Research ArticleResearch Letter

Megatrials for Bronchodilators in Chronic Obstructive Pulmonary Disease (COPD) Treatment: Time to Reflect

Wouter D. van Dijk, Lisette van den Bemt and Chris van Weel
The Journal of the American Board of Family Medicine March 2013, 26 (2) 221-224; DOI: https://doi.org/10.3122/jabfm.2013.02.110342

Abstract

Introduction: Chronic obstructive pulmonary disease (COPD) is an important cause of morbidity and mortality worldwide. Although (long-acting) bronchodilators are used to relieve symptoms, the impact of bronchodilators on COPD mortality remains an unresolved issue. Our aim was to explore the results and the interpretations of the results of studies of bronchodilator treatment from high-impact COPD trials.

Methods: We searched PubMed and Embase for primary publications of randomized controlled trials with more than 1000 participants with COPD and that studied the effectiveness of long-acting bronchodilator treatment. We assessed population characteristics, primary outcomes, focus of outcomes, and possible bias from concomitant pulmonary medication.

Results: We retrieved 5 primary publications of large trials. Participants tended to be patients with rather severe COPD who were cared for at a hospital. Only half of the primary outcomes were statistically significant. Reports tended to focus on statically significant outcomes and not necessarily on primary outcomes or outcomes of the whole study population. The relevance of study outcomes was rarely discussed.

Discussion: The rather small effects of bronchodilators in a COPD population that is not representative for daily care, together with the tendency of relying on statistical rather than clinical significance, hampers translation to the large number of patients with COPD in the community.

Chronic obstructive pulmonary disease (COPD) is a progressive chronic disease characterized by not fully reversible airflow obstruction. It is one of the most important causes of morbidity and mortality worldwide, directly related to cigarette smoking. Indeed, cessation of cigarette smoking is the single-most efficient intervention to prevent both disease development and progression.1,2 In addition, (long-acting) bronchodilators are used to relieve symptoms. An unresolved question is the impact of bronchodilators on COPD mortality, in part by attenuation of pulmonary function decline and exacerbations, independent from desired symptom relief. The last decade, a number of large studies on the effectiveness of long-acting bronchodilators received extensive attention in leading medical journals. Calverley observed that “ensuring that these expensive studies are done objectively to the highest standard is an important goal”.3 For that reason, the quality of these large trials, their external validity, and what they add to the current clinical practice, are of importance. We systematically reviewed the results and the interpretations of these results of megatrials on long-acting bronchodilators in COPD patients that were published in high impact journals.

Methods

WD and LB conducted a search in both PubMed and Embase until 2011, July 31st, containing (Mesh) terms of COPD and bronchodilators. We included primary publications in leading journals with an impact factor >15 in 2011 of randomized controlled trials with more than 1000 participants with COPD, that studied the effectiveness of long-acting bronchodilator treatment. WD and LB independently and systematically assessed population characteristics, primary outcomes, focus of outcomes, and possible bias from concomitant pulmonary medication.

Results

We retrieved five primary publications of large trials on bronchodilator effect in COPD patients, including 1465 to 7376 patients with a mean follow-up between 6 and 48 months (Table 1).48 Mean COPD severity as measured by percentage of predicted forced expiratory volumes ranged from 36% to 49% at baseline. The mean proportion of males was 77%. All studies included patients with at least 10 pack-years smoking history only, and patients with co-prevalence of asthma were excluded. Certain types of pulmonary co-medication were allowed during all studies, but none of the analyses were adjusted for these co-medications during follow-up. Table 1 also summarizes the various effects of bronchodilators on primary outcomes. Primary outcomes were mortality,6 exacerbations5,8 and lung function decline.4,7 Although all studies report positive outcomes for the study medication of interest in general, only three of six primary outcomes of the studies were statistically significant.4,5,8 Clinical significance was discussed in two trials only.4,5 The statistically significant primary outcomes include pre-bronchodilator FEV1 change (post-bronchodilator FEV1 was not statistically significant in this study),4 percentage of patients with exacerbations (the other primary outcome: number of hospitalizations for exacerbations, did not statistically differ significantly between groups),5 and time to exacerbations (a statistically significant modified population of analyses).8 Studies focused on statistically significant secondary outcomes,4,7 and statistically significant subgroup analyses.7 Although two studies acknowledged statistically non-significant results for the primary outcome they focused on its beneficial effect,6,7 and on the secondary outcome.6 One study did not always correctly stated the population key characteristics,8 whereas another used pre-bronchodilator values as primary outcome.4

View this table:
Table 1. Large Bronchodilator Trials According to Factors For Interpreting Good Clinical Practice on Design, Results, and Translation

Discussion

Despite the positive tone in the reports of large trials on long-acting bronchodilator therapy in COPD patients, only half of the primary outcomes were statistically significant. Next, reports tend to focus on statically significant outcomes and not necessarily on primary outcomes or outcomes of the whole study population.

Compared with combining results of smaller rigorous trials into meta-analyses, megatrials could provide a small advantage on minimizing confounding by change.9 However, since large trials increase their participant numbers by reducing protocol rigidness, bias can be introduced that weakens causative interpretations.10 For instance, in these COPD megatrials, various co-medications were allowed during the study without proper adjustments for it in the analyses. On the other hand, decreased rigidness may provide a generalization of results in daily practice, but only if the study population is representative of the target population to which its results will be applied.9 Moreover, the clinical relevance of the rather small effects in a possibly biased COPD population that is not representative for daily care should be debated, in particular as meta-analyses rate these trials on their patient numbers mostly.

Most patients with COPD are treated in the community, while the selection of patients for large trials is biased toward referred, hospital cared patients. This, together with the tendency of relying on statistical rather than clinical significance, hampers translation to the large number of patients with COPD in the community. Independent from symptom relief, we would therefore plea for some precaution on the customary prescription of long-acting bronchodilators for the COPD population at large.

Notes

  • This article was externally peer reviewed.

  • Funding: none.

  • Conflict of interest: none declared.

  • Received for publication December 23, 2011.
  • Revision received March 23, 2012.
  • Accepted for publication March 26, 2012.

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