Department of Clinical Pharmacology and Therapeutics, Seoul National University College of Medicine and Hospital, Seoul, Republic of Korea.
Clin Ther. 2010 Oct;32(11):1968-76. doi: 10.1016/j.clinthera.2010.10.001.
Recombinant human erythropoietin is indicated for the treatment of anemia resulting from chronic renal failure or chemotherapy. It is also used for patients at high risk for transfusions because of significant blood loss during surgery. A new recombinant human erythropoietin (epoetin alfa) that excludes fetal bovine serum and human serum albumin from among its ingredients was developed in Korea. This study was planned as part of a product development project at the request of the Korean regulatory agency.
The aim of this study was to compare the pharmacokinetic and pharmacodynamic characteristics of a new recombinant human erythropoietin (test) formulation with an existing branded (reference) formulation after a single subcutaneous administration.
An open-label, sequence-randomized, 2-period, 2-sequence, 2-treatment crossover study was conducted. Healthy male subjects were randomly assigned with a random number table into 1 of 2 sequence groups, and each subject was given recombinant human erythropoietin 4000 IU SC in the upper arm as the test formulation in one period and the reference formulation in the other period, according to the sequence group. Each period was separated by a 4-week washout period. Serial blood samples were taken up to 120 hours after drug administration for the pharmacokinetic assessments and up to 240 hours for reticulocyte counts as the pharmacodynamic end point. Pharmacokinetic analysis was performed without baseline correction. Adverse events (AEs) were collected by spontaneous reporting of the subjects or solicited by asking general health-related questions.
Twenty healthy men (mean [range] age, 25.6 [21-36] years; height, 175 [167-187] cm; weight, 70 [57.6-85.5] kg) were enrolled in and completed the study. The mean (SD) baseline erythropoietin plasma concentrations were 10.4 (2.4) mIU/mL for the test formulation and 10.8 (3.5) mIU/mL for the reference formulation. After the injection of 4000 IU SC per subject, the erythropoietin plasma concentrations reached a maximum at a median T(max) of 10 hours for both formulations (range: test formulation, 7.00-95.95 hours; reference formulation, 6.98-24.13 hours). The mean (SD) C(max) values for the test and reference formulations were 74.34 (30.63) and 80.46 (30.56) mIU/mL, respectively; the mean AUC(0-last) values were 3664 (731.5) and 3553 (723.2) mIU·h/mL. The ratios of the geometric mean (test/reference) for C(max) and AUC(0-last) were 0.92 (90% CI, 0.81-1.05) and 1.03 (90% CI, 0.98-1.09). The mean baseline hemoglobin, hematocrit, and reticulocyte counts were 15.4 g/dL, 45.5%, and 49.6 · 10(3)/μL, respectively, for the test formulation and 15.5 g/dL, 45.3%, and 47.5 · 10(3)/μL for the reference formulation. The mean reticulocyte counts slowly reached T(max) for both formulations at a median of 120 hours after administration (test formulation, 120.0 hours [range, 95.5-240.8 hours]; reference formulation, 120.1 hours [range, 72.0-240.5 hours]). The mean (SD) maximum reticulocyte counts for the test and reference formulations were 77.7 (12.2) · 10(3)/μL and 80.7 (15.2) · 10(3)/μL, respectively; values for area under the effect curve to the last observation (AUEC(0-last)) were 14,781.5 (2439.2) · 10(3)/μL · h and 14,783.8 (2415.4) · 10(3)/μL · h. The 2 agents did not exhibit any significant differences in maximum reticulocyte counts or AUEC(0-last). During the study, a total of 6 AEs were reported, which were mild in severity. After the administration of test formulation, 1 case each of rhinorrhea, epigastric discomfort, and joint sprain (left ankle) were reported. After the administration of reference formulation, 2 cases of rhinorrhea and 1 case of cough were reported.
In this small, selected group of healthy male volunteers, there were no significant differences in pharmacokinetic parameters or effects on reticulocytes between a test formulation and a reference formulation of recombinant human erythropoietin.
重组人红细胞生成素用于治疗慢性肾衰竭或化疗引起的贫血。它也用于因手术期间大量失血而有显著输血风险的患者。一种新的重组人红细胞生成素(epoetin alfa)已在韩国开发,其成分中不包含胎牛血清和人血清白蛋白。这项研究是作为韩国监管机构要求的产品开发项目的一部分进行的。
本研究旨在比较单次皮下给予新型重组人红细胞生成素(试验)制剂与现有品牌(参比)制剂后的药代动力学和药效学特征。
这是一项开放标签、随机、2 期、2 序列、2 治疗交叉研究。健康男性受试者通过随机数字表被随机分配到 2 个序列组中的 1 个,根据序列组,每组受试者在一个时期内接受重组人红细胞生成素 4000IU SC 在上臂,另一个时期接受参比制剂。每个时期之间有 4 周的洗脱期。在给药后至 120 小时进行血清样本采集,以进行药代动力学评估,至 240 小时进行网织红细胞计数作为药效学终点。药代动力学分析未经基线校正进行。通过受试者自发报告或通过询问一般健康相关问题收集不良事件(AE)。
20 名健康男性(平均[范围]年龄,25.6[21-36]岁;身高,175[167-187]cm;体重,70[57.6-85.5]kg)被纳入并完成了这项研究。试验制剂和参比制剂的基线红细胞生成素血浆浓度分别为 10.4(2.4)mIU/mL 和 10.8(3.5)mIU/mL。每位受试者皮下注射 4000IU 后,红细胞生成素血浆浓度在 10 小时达到中位数 T(max),两种制剂均为 10 小时(范围:试验制剂为 7.00-95.95 小时;参比制剂为 6.98-24.13 小时)。试验和参比制剂的 C(max)值分别为 74.34(30.63)和 80.46(30.56)mIU/mL,AUC(0-last)值分别为 3664(731.5)和 3553(723.2)mIU·h/mL。C(max)和 AUC(0-last)的几何均数(试验/参比)比值分别为 0.92(90%CI,0.81-1.05)和 1.03(90%CI,0.98-1.09)。试验制剂和参比制剂的基线血红蛋白、血细胞比容和网织红细胞计数分别为 15.4g/dL、45.5%和 49.6·10(3)/μL,15.5g/dL、45.3%和 47.5·10(3)/μL。两种制剂的网织红细胞计数均在 120 小时缓慢达到 T(max),中位数为 120 小时(试验制剂,120.0 小时[范围,95.5-240.8 小时];参比制剂,120.1 小时[范围,72.0-240.5 小时])。试验和参比制剂的最大网织红细胞计数分别为 77.7(12.2)·10(3)/μL 和 80.7(15.2)·10(3)/μL,AUC(0-last)至最后观察的效应曲线下面积分别为 14781.5(2439.2)·10(3)/μL·h 和 14783.8(2415.4)·10(3)/μL·h。两种制剂的最大网织红细胞计数或 AUC(0-last)均无显著差异。在研究期间,共报告了 6 例不良事件,均为轻度。给予试验制剂后,分别报告了 1 例鼻塞、上腹部不适和左踝关节扭伤。给予参比制剂后,分别报告了 2 例鼻塞和 1 例咳嗽。
在这个小型、选择性的健康男性志愿者群体中,新型重组人红细胞生成素试验制剂与参比制剂在药代动力学参数或对网织红细胞的影响方面没有显著差异。
