen formulation with the longest biological action and strongest pharmacodynamic efficacy in terms of gonadotrophin suppression. The pharmacokinetic features are advantageous compared to other T preparations and the patient acceptance is high.
目前所有用于性腺功能减退男性的睾酮替代类型都各有优缺点。我们开展此项研究以获取皮下植入睾酮(T)丸剂的药代动力学、药效学、可行性及副作用的详细数据。
在一项单剂量、开放标签、非随机研究中,将6粒T丸剂(每粒含200mg融合结晶T)植入14例性腺功能减退男性下腹壁的皮下脂肪组织。在植入后0、0.5、1、2、4、8、12、24、36、48小时、第21天,然后每3周直至第189天,以及随访期间的第246天和第300天采集血样,用于测定T、LH、FSH、5α - 双氢睾酮(DHT)、性激素结合球蛋白(SHBG)和雌二醇(E2)。在另外36例性腺功能减退男性中评估了T丸剂的可行性和副作用。
14例患者参与了详细的药代动力学研究,另外36例患者参与了可行性和副作用评估。所有患者(年龄范围18 - 61岁)均患有原发性或继发性性腺功能减退(T < 3.6 nmol/l)。
14例性腺功能减退男性的药代动力学研究显示,T最初有一个短暂的突发释放,在0.5±0.13天达到峰值浓度49.0±3.7 nmol/l,随后是一个稳定的平台期,持续到第63天(第2天,35.2±2.3;第63天,34.8±2.6 nmol/l)。此后血清T逐渐下降,在第300天接近基线浓度。表观终末消除半衰期(t1/2)为70.8±10.7天,表观平均驻留时间为87.0±4.5天。平均而言,180天后血清T低于10 nmol/l。T的吸收遵循零级释放动力学,吸收半衰期为74.7天(95%置信区间:71.1 - 78.5),到第189天几乎完全吸收(95.9±0.84%)。从第21天到第105天,血清DHT和E2显著升高,且与T显著相关(DHT,r = 0.65,P < 0.0001;E2,r = 0.67,P < 0.0001)。从第21天到第168天,SHBG显著降低。在6例原发性性腺功能减退男性中,T分别从第21天到126天以及第42天到105天将LH和FSH抑制到正常性腺功能范围,最低点分别出现在第84天(LH)和第63天(FSH)。LH和FSH与T高度负相关(r = -0.47和 -0.57)。在总共50名男性的112次植入过程中观察到的唯一副作用是6例局部感染(5.4%),导致3名男性的5粒丸剂挤出。当有选择时,除1名患者外,所有患者在永久性替代治疗中更喜欢T丸剂而非他们之前的T药物。
就促性腺激素抑制而言,T丸剂是生物作用时间最长且药效学效力最强的雄激素制剂。与其他T制剂相比,其药代动力学特征具有优势,患者接受度高。
