Comparison of biosimilar Tigerase and Pulmozyme in long-term symptomatic therapy of patients with cystic fibrosis and severe pulmonary impairment (subgroup analysis of a Phase III randomized open-label clinical trial (NCT04468100))

Amelina, Elena L. and Krasovsky, Stanislav A. and Akhtyamova-Givirovskaya, Nina E. and Kashirskaya, Nataliya Yu. and Abdulganieva, Diana I. and Asherova, Irina K. and Zilber, Ilya E. and Kozyreva, Liliya S. and Kudelya, Lubov M. and Ponomareva, Natalya D. and Revel-Muroz, Nataliya P. and Reutskaya, Elena M. and Stepanenko, Tatiana A. and Seitova, Gulnara N. and Ukhanova, Olga P. and Magnitskaya, Olga V. and Kudlay, Dmitry A. and Markova, Oksana A. and Gapchenko, Elena V. and Plavec, Davor (2021) Comparison of biosimilar Tigerase and Pulmozyme in long-term symptomatic therapy of patients with cystic fibrosis and severe pulmonary impairment (subgroup analysis of a Phase III randomized open-label clinical trial (NCT04468100)). PLOS ONE, 16 (12). e0261410. ISSN 1932-6203

[thumbnail of journal.pone.0261410.pdf] Text
journal.pone.0261410.pdf - Published Version

Download (1MB)

Abstract

Background
Patients with cystic fibrosis (CF) need costly medical care and adequate therapy with expensive medicinal products. Tigerase® is the first biosimilar of dornase alfa, developed by the lead Russian biotechnology company GENERIUM. The aim of the manuscript to present post hoc sub-analysis of patients’ data with cystic fibrosis and severe pulmonary impairment of a larger comparative study (phase III open label, prospective, multi-centre, randomized study (NCT04468100)) of a generic version of recombinant human DNase Tigerase® to the only comparable drug, Pulmozyme®

Methods
In the analyses included subgroup of 46 severe pulmonary impairment patients with baseline FEV1 level 40–60% of predicted (23 patients in each treatment group) out of 100 patients registered in the study phase III open label, prospective, multi-center, randomized study (NCT04468100), and compared efficacy endpoints (FEV1, FVC, number and time of exacerbations, body weight, St.George’s Respiratory Questionnaire) as well as safety parameters (AEs, SAEs, anti-drug antibody) within 24 treatment weeks.

Results
All outcomes were comparable among the studied groups. In the efficacy dataset, the similar mean FEV1 and mean FVC changes for 24 weeks of both treatment groups were observed. The groups were also comparable in safety, all the secondary efficacy parameters and immunogenicity.

Conclusions
The findings from this study support the clinical Tigerase® biosimilarity to Pulmozyme® administered in CF patients with severe impairment of pulmonary function.

Item Type: Article
Subjects: Institute Archives > Biological Science
Depositing User: Managing Editor
Date Deposited: 03 Jan 2023 06:35
Last Modified: 16 Apr 2024 03:59
URI: http://eprint.subtopublish.com/id/eprint/503

Actions (login required)

View Item
View Item