Background §§ Two large clinical studies (TONADO® 1 + 2) demonstrated the benefits of treatment with a combination of once-daily tiotropium (T), a long-acting muscarinic antagonist, and olodaterol (O), a long-acting 2 -agonist, compared to treatment with the monocomponents in patients with moderate to very severe chronic obstructive pulmonary disease (COPD) over 52 weeks.1 §§ Until recently, the focus of treatment had been on improving the single outcome of lung function. However, it is becoming clear that many factors come into play as COPD deteriorates, and it is of interest to investigate whether these clinically significant events can also be delayed with optimized bronchodilation, which, in turn, could lead to longer-term disease stabilization. §§ A post hoc analysis of the UPLIFT study demonstrated that composite end points, which included clinically significant events for patients with Global initiative for chronic Obstructive Lung Disease (GOLD) 2 and GOLD stage B COPD, can be sensitive to treatment effects, with T delaying clinically significant events compared to placebo.2 §§ The two composite end points in the UPLIFT analysis evaluated the time to first clinically important deterioration in: (1) trough forced expiratory volume in 1 second (FEV1 ), St. George’s Respiratory Questionnaire (SGRQ) score, severe exacerbation, or death; or (2) trough FEV1 , SGRQ score, or moderate or severe exacerbation.2 The first composite end point showed limitations, with the severe exacerbations and death components not of value in patients with moderate COPD. §§ Using the same methodology as for the UPLIFT analysis, we investigated whether T+O is more effective than T at delaying clinically significant events in patients with GOLD stage B COPD (symptomatic COPD and a low risk of exacerbations) in a post hoc analysis of the TONADO® studies. Methods Study design §§ A total of 5162 patients were randomized to T+O 2.5/5 µg or 5/5 µg, T 2.5 µg or 5 µg, or O 5 µg (delivered via Respimat® inhaler) in two 52-week, parallel-group, double-blind studies (TONADO® 1 [NCT01431274] and TONADO® 2 [NCT01431287]) (Figure 1). §§ Assessment of trough FEV1 was performed on Day 1 and at Weeks 2, 6, 12, 18, 24, 32, 40, and 52. §§ SGRQ was completed on Day 1 and after 12, 24, and 52 weeks. Analyses §§ Post hoc analysis of time to first clinically important deterioration in patients classified as GOLD stage B using combined TONADO® study data. §§ Clinically important deterioration was defined according to two composite end points. –– Composite end point 1: time to first decrease in trough FEV1 from baseline of 100 mL, time to first increase in SGRQ total score from baseline of 4 units, time to first severe (hospitalized) exacerbation, or time to death. –– Composite end point 2: time to first decrease in trough FEV1 from baseline of 100 mL, time to first increase in SGRQ total score from baseline of 4 units, or time to first moderate or severe exacerbation. §§ The time to first occurrence of one of these events was recorded as the time to clinically important deterioration. §§ Data are presented for comparisons of the licensed doses of T+O 5/5 µg and T 5 µg. Statistical analyses §§ Time to first clinically significant event (individual components of composite end points) and time to first clinical deterioration (composite end points) were calculated in days and reported for the 25th percentile (median time not reached for most events) for each treatment group. §§ Hazard ratios (HRs) for treatment comparisons were obtained from fitting a Cox proportional hazard regression model with treatment as the only covariate. §§ Kaplan–Meier estimates of probability of clinical deterioration based on the composite end points were generated for each treatment group. Results §§ Patient demographics and disease characteristics were comparable for GOLD stage B patients in the T+O 5/5 µg and T 5 µg treatment groups included in this analysis (Table 1). §§ Using composite end point 1 (time to first trough FEV1 decline, SGRQ total score increase, severe exacerbation, or death), time to clinically important deterioration was significantly longer with T+O 5/5 µg than T 5 µg (HR [95% confidence interval (CI)] 0.65 [0.52, 0.81]; p0.0001) (Figure 2). §§ For the individual clinically significant events included in composite end point 1, time to trough FEV1 decline (HR [95% CI] 0.66 [0.51, 0.86]; p=0.0016) and time to SGRQ score increase (HR [95% CI] 0.71 [0.52, 0.96]; p=0.0271) were significantly longer with T+O 5/5 µg than T 5 µg (Table 2). –– Event rates for time to severe exacerbation and time to death were very low (one death and 16 patients with severe exacerbations across both treatment groups) and 25th percentiles were non-estimable. §§ For time to moderate or severe exacerbation, the HR (95% CI) was 0.94 (0.67, 1.32) and 25th percentiles were non-estimable (Table 2). However, event rates were greater than for severe exacerbations: T+O 5/5 µg, 67 patients (21.6%); T 5 µg, 69 patients (22.5%). §§ Using composite end point 2 (including time to first trough FEV1 decline, SGRQ total score increase, or moderate or severe exacerbation, and excluding severe exacerbation or death), time to clinically important deterioration was significantly longer with T+O 5/5 µg than T 5 µg (HR [95% CI] 0.68 [0.56, 0.83]; p=0.0002) (Figure 3) Limitations §§ In contrast to the UPLIFT study analysis,2 a clinically significant event did not have to be confirmed at a second clinic visit in order to be included in the analysis. This was a consequence of the length of the TONADO® studies (52 weeks) and the number of assessments occurring during this period (only three SGRQ assessments). §§ The temporal relationship between clinically significant events is not known, as only the time to first individual event is included in the analysis. Benefits of tiotropium + olodaterol over tiotropium at delaying clinically significant events in patients with COPD classified as GOLD B Roland Buhl,1 Lorcan McGarvey,2 Stephanie Korn,1 Gary T. Ferguson,3 Lars Grönke,4 Christoph Hallmann,4 Florian Voß,4 Klaus F. Rabe,5 François Maltais6 1 Pulmonary Department, Mainz University Hospital, Mainz, Germany; 2 Centre for Infection and Immunity, School of Medicine, Dentistry and Biomedical Sciences, Queen’s University Belfast, Belfast, UK; 3 Pulmonary Research Institute of Southeast Michigan, Farmington Hills, Michigan, USA; 4 Boehringer Ingelheim Pharma GmbH & Co. KG, Ingelheim, Germany; 5 Lung Clinic Grosshansdorf, Grosshansdorf, Germany; 6 Centre de Recherche, Institut Universitaire de Cardiologie et de Pneumologie de Québec, Québec, Canada http://goo.gl/7Eya01 Poster presented at the American Thoracic Society International Conference, San Francisco, California, USA, May 13–18, 2016 Poster P9 References 1. Buhl R et al. Eur Respir J 2015; 45: 969–979. 2. Rabe K et al. Abstract presented at the American Thoracic Society Annual Meeting, San Francisco, California, USA, May 13–18, 2016. Acknowledgments This study was supported by Boehringer Ingelheim. Under the authors’ conceptual direction, medical writing assistance for this poster was provided by Gail Rickard at Complete HealthVizion; medical writing assistance was supported by Boehringer Ingelheim. Disclosures RB reports financial support to his institution from Boehringer Ingelheim during the conduct of the study, and outside of the submitted work, financial support from Boehringer Ingelheim, AstraZeneca, Chiesi, Novartis, TEVA, Roche, and GlaxoSmithKline for attendance at advisory boards and speaking activities, and research support to his institution from Boehringer Ingelheim, GlaxoSmithKline, Novartis, and Roche. FM reports financial support from Boehringer Ingelheim during the conduct of the study, and, outside of the submitted work, financial support from Boehringer Ingelheim and GlaxoSmithKline for attendance at advisory boards, financial support from Boehringer Ingelheim, GlaxoSmithKline, AstraZeneca, and Novartis for speaking activities, and research support from Boehringer Ingelheim, GlaxoSmithKline, AstraZeneca, Nycomed, and Novartis. Conclusions §§ In the TONADO® studies, T+O increased time to clinically important deterioration compared to T alone in patients with GOLD stage B COPD, suggesting that T+O is more effective than T in preventing these significant events in this patient population. §§ Based on these results, T+O not only significantly improves lung function but may also lead to a slower clinical deterioration of the disease through its effects beyond lung function. §§ For this patient population with less severe disease, and in which severe exacerbations and deaths occur infrequently, it appears that comparing the effectiveness of different treatments in delaying clinically important deterioration can be achieved using a composite end point that includes time to first trough FEV1 decline or SGRQ score increase, or moderate or severe exacerbation. §§ Further studies are warranted to prospectively study this effect. Figure 2. Kaplan–Meier estimates of probability of decline from baseline in trough FEV1 of 100 mL, increase from baseline of 4 units in SGRQ score, severe exacerbation, or death (composite end point 1) in patients with GOLD stage B COPD.a 1.00 Estimatedprobabilityofnoevent 0.95 0.90 0.85 0.80 0.75 0.70 0.65 0.60 0.55 0.50 0.45 0.40 0.35 0.30 0.25 0.20 0.15 0.10 0.05 0.00 0 50 100 150 200 250 300 350 Patients at risk T+O 5/5 µg T 5 µg 278 239 310 306 229 187 220 172 192 141 177 128 163 112 166 114 Study day 380 Patients with event, n (%) 188 (61.4) 150 (48.4) HR (95% CI) 0.65 (0.52, 0.81) p value <0.0001 Time to event (25th percentile), days 85 128 T+OT T+O 5/5 µg T 5 µg a Full analysis set Figure 3. Kaplan–Meier estimates of probability of decline from baseline in trough FEV1 of 100 mL, increase from baseline of 4 units in SGRQ score, or moderate or severe exacerbation (composite end point 2) in patients with GOLD stage B COPD.a 1.00 Estimatedprobabilityofnoevent 0.95 0.90 0.85 0.80 0.75 0.70 0.65 0.60 0.55 0.50 0.45 0.40 0.35 0.30 0.25 0.20 0.15 0.10 0.05 0.00 0 50 100 150 200 250 300 350 380 Patients at risk T+O 5/5 µg T 5 µg 267 229 310 306 217 179 201 161 175 128 156 112 136 94 143 98 Study day Patients with event, n (%) 210 (68.6) 174 (56.1) HR (95% CI) 0.68 (0.56, 0.83) p value 0.0002 Time to event (25th percentile), days 78 89 T+OT T+O 5/5 µg T 5 µg a Full analysis set Figure 1. TONADO® 1 + 2 study designs. -2 0 2 52 +324a Weeks Run-in R Treatment T+O Respimat® 5/5 µg once daily T+O Respimat® 2.5/5 µg once daily O Respimat® 5 µg once daily T Respimat® 5 µg once daily T Respimat® 2.5 µg once daily Follow-up S C R E E N I N G a Primary end-point assessment R, randomization Table 1. Baseline demographic and disease characteristics for GOLD B patients with COPD: treated set. T 5 µg T+O 5/5 µg Patients, n 307 311 Male, n (%) 199 (64.8) 210 (67.5) Mean ± SD age, years 63.4 ± 9.3 63.8 ± 8.4 Mean ± SD body mass index, kg/m2 26.8 ± 5.4 26.9 ± 5.4 Smoking status, n (%) Ex-smoker 166 (54.1) 166 (53.4) Current smoker 141 (45.9) 145 (46.6) Mean ± SD smoking history, pack-years 45.0 ± 26.0 47.2 ± 23.4 Mean ± SD pre-bronchodilator FEV1 ,a L 1.53 ± 0.47 1.51 ± 0.46 Mean ± SD % of predicted FEV1 a 55.3 ± 10.2 55.4 ± 10.5 Medication use, n (%) 230 (74.9) 238 (76.5) LAMA 92 (30.0) 113 (36.3) LABA 121 (39.4) 122 (39.2) ICS 113 (36.8) 125 (40.2) a At screening. SD, standard deviation; LAMA, long-acting muscarinic antagonist; LABA, long-acting 2 -agonist; ICS, inhaled corticosteroid. Table 2. Individual components of composite end points: event rates and time to first event (25th percentile). Event, n (%) Time to first event (25th percentile), days Time to first event treatment comparison (T+O – T) T 5 µg (n=306) T+O 5/5 µg (n=310) T 5 µg (n=306) T+O 5/5 µg (n=310) HR (95% CI) p value Trough FEV1 decline from baseline 100 mLa 135 (44.1) 103 (33.3)b 91 226b 0.66 (0.51, 0.86) 0.0016 SGRQ score increase from baseline 4 unitsa 95 (32.5)c 73 (24.4)d 175c 369d 0.71 (0.52, 0.96) 0.0271 Moderate or severe exacerbation 69 (22.5) 67 (21.6) NE NE 0.94 (0.67, 1.32) NS Severe exacerbation 6 (2.0) 10 (3.2) NE NE 1.64 (0.60, 4.51) NS Death 0 (0.0) 1 (0.3) NE NE – – a Only patients with baseline and post-baseline trough FEV1 and SGRQ score values are included; b n=309; c n=292; d n=299. NE, non-estimable, NS, not significant.