Weigang-Köhler Karin, Vetter Andrea, Thyroff-Friesinger Ursula
Klinikum Nurnberg Nord/5, Medizinische Klinik, Nürnberg, Germany.
Onkologie. 2009 Apr;32(4):168-74. doi: 10.1159/000200783. Epub 2009 Mar 6.
Recombinant human epoetin alfa, HX575, is the first biosimilar erythropoiesis-stimulating agent (ESA) with European marketing authorisation. The primary objective of this double-blind, randomised, multicentre study was to assess the efficacy and safety of HX575 in treating chemotherapy-associated symptomatic anaemia in patients with solid tumours.
The patients (n = 114) were treated with HX575 or active control (epoetin alfa) at 150 IU/kg body weight 3 times weekly for 12 weeks, increased to 300 IU/kg body weight 3 times weekly if the haemoglobin/reticulocyte increase was insufficient after 4 or 8 weeks.
With HX575, haemoglobin increased by > or =20 g/l in 62% (37/60 patients). The confidence interval (48.2%, 73.9%) was entirely above the pre-defined 30% threshold. Both groups showed similar results for safety profiles and secondary efficacy parameters. Transfusion requirements were 32% (19/60) (HX575) and 38% (13/34) (epoetin alfa).
In treating chemotherapy-associated symptomatic anaemia in patients with solid tumours, the biosimilar ESA, HX575, is efficacious with a safety profile as expected for the therapeutic area.
重组人促红细胞生成素α(HX575)是首个获得欧洲上市许可的生物类似物促红细胞生成剂(ESA)。这项双盲、随机、多中心研究的主要目的是评估HX575治疗实体瘤患者化疗相关症状性贫血的疗效和安全性。
114例患者接受HX575或活性对照(促红细胞生成素α)治疗,体重150 IU/kg,每周3次,共12周;如果4周或8周后血红蛋白/网织红细胞升高不足,则增加至体重300 IU/kg,每周3次。
使用HX575治疗的患者中,62%(37/60例)血红蛋白升高≥20 g/l。置信区间(48.2%,73.9%)完全高于预先设定的30%阈值。两组在安全性和次要疗效参数方面结果相似。输血需求分别为32%(19/60)(HX575组)和38%(13/34)(促红细胞生成素α组)。
在治疗实体瘤患者化疗相关症状性贫血方面,生物类似物ESA HX575有效,且具有该治疗领域预期的安全性。