Dobs A S, Meikle A W, Arver S, Sanders S W, Caramelli K E, Mazer N A
Johns Hopkins Medical Center, Baltimore, Maryland 21287, USA.
J Clin Endocrinol Metab. 1999 Oct;84(10):3469-78. doi: 10.1210/jcem.84.10.6078.
The pharmacokinetics, efficacy, and safety of the Androderm testosterone (T) transdermal system (TTD) and intramuscular T enanthate injections (i.m.) for the treatment of male hypogonadism were compared in a 24-week multicenter, randomized, parallel-group study. Sixty-six adult hypogonadal men (22-65 years of age) were withdrawn from prior i.m. treatment for 4-6 weeks and then randomly assigned to treatment with TTD (two 2.5-mg systems applied nightly) or i.m. (200 mg injected every 2 weeks); there were 33 patients per group. Twenty-six patients in the TTD group and 32 in the i.m. group completed the study. TTD treatment produced circadian variations in the levels of total T, bioavailable T, dihydrotestosterone, and estradiol within the normal physiological ranges. i.m. treatment produced supraphysiological levels of T, bioavailable T, and estradiol (but not dihydrotestosterone) for several days after each injection. Mean morning sex hormone levels were within the normal range in greater proportions of TTD patients (range, 77-100%) than i.m. patients (range, 19-84%). Both treatments normalized LH levels in approximately 50% of patients with primary hypogonadism; however, LH levels were suppressed to the subnormal range in 31% of i.m. patients vs. 0% of TTD patients. Both treatments maintained sexual function (assessed by questionnaire and Rigiscan) and mood (Beck Depression Inventory) at the prior treatment levels. Prostate-specific antigen levels, prostate volumes, and lipid and serum chemistry parameters were comparable in both treatment groups. Transient skin irritation from the patches was reported by 60% of the TTD patients, but caused only three patients (9%) to discontinue treatment. i.m. treatment produced local reactions in 33% of patients and was associated with significantly more abnormal hematocrit elevations (43.8% of patients) compared with TTD treatment (15.4% of patients). Gynecomastia resolved more frequently during TTD treatment (4 of 10 patients) than with i.m. treatment (1 of 9 patients). Although both treatments seem to be efficacious for replacing T in hypogonadal men, the more physiological sex hormone levels and profiles associated with TTD may offer possible advantages over i.m. in minimizing excessive stimulation of erythropoiesis, preventing/ameliorating gynecomastia, and not over-suppressing gonadotropins.
在一项为期24周的多中心、随机、平行组研究中,比较了安特尔睾酮(T)透皮系统(TTD)和肌肉注射庚酸睾酮(i.m.)治疗男性性腺功能减退的药代动力学、疗效和安全性。66名成年性腺功能减退男性(22 - 65岁),在停止先前的肌肉注射治疗4 - 6周后,被随机分配接受TTD治疗(每晚使用两片2.5毫克系统)或肌肉注射(每2周注射200毫克);每组33例患者。TTD组26例患者和i.m.组32例患者完成了研究。TTD治疗使总T、生物可利用T、双氢睾酮和雌二醇水平在正常生理范围内产生昼夜变化。肌肉注射治疗在每次注射后的几天内使T、生物可利用T和雌二醇水平高于生理范围(但双氢睾酮水平未升高)。TTD组患者早晨性激素平均水平在正常范围内的比例(77% - 100%)高于肌肉注射组患者(19% - 84%)。两种治疗方法使约50%的原发性性腺功能减退患者的促黄体生成素(LH)水平恢复正常;然而,31%的肌肉注射组患者LH水平被抑制至低于正常范围,而TTD组患者中这一比例为0%。两种治疗方法都将性功能(通过问卷和阴茎硬度扫描仪评估)和情绪(贝克抑郁量表)维持在先前治疗水平。两个治疗组的前列腺特异性抗原水平、前列腺体积以及血脂和血清化学参数相当。60%的TTD组患者报告有贴片引起的短暂皮肤刺激,但只有3例患者(9%)因此停止治疗。肌肉注射治疗使33%的患者出现局部反应,与TTD治疗(15.4%的患者)相比,与血细胞比容异常升高显著相关(43.8%的患者)。TTD治疗期间乳腺增生消退的患者(10例中的4例)比肌肉注射治疗(9例中的1例)更常见。虽然两种治疗方法似乎都能有效替代性腺功能减退男性体内的T,但与TTD相关的更生理性的性激素水平和变化模式,在最小化对红细胞生成的过度刺激、预防/改善乳腺增生以及不过度抑制促性腺激素方面,可能比肌肉注射具有潜在优势。
