Copd Clinical Trial
Official title:
Effect of Sublingual Fentanyl on Breathlessness in COPD : A Randomized Cross-over Trial
There is actually no physiologic or clinical data in the literature to clearly define the potential benefits and side effects of sublingual fentanyl in patients with COPD. Therefore, the purpose of this study is to test the hypothesis that sublingual fentanyl will improve exercise capacity and dyspnea control in severe COPD patients experiencing persistent breathlessness despite optimal management.
The purpose of this study is to test the hypothesis that sublingual fentanyl will improve
exercise capacity and dyspnea control in severe COPD patients experiencing persistent
breathlessness despite optimal management.
To demonstrate the effectiveness of sublingual fentanyl, the investigators suggest a dose of
12,5 mcg. The investigators base this decision on several considerations :
- Local practice and experience : the safety of a dose of 12,5 mcg of sublingual fentanyl
has been show in the investigators local experience (see section 1.3 Clinical experience
with fentanyl).
- Although there is not enough information to determine the exact equivalence between
sublingual fentanyl and oral morphine, the conversion between intravenous fentanyl and
oral morphine can be done. Based on the monograph of fentanyl citrate, 10 mcg of
intravenous fentanyl citrate are equivalent to 10 mg of intravenous morphine, which are
equivalent to 20 to 30 mg of oral morphine. Subsequently, 12,5 mcg of sublingual
fentanyl may be equivalent to a oral morphine dose between 2,5 and 3,75 milligrams. This
represent a smaller dose than the dose of 0,1 mg/kg oral morphine that was demonstrated
to be safe in a recent study done by a group at McGill in a severe COPD population
(Abdallah et al. Eur Respir J 2017; 50: 1701235).
- The study will only include patients who are already on morphine, because they represent
the target population and have less risk of adverse events than an opioid-naive
population.
- To ensure safety, participants will be actively monitored during the study. A doctor
will be present at administration of the drug and the antidote, naloxone, will be
readily available if needed. Participants will be monitored on-site for 30 minutes after
completion of CPET and discharge only if no evidence of side effects. Participants will
be informed to not drive for 24 hours following each period of treatment. A phone call
follow-up will be done 24-48 hours after treatment visits.
General Objective:
The general objective is to demonstrate the role of sublingual fentanyl liquid to improve
exertional shortness of breath in patients with severe to very severe COPD.
Primary Objective :
The primary objective is to evaluate in severe/very-severe COPD the effect of 12,5 mcg
fentanyl sublingual liquid as compared with placebo, on i) post-dose difference in exertional
breathlessness at isotime (Isotime definition : highest equivalent 2 min interval of exercise
completed by a given participant) ii) Post-dose difference in exercise endurance time (EET)
The study is a single centre randomized clinical trial, double-blinded, cross-over design,
comparing fentanyl sublingual at a dose 12,5 mcg to placebo in severe/very-severe COPD
already taking low dose of morphine because of refractory dyspnea.
To detect a minimally clinically important (MCID) difference of 1 Borg unit (40) at iso-time
between treatments, we assume an α of 0.05 and a within-subject standard deviation of 1 Borg
unit: a total of 20 patients will provide >80% power; assuming an attrition rate of 20%, a
total of 24 patients will be recruited for this study.
All data will be de-nominalized in order to respect privacy. Data will be collected in an
anonymous data sheet, protected by a password. Only investigators and statistician will have
access to this data sheet.
The principal analysis of the relative change in dyspnea intensity at iso-time (primary
end-point) after treatment with morphine sulfate vs. placebo will be conducted using an
unadjusted paired t-test. Secondary analyses to assess treatment responses on secondary
end-points (e.g. arterialized capillary PCO2, EET, dyspnea unpleasantness, ventilation,
breathing pattern, operating lung volumes, etc.) will be done using paired t-tests adjusted
(Bonferroni) for multiple comparisons. Pearson correlations will be used to establish
associations between intra-subject post-dose differences in iso-time dyspnea intensity
ratings and relevant independent variables (e.g. arterialized capillary PCO2, ventilation,
breathing pattern, MDP results, etc.) and various baseline patient characteristics (possible
covariates). Stepwise multiple regression analysis will then be carried out with significant
independent variables and relevant covariates.
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