Background- Generic formulations of pirfenidone are increasingly adopted in idiopathic pulmonary fibrosis (IPF), yet real-world evidence supporting their clinical equivalence to the originator remains limited. We aimed to evaluate whether switching from branded pirfenidone (Esbriet®) to a generic formulation affects treatment efficacy or tolerability. Methods- We conducted a retrospective, within-patient observational study including consecutive patients with IPF treated with Esbriet® for ≥6 months before switching to generic pirfenidone. Pulmonary function was assessed at three time points: 6 months before the switch (T−6), at switch (T0), and 6 months after (T+6). The primary endpoint was the within-patient percentage change in FVC over two consecutive 6-month periods (T−6→T0 vs T0→T+6), analysed within a pre-specified equivalence framework (±5 percentage points). Secondary endpoints included DLCO changes and treatment related adverse events (AEs), analysed at the patient level using paired comparisons. Results- Sixty-five patients (median age 77.0 years [72.3–80.0] years, 78% male) had complete functional follow-up. The mean percentage decline in FVC was −1.9% before the switch and −1.7% after the switch. The estimated between-period difference in FVC change was 0.2 percentage points (95% CI −1.1 to 1.5), fully contained within the pre-specified equivalence margins. Similar findings were observed for DLCO, with no significant difference between periods. Overall, 43% of patients experienced at least one AE during treatment. Gastrointestinal AEs were the most frequent, but paired analyses showed no significant difference in patient-level AE occurrence between branded and generic periods. No severe AEs or treatment discontinuations were observed. Conclusions- In this real-world cohort of patients with IPF, switching from branded to generic pirfenidone was not associated with clinically meaningful differences in lung function decline or treatment tolerability.
Efficacy and Tolerability of Generic Pirfenidone After Switch from Esbriet® in Idiopathic Pulmonary Fibrosis: A Real-World Observational Study / Tonelli, Roberto; Giulia Turchiano, Maria; Moretti, Antonio; Andrisani, Dario; Gozzi, Filippo; Raineri, Giulia; Samarelli, Anna Valeria; Ruggieri, Valentina; Clini, Enrico; Cerri, Stefania. - In: INTERNAL AND EMERGENCY MEDICINE. - ISSN 1828-0447. - (2026), pp. 1-9. [10.1007/s11739-026-04343-9]
Efficacy and Tolerability of Generic Pirfenidone After Switch from Esbriet® in Idiopathic Pulmonary Fibrosis: A Real-World Observational Study
Roberto Tonelli;Giulia Raineri;Anna Valeria Samarelli;Enrico Clini
;Stefania Cerri
2026
Abstract
Background- Generic formulations of pirfenidone are increasingly adopted in idiopathic pulmonary fibrosis (IPF), yet real-world evidence supporting their clinical equivalence to the originator remains limited. We aimed to evaluate whether switching from branded pirfenidone (Esbriet®) to a generic formulation affects treatment efficacy or tolerability. Methods- We conducted a retrospective, within-patient observational study including consecutive patients with IPF treated with Esbriet® for ≥6 months before switching to generic pirfenidone. Pulmonary function was assessed at three time points: 6 months before the switch (T−6), at switch (T0), and 6 months after (T+6). The primary endpoint was the within-patient percentage change in FVC over two consecutive 6-month periods (T−6→T0 vs T0→T+6), analysed within a pre-specified equivalence framework (±5 percentage points). Secondary endpoints included DLCO changes and treatment related adverse events (AEs), analysed at the patient level using paired comparisons. Results- Sixty-five patients (median age 77.0 years [72.3–80.0] years, 78% male) had complete functional follow-up. The mean percentage decline in FVC was −1.9% before the switch and −1.7% after the switch. The estimated between-period difference in FVC change was 0.2 percentage points (95% CI −1.1 to 1.5), fully contained within the pre-specified equivalence margins. Similar findings were observed for DLCO, with no significant difference between periods. Overall, 43% of patients experienced at least one AE during treatment. Gastrointestinal AEs were the most frequent, but paired analyses showed no significant difference in patient-level AE occurrence between branded and generic periods. No severe AEs or treatment discontinuations were observed. Conclusions- In this real-world cohort of patients with IPF, switching from branded to generic pirfenidone was not associated with clinically meaningful differences in lung function decline or treatment tolerability.
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Tonelli (comparison of branded vs generic pirfenidone in IPF- 2026).pdf
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