54 episodes before study entry; this was reduced to 026 during p

54 episodes before study entry; this was reduced to 0.26 during prophylaxis with Human-cl rhFVIII (Fig. 3). The efficacy of Human-cl rhFVIII in the treatment of breakthrough bleeding was rated as excellent in 71.4% of cases and good in 28.6% of cases. 88.9% of all bleeding episodes were managed with one (81.5%) or two (7.4%) infusions. The median dose per infusion was 32.1 IU kg−1, range 20–53. In the attempt to compare GENA-01 and GENA-08 study results, adult patients on prophylactic regimens with Human-cl rhFVIII experienced significantly fewer bleeding episodes than

those using on-demand treatment (Fig. 4). There was a 96% reduction in mean monthly bleeding rates with prophylaxis vs. on-demand treatment (4.77 vs. 0.19, Fig. 4), whereas factor consumption increased by a factor of 3 (156.9 vs. 474.1 IU kg−1 month−1). In summary, these studies in adult and selleck compound adolescent patients with severe haemophilia A indicated that Human-cl rhFVIII is safe and effective in the Erismodegib molecular weight prevention and treatment of bleeding episodes. There were no product-related serious adverse events and none of the PTPs treated with Human-cl rhFVIII developed inhibitors or an allergic reaction. It is concluded that prophylaxis with Human-cl rhFVIII, in comparison to on-demand treatment in a comparable cohort, appears to prevent >90% of bleeding episodes in adults with severe haemophilia A. A completed Phase III

study (GENA-03) investigated the pharmacokinetics, efficacy, safety and immunogenicity of Human-cl rhFVIII in previously treated children aged 2–12 years with severe haemophilia A. The primary objectives of the trial were to assess the efficacy of prophylactic treatment and the treatment of breakthrough bleeding. The secondary objectives were to measure pharmacokinetics in different age groups, incremental recovery of FVIII:C, immunogenicity, efficacy during surgery, safety and tolerability. Fifty-nine patients from 15 sites in seven countries (UK, Poland, France, Russia,

Turkey, Romania and Czech Republic) were enroled. Thirteen children from each age group (younger group I: 2–5 years, older group II: 6–12 years) participated in the comparative pharmacokinetic investigation. Prophylactic treatment was given as 30–40 IU kg−1 every other day or three times per week for ≥6 months and ≥50 exposure days. With regard to demographics the mean age of the children 上海皓元医药股份有限公司 was 6.1 years (range 2–12); weight was 26.7 kg (range 8–73), all patients were white and 53 patients (89.8%) were on prophylaxis prior to the start of the study. Mean pharmacokinetic parameters of Human-cl rhFVIII were similar for the chromogenic and the one-stage assay (Fig. 5). In younger children (2–5 years old) the half-life was 9.49 ± 3.32 h for the chromogenic assay and 11.91 ± 5.36 for the one-stage assay. The corresponding figures in older children (6–12 years old) were 9.99 ± 1.88 h and 13.08 ± 2.59 h, respectively. In vivo recovery remained stable throughout the study.

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