Real-World Outcomes in Patients with COPD Initiating Budesonide/Glycopyrronium/Formoterol Fumarate Dehydrate in Spain: ORESTES Study
Bernardino Alcázar Navarrete, Juan Marco Figueira Gonçálves, Carmen Corregidor-García, Eunice Funenga Fitas, Joaquín Sánchez-Covisa, ORESTES group, Eduardo Márquez-Martín, Jose Luis Velasco-Garrido, Marta Martín-Lana, Marta María García-Clemente, Antonia Fuster-Gomila, Jessica González-Gutiérrez, Nuria Bruguera-Avila, Sergio Pascual-Guardia, Galo David Granados-Rosales, Nagore Blanco-Cid, Abel Pallarés-Sanmartín, Raquel Casitas-Mateo, Raúl Galera-Martínez, Carolina María Gotera-Rivera, Juan Margallo-Iribarnegaray, Roberto Bernabeu-Mora, Igor Murga-Arizabaleta, Alberto Saura-Vinuesa, Alberto Herrejón-Silvestre, Hassan Khadour-Khadour
Abstract
INTRODUCTION: Chronic obstructive pulmonary disease (COPD) often results in progressive airflow limitation and is a major cause of morbidity, mortality, and healthcare resource utilization (HCRU). Single-inhaler triple therapy with budesonide/glycopyrronium/formoterol fumarate dehydrate (BGF) is recommended for maintenance in adults with moderate-to-severe COPD not adequately controlled by dual therapy. The ORESTES study aimed to describe the occurrence of exacerbations, clinical characteristics, and HCRU in patients with COPD initiating BGF in a real-life setting in Spain. METHODS: Observational, retrospective, multicenter study in patients with COPD aged ≥ 40 years starting BGF treatment at their physician's discretion in routine clinical practice. Data were retrieved 12 months before and up to 12 months after BGF initiation. Occurrence of exacerbations, HCRU, and use of additional COPD medications, together with the patient demographic and clinical profiles, were evaluated. RESULTS: A total of 718 patients were evaluated, of whom 89.3% completed 12 months of BGF treatment. At BGF initiation, most patients were classified as having high-risk phenotype (72.3%), 78.4% presented with dyspnea (mMRC grade ≥ 2), 50.9% were GOLD E, 93.0% had ≥ 3 comorbidities, and 79.7% ≥ 1 cardiovascular comorbidity. Prior initiation of BGF, 41.1% had received dual therapy and 49.6% triple therapy. After BGF initiation, the proportions of patients experiencing moderate and severe exacerbations decreased by 20.8% and 23.1%, respectively. Additionally, the use of all rescue medication decreased by 21.3%, with a similar reduction (21.1%) observed specifically for short-acting beta-2 agonists (SABA). Oral corticosteroids and antibiotics use decreased 17.1%, and 18.2%, respectively. Primary care visits, admissions to the emergency room, and hospitalizations decreased by 18.0%, 25.5%, and 24.7%, respectively. CONCLUSIONS: These real-world findings suggest that BGF may provide clinical benefit with high treatment persistence in complex, high-risk patients with COPD, even following high-intensity therapy. The observed improvements, despite advanced disease, raise the possibility that earlier initiation of BGF may help optimize outcomes; however, further study is warranted. CLINICAL TRIAL REGISTRATION: NCT06321731.