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Phase 4 N=7,376 Randomized Double-blind Treatment

Tiotropium Once Daily 18 Mcg Versus Salmeterol Twice Daily 50 Mcg on Time to First Exacerbation in COPD Patients.

Pulmonary Disease, Chronic Obstructive

Bottom Line

View on ClinicalTrials.gov: NCT00563381 ↗
Enrolled (actual)
7,376
Serious AEs
15.6%
Results posted
May 2011
Primary outcome: Primary: First Occurrence of (Moderate or Severe) COPD Exacerbation — 1277; 1414 number of first occurrences — p=<0.0001

Study Design & Population

Study type
Interventional
Phase
Phase 4
Interventions
Tiotropium bromide (Drug); Salmeterol (Drug); Placebo Salmeterol (Drug); Placebo Tiotropium (Drug)
Age
Adult, Older Adult · 40+ yrs
Sex
All
Sponsor
Boehringer Ingelheim
Primary completion
Apr 2010

Outcome Measures

OutcomeResultp-value
PRIMARY
First Occurrence of (Moderate or Severe) COPD Exacerbation		 1277; 1414 <0.0001 sig
SECONDARY
COPD Exacerbations Per Patient-year Leading to Hospitalisation		 0.09; 0.13 <0.0001 sig
SECONDARY
Number of Participants With at Least One COPD Exacerbation		 1277; 1414; 2430; 2255 0.0002 sig
SECONDARY
COPD Exacerbations Per Patient-year		 0.64; 0.72 0.0017 sig
SECONDARY
First Occurrence of COPD Exacerbation Leading to Hospitalization		 262; 336 <0.0001 sig
SECONDARY
Number of Participants With at Least One COPD Exacerbation Leading to Hospitalisation		 262; 336; 3445; 3333 0.0005 sig
SECONDARY
Occurrence of Premature Discontinuation of Trial Medication		 585; 648 0.0242 sig
SECONDARY
Number of Participants With Premature Discontinuation of Trial Medication		 585; 648; 3122; 3021 0.0406 sig
SECONDARY
First Occurrence of COPD Exacerbation or Discontinuation of Trial Medication Because of Worsening of Underlying Disease, Whichever Comes First		 1316; 1448 <0.0001 sig
SECONDARY
First Occurrence of COPD Exacerbations Treated With Systemic Steroids		 715; 852 <0.0001 sig
SECONDARY
First Occurrence of COPD Exacerbations Treated With Antibiotics		 1154; 1259 <0.0001 sig
SECONDARY
First Occurrence of COPD Exacerbations Treated With Systemic Steroids and Antibiotics		 562; 671 <0.0001 sig
SECONDARY
COPD Exacerbations Treated With Systemic Steroids Per Patient-year		 0.33; 0.41 <0.0001 sig
SECONDARY
COPD Exacerbations Treated With Antibiotics Per Patient-year		 0.53; 0.59 0.0036 sig
SECONDARY
COPD Exacerbations Treated With Systemic Steroids and Antibiotics Per Patient-year		 0.23; 0.28 <0.0001 sig
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 1		 222.85; 224.45 0.1035
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 2		 225.15; 227.21 0.0369 sig
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 3		 226.31; 228.38 0.0362 sig
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 4		 227.37; 229.25 0.0573
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 5		 228.27; 229.37 0.2641
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 6		 228.80; 229.81 0.3068
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 7		 229.35; 230.13 0.4299
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 8		 229.95; 230.43 0.6277
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 9		 229.72; 230.57 0.3931
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 10		 230.30; 231.27 0.3297
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 11		 230.61; 231.91 0.1904
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 12		 231.04; 232.04 0.3172
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 13		 231.23; 231.89 0.5017
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 14		 231.19; 232.42 0.2174
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 15		 231.64; 232.75 0.2682
SECONDARY
Pre-dose Morning PEFR Measured by Patients at Home During the First Four Months of Randomised Treatment (Weekly Means Will be Calculated), Week 16		 232.06; 232.65 0.5520

Summary

This is a randomised, double-blind, double-dummy, multinational, multicentre, parallel group trial comparing tiotropium (18 mcg) inhalation capsule via HandiHaler and salmeterol (50 mcg) via MDI in patients with COPD. There will be a two-week run-in period followed by a 52-week randomised treatment phase. Patients who withdraw prematurely from trial medication will be encouraged to remain in the trial and participate in follow-up telephone contacts until their predicted normal exit date from the trial (i.e. 52 weeks after taking the first dose of randomised treatment). The phone calls will be made at all scheduled visits. The primary objective of this study is to compare the effect of tiotropium (18 mcg) inhalation capsule via HandiHaler with that of salmeterol (50 mcg) via MDI on COPD exacerbations. The primary endpoint is time to first COPD exacerbation during the 52 week randomised treatment period. A COPD exacerbation will be defined as a complex of respiratory events / symptoms (increase or new onset) of more than one of the following: cough, sputum, wheezing, dyspnoea or chest tightness with at least one symptom lasting at least three days requiring treatment with antibiotics and/or systemic steroids and/or hospitalisation. The onset of an exacerbation is defined as the onset of the first new or increased reported symptom. The end of the exacerbation should be recorded as defined by the investigator. Only COPD exacerbations with onset during randomised treatment will be included in the analysis.

Eligibility Criteria

Inclusion Criteria

  • All patients must have a diagnosis of chronic obstructive pulmonary disease (COPD) and must meet the following criteria at Visit 1:

Patients must have relatively stable, moderate to very severe airway obstruction with a post-bronchodilator FEV1 = 10 pack-years. (Patients who have never smoked cigarettes must be excluded.)

  • Patients must be able to perform all study-related procedures including technically acceptable pulmonary function tests (PFTs).
  • Patients must be able to inhale medication in a competent manner from the HandiHaler and a metered dose inhaler (MDI).
  • Patients must be able to maintain records (patient daily diary card) during the study period as required in the protocol.

Exclusion Criteria

  • Significant diseases other than COPD. A significant disease is defined as a disease or condition which, in the opinion of the investigator, may put the patient at risk because of participation in the study or may influence either the results of the study or the patients' ability to participate in the study.
  • Patients with a diagnosis of asthma.
  • Patients with a life-threatening pulmonary obstruction, or a history of cystic fibrosis.
  • Patients with known active tuberculosis.
  • Patients with a known symptomatic prostatic hyperplasia or bladder neck obstruction. Patients with symptomatically-controlled prostatic hyperplasia on medication may be included and should continue their medication.
  • Patients with known narrow-angle glaucoma.
  • Patients with a history of myocardial infarction within the year prior to Visit 1.
  • Patients with a history of hospital admission for heart failure within the year prior to Visit 1.
  • Patients with cardiac arrhythmia requiring medical or surgical treatment.
  • Patients with severe cardiovascular disorders.
  • Patients with a known hypersensitivity to anticholinergic drugs, beta-adrenergics, lactose or any other component of the medication delivery system.
  • Patients with known moderate or severe renal insufficiency (known creatinine clearance of <= 50 mL/min).
  • Patients with untreated known hypokalaemia.
  • Patients with untreated known thyrotoxicosis.
  • Patients with brittle/unstable diabetes mellitus.
  • Patients with a history of and/or active significant alcohol or drug abuse. See exclusion criterion 1.
  • Patients who have taken an investigational drug within 30 days or six half-lives (whichever is greater) prior to Screening Visit (Visit 1).
  • Use of systemic corticosteroid medication at unstable doses (i.e less than six weeks on stable dose) or at doses in excess of the equivalent of 10 mg prednisolone per day or 20 mg every other day.
  • Pregnant or nursing women or women of childbearing potential not using a medically approved means of contraception (i.e oral contraceptives, intrauterine devices, diaphragm or subdermal implants e.g Norplant) for at least three months prior to, and for the duration of the trial.
  • Previous participation (receipt of randomised treatment) in this study.
  • Patients who are currently participating in another study.
  • Patients with any respiratory infection or COPD exacerbation in the four weeks prior to the Screening Visit (Visit 1) or during the run-in period should be postponed. In the case of a respiratory infection or COPD exacerbation during the run-in period, the latter may be extended up to four weeks.
View full record on ClinicalTrials.gov →

Data sourced from ClinicalTrials.gov (NCT00563381). Outcome figures and adverse-event rates are extracted automatically from the registry's posted results and are provided for clinician reference, not as a substitute for the primary publication.

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