Efficacy and safety of indacaterol/glycopyrronium fixed-dose combination in mild-to-moderate COPD patients symptomatic on tiotropium in Korea: study protocol for a randomized controlled trial

This is a 12-week, randomized, multicenter, open-label, parallel-group, phase IV study. At an initial pre-screening visit (visit 0), a written informed consent will be obtained, followed by assessing the inclusion/exclusion criteria and baseline COPD medication and demographics data. Following a 3-week screening period, at visit 1, eligible patients will be randomized in a 1:1 ratio to receive either once-daily IND/GLY 110/50 μg delivered via the Breezhaler^® device (Novartis Pharma AG, Basel, Switzerland) or once-daily tiotropium 18 μg delivered via the HandiHaler^® device (Boehringer Ingelheim, Ingelheim, Germany) during a 12-week treatment period (Fig. 1). Spirometry measurements assessing the post-bronchodilator FEV_1, along with the baseline dyspnea index (BDI), mMRC and CAT assessments will also be performed at visit 1.During the study, patients will be permitted to use salbutamol/albuterol (short-acting bronchodilator) as a rescue medication, as needed. The schedule of visits and measurements is given in Fig. 2.

This study will be conducted in 20 centers, comprising of general hospitals. The study will be conducted in accordance with the Declaration of Helsinki and Good Clinical Practice guidelines and has been approved by the institutional review boards and ethics committees at participating centers (list included in Additional file 1).

Written informed consent will be obtained from every participant in the study.

The first patient’s first visit for the study took place in January 2016 and the recruitment is expected to conclude by the end of 2017. In line with the inclusion/exclusion criteria, this study aims to enroll a total of 404 symptomatic patients with mild-to-moderate COPD in Korea who would have received tiotropium for at least 12 weeks prior to the study initiation and would be given either IND/GLY or tiotropium for 12 weeks.

The primary objective of the study is to demonstrate the superiority of IND/GLY over tiotropium monotherapy in terms of trough FEV₁ (defined as the mean of the pre-dose 45 and 15 minutes FEV₁ values), following 12 weeks of treatment in patients with mild-to-moderate symptomatic COPD. Secondary objectives are to evaluate pre-dose trough FEV₁ after 4 weeks of treatment, transition dyspnea index (TDI) total score, total CAT score, and rescue medication use following the 12-week treatment. Safety and tolerability will also be assessed over the 12-week treatment. Safety assessment will include monitoring of all the adverse events (AEs) and serious adverse events (SAEs) (regardless of causality); measuring vital signs, including pulse rate and blood pressure; and performing complete physical examinations, clinical laboratory tests, and electrocardiograms. The occurrence of AEs will be sought by non-directive questioning of the patient at each visit during the study or may also be detected by patient volunteering during or between visits or through physical examination, laboratory test, or other assessments.

Exploratory objectives will assess patient preference and satisfaction with IND/GLY in the group of patients receiving IND/GLY, after the patients have been treated with both regimens. Other exploratory outcome measures will comprise of mMRC dyspnea scale scores after 4 and 12 weeks of the treatment and the correlation between patients’ mMRC and CAT scores.

The efficacy analysis will be performed on the full analysis set (FAS), whereas the per protocol set (PPS) will be used for supportive analysis of the primary variable. The FAS will comprise all randomized patients who receive at least one dose of study treatment and will have at least one evaluable post-baseline assessment. The PPS will include all patients in the FAS without any major protocol deviations. All safety analyses will be performed on the safety set comprising of all patients who receive at least one dose of the study treatment.

An analysis of covariance (ANCOVA) model will be used for the primary analysis with treatment, smoking status as fixed effects, baseline trough FEV₁ as a covariate and center as a random effect. The superiority of IND/GLY to tiotropium will be demonstrated if the p value is less than 0.05, and the 95% confidence interval lies entirely to the right of (higher than) 0 mL. In addition, the primary analysis will be repeated for the PPS as a supportive analysis. The missing FEV₁ values will be imputed by the last observation carried forward (LOCF) method.

Moreover, trough FEV₁ at week 4 will be analyzed using an ANCOVA model similar to the primary analysis, with visit and treatment by visit interactions as additional fixed effects. The TDI total score at week 12 will be analyzed using the same ANCOVA model with the baseline dyspnea index (BDI) focal score as the baseline covariate. The proportion of patients with a clinically important improvement of at least 1 in the TDI focal score will be analyzed using logistic regression. The CAT score after 12 weeks of treatment will be summarized based on treatment and analyzed using similar ANCOVA model, with the baseline covariate replaced by baseline CAT score.

This study aims to randomize 182 patients in each treatment arm (IND/GLY and tiotropium) to demonstrate the superiority of IND/GLY over tiotropium in terms of pre-dose trough FEV₁ following 12 weeks of treatment at 5% level of significance with 80% power on a two-sided test. This is based on the assumptions that the estimated treatment difference between IND/GLY and tiotropium is 80 mL and corresponding standard deviation is 271 mL [10]. Therefore, considering a dropout rate of 11%, approximately 404 patients are to be enrolled in the study.

The first patient’s first visit for the study took place in January 2016 and the recruitment is expected to conclude by the end of 2017