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促性腺激素缺乏男性中人类促卵泡激素的药代动力学

Pharmacokinetics of human follicle-stimulating hormone in gonadotropin-deficient men.

作者信息

Handelsman D J, Turner L, Boylan L M, Conway A J

机构信息

Andrology Unit, Royal Prince Alfred Hospital, Sydney, New South Wales, Australia.

出版信息

J Clin Endocrinol Metab. 1995 May;80(5):1657-63. doi: 10.1210/jcem.80.5.7745014.

DOI:10.1210/jcem.80.5.7745014
PMID:7745014
Abstract

Gonadotropin treatment of hypogonadotropic infertile men usually requires regular im administration of human urinary FSH (uFSH); however, testicular function is rarely normalized despite years of treatment. As the pharmacokinetics of standard FSH doses (75 IU, two or three times weekly) in gonadotropin-deficient men are poorly characterized, we studied 10 gonadotropin-deficient men by measuring plasma FSH levels with an ultrasensitive fluoroimmunoassay (Delfia, Pharmacia) in single dose and multidose studies. The single dose studies involved blood samples taken 15 min before and 0, 1, 2, 4, 6, 8, 10, 12, 15, 18, 21, 24, 48, 72, and 96 h after the injection of 75 IU uFSH in 1 mL diluent, either sc under the abdominal wall skin or im into the deltoid muscle, in a random sequence, cross-over design (n = 7 men) and after the injection of 150 IU, sc, with additional blood sampling at 120 and 168 h (n = 7 men). The multidose studies used a fixed ascending dose sequence, with blood sampled at 24-h intervals posttreatment after at least 1 month of regular administration of either 75 or 150 IU uFSH, sc, at injection intervals of 72, 48, and 24 h (n = 6 men). From the single dose studies, pharmacokinetic variables were estimated from a one-compartment open model fitted by a weighted polyexponential curve fit of plasma FSH over time. The bioavailability of uFSH via the sc route was high (mean area under the curve, 90% for 75 IU and 143% for 150 IU vs. 75 IU, im). Peak plasma FSH levels were later (21.1 vs. 7.1 h; P < 0.001) and lower (2.0 vs. 2.7 IU/L; P < 0.001) after sc compared with im administration of 75 IU due to a slower absorption half-time (6.1 h vs. 1.4 h; P < 0.001), whereas mean residence times and clearance half-times were similar. The pharmacokinetic features of the 150- and 75-IU doses sc were essentially identical, apart from expected dose-dependent increases in peak plasma FSH level (2.8 vs. 2.0 IU/L; P < 0.001) and area under the curve (206 vs. 129 IU.h/L; P < 0.05). Multidose simulations based on the single dose pharmacokinetic models predicted that during chronic sc administration of standard FSH doses, plasma FSH levels would be in the lower half of the eugonadal range and fluctuate less than with im administration. The multidose study confirmed empirically these predictions. These studies form a pharmacological basis for a more flexible, cost-effective, and convenient self-administered sc regimen.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

促性腺激素治疗低促性腺激素性不育男性通常需要定期肌肉注射人尿促卵泡素(uFSH);然而,尽管经过多年治疗,睾丸功能很少恢复正常。由于缺乏促性腺激素男性中标准FSH剂量(75 IU,每周两到三次)的药代动力学特征尚不明确,我们通过超灵敏荧光免疫分析法(Delfia,Pharmacia)在单剂量和多剂量研究中测量血浆FSH水平,对10名促性腺激素缺乏男性进行了研究。单剂量研究包括在1 mL稀释剂中注射75 IU uFSH后,于注射前15分钟以及注射后0、1、2、4、6、8、10、12、15、18、21、24、48、72和96小时采集血样,注射方式为经皮下腹壁皮肤或肌肉注射入三角肌,采用随机序列交叉设计(n = 7名男性),以及在皮下注射150 IU后,于120和168小时额外采集血样(n = 7名男性)。多剂量研究采用固定的递增剂量序列,在至少1个月定期皮下注射75或150 IU uFSH后,以72、48和24小时的注射间隔,于治疗后每隔24小时采集血样(n = 6名男性)。从单剂量研究中,通过对血浆FSH随时间的加权多指数曲线拟合得到的一室开放模型估算药代动力学变量。uFSH经皮下途径的生物利用度较高(曲线下平均面积,75 IU时为90%,150 IU时为143%,相比肌肉注射75 IU)。与肌肉注射75 IU相比,皮下注射后血浆FSH峰值水平出现较晚(21.1小时对7.1小时;P < 0.001)且较低(2.0 IU/L对2.7 IU/L;P < 0.001),这是由于吸收半衰期较慢(6.1小时对1.4小时;P < 0.001),而平均驻留时间和清除半衰期相似。皮下注射150 - 和75 - IU剂量的药代动力学特征基本相同,除了血浆FSH峰值水平(2.8 IU/L对2.0 IU/L;P < 0.001)和曲线下面积(206 IU·h/L对129 IU·h/L;P < 0.05)有预期的剂量依赖性增加。基于单剂量药代动力学模型的多剂量模拟预测,在长期皮下注射标准FSH剂量期间,血浆FSH水平将处于正常性腺功能范围的下半部分,且波动小于肌肉注射。多剂量研究通过实验证实了这些预测。这些研究为更灵活、经济有效且方便的自我皮下给药方案奠定了药理学基础。(摘要截选至400字)

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