Langbakke Irene H, Nielsen Jakob N, Skettrup Mia P, Harper Angela, Klitgaard Thomas, Weil Angelika, Engelhardt Eva, Lange Martin
Department of Clinical Pharmacology, Novo Nordisk A/S, Bagsvaerd, Denmark.
Clin Endocrinol (Oxf). 2007 Nov;67(5):776-83. doi: 10.1111/j.1365-2265.2007.02962.x. Epub 2007 Jul 18.
GH may be beneficial in treating patients with end-stage renal disease (ESRD). However, the efficacy and safety of GH could be compromised by the potential for accumulation in the circulation.
The objective was to investigate the pharmacokinetics and safety of GH treatment in ESRD patients.
This was an open, nonrandomized, single-centre parallel-group study lasting 8-9 days.
Eleven adult ESRD patients and 10 matched healthy individuals received recombinant human GH (50 microg/kg/day for 7 days) by subcutaneous injection; there were two dose reductions (25%) from Day 5/7. ESRD patients underwent dialysis four times.
Serum concentrations of GH, insulin-like growth factor-I (IGF-I), insulin-like growth factor binding protein-I (IGFBP-I), IGFBP-III and GHBP were measured. The primary end-point was GH exposure [area-under-the-curve (AUC) calculated from the 24-h profile] on Days 7-8.
GH AUC(0-24 h) was greater for patients (387.91 +/- 134.13 microg h/l) than healthy subjects (225.35 +/- 59.63 microg h/l) and the 90% confidence interval (CI) for the estimated patient : healthy subject ratio (1.40-2.07) was not within the acceptance interval (0.67-1.50). GH AUC(18-24 h) for patients and healthy subjects (3.03 +/- 2.71 microg h/l and 6.37 +/- 4.21 microg h/l) returned approximately to baseline (2.86 +/- 3.91 microg h/l and 1.09 +/- 1.43 microg h/l); terminal half-life (t(1/2,z)) was shorter for patients (2.28 +/- 00.43 h vs. 3.23 +/- 00.75 h). No major safety issues were identified.
Results demonstrate a difference between patients and healthy subjects regarding GH AUC(0-24 h). However, GH concentrations for both groups were comparable to baseline by 20-22 h, thus GH was not retained in the circulation of ESRD patients.
生长激素(GH)可能对终末期肾病(ESRD)患者的治疗有益。然而,GH在循环中的潜在蓄积可能会影响其疗效和安全性。
研究GH治疗ESRD患者的药代动力学及安全性。
这是一项开放、非随机、单中心平行组研究,持续8 - 9天。
11例成年ESRD患者和10例匹配的健康个体接受重组人生长激素(50μg/kg/天,共7天)皮下注射;从第5/7天起剂量减少两次(每次25%)。ESRD患者每周进行4次透析。
检测血清GH、胰岛素样生长因子-I(IGF-I)、胰岛素样生长因子结合蛋白-I(IGFBP-I)、IGFBP-III和GH结合蛋白(GHBP)的浓度。主要终点是第7 - 8天的GH暴露量[根据24小时曲线计算的曲线下面积(AUC)]。
患者的GH AUC(0 - 24 h)(387.91±134.13μg·h/l)高于健康受试者(225.35±59.63μg·h/l),患者与健康受试者估计比值的90%置信区间(CI)(1.40 - 2.07)不在可接受区间(0.67 - 1.50)内。患者和健康受试者的GH AUC(18 - 24 h)(分别为3.03±2.71μg·h/l和6.37±4.21μg·h/l)大约恢复到基线水平(分别为2.86±3.91μg·h/l和1.09±1.43μg·h/l);患者的终末半衰期(t(1/2,z))较短(2.28±0.43小时对3.23±0.75小时)。未发现重大安全问题。
结果表明患者与健康受试者在GH AUC(0 - 24 h)方面存在差异。然而,两组的GH浓度在20 - 22小时时与基线水平相当,因此GH未在ESRD患者的循环中蓄积。
