Summarized data on concentrations (including endogenous dornase alfa concentrations) showed no statistically significant differences in terms of Cmax (p>0.05) and significant difference in terms of Tmax (p=0.0122). This difference may be explained by fluctuations of endogenous dornase alfa, since dornase alfa has low systemic absorption after inhalation. It should be noted that median values of Tmax were equal in both groups.

Data on concentrations excluding the baseline endogenous dornase alfa concentrations showed no significant differences (p>0.05) of pharmacokinetic parameters between groups (Cmax, AUC0-t, Tmax).

Thus, in phase 1 study it was established that Tigerase and Pulmozyme are comparable in terms of safety, tolerability and pharmacokinetic parameters after 5 days of inhalations in healthy volunteers (Study №КИ 39/14).

A phase 2 open label randomized clinical trial was conducted to compare the pharmacokinetics, efficacy and safety of the biosimilar medicinal product Tigerase (AO Generium, Russia) and the reference medicinal product Pulmozyme (F.Hoffmann-La Roche Ltd, Switzerland) in cystic fibrosis patients. The study included 100 patients aged 18 years and older with a confirmed diagnosis of CF, who were divided into two groups by stratified randomization in a ratio of 1:1 based on the initial level of FEV1 (40–60% or > 60–100% from due value). SM001 or Pulmozyme were used in a dose of 2.5 mg daily, once a day in the form of inhalations using a jet nebulizer compressor for 24 weeks (Study NCT04468100).

The analysis of the data regarding the primary efficacy endpoint – changes in FEV1 – showed that in both groups (FAS population (Full analyses set) and PP population (Per protocol), similar changes in FEV1 were observed. The average value of changes in FEV1 after 24 weeks of treatment compared with the initial level in the FAS population was –1.3% ± 9.8 % (95% CI (–4.1; 1.6) in Group I (Tigerase) and –1.9% ± 10.0% (95% CI (–4.7; 1.0) in Group II (Pulmozyme). The point estimate for the intergroup difference in changes in FEV1 (Group I – Group II) was 0.6%. The calculated 95% CI for the difference in changes in FEV1 in the FAS population was (–3.3; 4.6%]. In both populations studied, the intergroup difference in changes in FEV1 did not exceed 6%. During long-term treatment of patients with CF, no statistically significant differences were found in terms of efficacy (changes in FEV1 and FVC; number of exacerbations of chronic pulmonary disease and the number of days before its development; change in body weight; quality of life) between medicinal products in both studied populations (FAS and PP).

A safety analysis demonstrated the comparability of Tigerase and Pulmozyme in terms of the incidence of adverse events. No statistically significant differences were found in terms of efficacy or pharmacokinetic parameters (Cmax, AUC0-t, Tmax). The frequency of detection of antibodies to dornase alpha during the study was similar in the treatment groups; the formation of antibodies did not lead to a decrease in the efficacy and safety of therapy (Study NCT04468100).