Healthy Male Subjects Clinical Trial
Official title:
Evaluation of Dose-response, Pharmacodynamic and Pharmacokinetic Bioequivalence of Filgrastim in Healthy Male Volunteers After Single and Multiple-dose Subcutaneous Administration of the BK0023 Injectable Formulation vs. Neupogen®
Study rationale: Bio-ker has developed the new formulation of filgrastim BK0023 with the
same active content as Neupogen®. BK0023 is expected to have the same tolerability profile
and clinical effects as Neupogen® in controlling myelo-toxicity induced by chemotherapy
given for the treatment of solid and haematological tumours. It is worth noting that the
production and manufacturing procedures allow to have a reduction of drug cost thus it is
likely to have pharmacoeconomic advantages.
The study is aimed at investigating the pharmacodynamic equivalence and the pharmacokinetic
bioequivalence of the new BK0023 injectable formulation of filgrastim 0.3 mg/mL by Bio-Ker
S.r.l. vs. the comparator (Neupogen® 0.3 mg/mL, Dompé Biotec S.p.A., Italy). Healthy male
subjects will receive test and reference at the doses of 2.5 and 5 µg/kg/day for 7
consecutive days and at the dose of 10 µg/kg/day for 5 consecutive days according to a
randomised cross-over design. Pharmacodynamics, pharmacokinetics and safety of BK0023
injectable formulation 0.3 mg/mL and of Neupogen® 0.3 mg/mL, administered in 2 consecutive
periods with a wash-out of at least 28 days elapsing between the last injection of period I
and the first of period II, are compared.
Study design: Single and multiple escalating dose, double-blind, randomised, two-way
cross-over, pharmacodynamic and pharmacokinetic bioequivalence study.
In a first part of the study, 16 healthy male subjects will be included in each dose group
and will receive test and reference product according to the cross-over design. After the
end of the second period of each dose group (completion of both cross-over periods for each
dose group) the pharmacodynamic and pharmacokinetic primary parameters will be calculated.
The blinding will be temporarily broken by one statistician for the ad interim analysis of
primary parameters that will be performed after conclusion of the treatment of 16 subjects
for each dose group (results are not disclosed) with the aim to re-calculate the sample size
and to conclude the study with the necessary and sufficient number of subjects for each dose
regimen.
The study design was chosen according to the internationally recognised guideline for
pharmacokinetics studies and in accordance with the EMEA guidance on similar medicinal
products containing recombinant granulocyte-colony stimulating factor (G-CSF), which is
annexed to the guideline on similar biological medicinal products containing
biotechnology-derived proteins as active substance: non-clinical and clinical issues. A
clinical development plan including the study outline was also submitted to EMEA, which
examined the documentation and gave advice about the present study design .
A multiple-dose design was chosen instead of a single-dose design, since G-CSF
pharmacokinetics is non linear due to 2 reasons: non-proportional increase with dose and
time dependent non-linearity. However, pharmacodynamic equivalence and pharmacokinetic
bioequivalence will be both tested after the 1st and the last dose of the multiple dose
treatment.
Since the effects of r-h-met-G-CSF can be directly measured as pharmacodynamic responses,
i.e. the increase in the absolute neutrophil count (ANC) and the development of peripheral
blood cells (CD34+ cells), both parameters will be evaluated for the equivalence testing.
Dose levels of 2.5 and 5 μg/kg/day were chosen for the pharmacodynamic equivalence, since
literature data show a clear dose-response relationship in terms of the pharmacodynamic
parameters over this range. The 10 μg/kg/day dose was chosen to make the investigated range
relevant with respect to the clinical indications and the usual praxis for Neupogen®.
Moreover, the subcutaneous administration was chosen, since this administration route is the
most commonly used in the clinical setting.
;
Allocation: Randomized, Endpoint Classification: Bio-equivalence Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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