Haag-Weber Marianne, Eckardt Kai-Uwe, Hörl Walter H, Roger Simon D, Vetter Andrea, Roth Karsten
Department of Nephrology and Hypertension, University of Erlangen-Nürnberg, Erlangen,Germany.
Clin Nephrol. 2012 Jan;77(1):8-17. doi: 10.5414/cn107304.
HX575 is a biosimilar version of epoetin-α that is approved for the treatment of anemia associated with chronic kidney disease (CKD) using the intravenous route of administration. Here we report data from a study of anemic pre-dialysis patients to assess the safety, immunogenicity and efficacy of subcutaneous (s.c.) administration of HX575 vs. Erypo®/Eprex® (Ortho Biotech, Neuss, Germany).
This was a randomized, double-blind study in adult patients (n = 337) with Stage III - V CKD and a hemoglobin (Hb) level of 7.5 - 11.0 g/dl. Eligible patients were randomized to 52 weeks of treatment with HX575 or Erypo®/Eprex® at a starting dose of 25 IU/kg body weight 3 times weekly or 75 IU/kg body weight once weekly during Weeks 1 - 5. This could be adjusted after 5 weeks to maintain Hb levels between 10 and 12 g/dl. The primary objective was to assess the safety and immunogenicity of HX575 compared with Erypo®/Eprex®. Efficacy endpoints were mean absolute change in Hb from baseline to end of Week 13 and mean weekly epoetin dosage in Weeks 11 - 13.
HX575 was equivalent to Erypo®/Eprex® in terms of maintaining Hb levels and epoetin dose requirements. Two patients in the HX575 group developed neutralizing antibodies (NAbs) to erythropoietin, which resulted in the study being terminated prematurely. Aside from these two events, reported adverse events were as expected for patients with Stage III - V CKD and similar in both treatment groups.
This study demonstrated the efficacy and therapeutic equivalence of s.c. HX575 compared with the reference epoetin-α, but 2 patients developed NAbs during treatment with s.c. HX575 in this study. Results of a thorough root-cause analysis reported elsewhere indicate that increased tungsten exposure in pre-filled syringes precipitated immunogenic reactions.
HX575是促红细胞生成素-α的生物类似药,已获批通过静脉给药途径治疗与慢性肾脏病(CKD)相关的贫血。在此,我们报告一项针对贫血的透析前患者的研究数据,以评估皮下注射HX575与Erypo®/Eprex®(德国诺伊斯奥多生物制药公司)相比的安全性、免疫原性和疗效。
这是一项针对成年患者(n = 337)的随机、双盲研究,这些患者患有III - V期CKD,血红蛋白(Hb)水平为7.5 - 11.0 g/dl。符合条件的患者被随机分配接受52周的HX575或Erypo®/Eprex®治疗,起始剂量为25 IU/kg体重,每周3次,或在第1 - 5周期间每周1次,剂量为75 IU/kg体重。5周后可进行调整,以维持Hb水平在10至12 g/dl之间。主要目的是评估HX575与Erypo®/Eprex®相比的安全性和免疫原性。疗效终点为从基线到第13周结束时Hb的平均绝对变化以及第11 - 13周的平均每周促红细胞生成素剂量。
在维持Hb水平和促红细胞生成素剂量需求方面,HX575与Erypo®/Eprex®相当。HX575组有两名患者产生了针对促红细胞生成素的中和抗体(NAbs),这导致研究提前终止。除了这两起事件外,报告的不良事件与III - V期CKD患者预期的情况一致,且两个治疗组相似。
本研究证明了皮下注射HX575与参比促红细胞生成素-α相比的疗效和治疗等效性,但在本研究中,有两名患者在皮下注射HX575治疗期间产生了NAbs。其他地方报告的深入根本原因分析结果表明,预填充注射器中钨暴露增加引发了免疫原性反应。
