REgistry-based randomized controlled trial of treatment and Duration and mortality in long-term OXygen therapy (REDOX) study protocol

Long-Term Oxygen Therapy (LTOT) is an established treatment to improve survival in patients with chronic daytime hypoxemia due to chronic obstructive pulmonary disease (COPD) [1]. Internationally accepted guidelines recommending that LTOT should be given for 15 h/day or more [2] are based on two small randomized controlled trials (RCTs) conducted in the 1970s with a total of 290 patients; the ‘Continuous or Nocturnal Oxygen Therapy’ trial (NOTT) published in 1980 [3] and the ‘Medical Research Council’ (MRC) study published in 1981 [4]. In NOTT, prescribed oxygen duration 24 h/day (mean use 18 h/day) increased survival compared with 12 h/day, and in the MRC study oxygen 15 h/day increased survival compared with no oxygen. The internationally accepted recommendation to use LTOT at least 15 h/day and preferably 24 h/day is based on an unadjusted observational comparison of the treatment arms of these two trials, where the crude mortality rate was lower for the 18 h/day group in NOTT than for the 15 h/day group in the MRC trial [5] (21% vs 41%). However, the presumed survival benefit of continuous LTOT over 15 h /day has not been proven in a randomized controlled trial. Our recently performed observational study of 2249 patients using LTOT for hypoxemic COPD suggested that there may indeed be no differences in survival for LTOT 24 h/day compared with 15 h/day [6]. As for LTOT to patients with mild hypoxemia at rest or with isolated hypoxemia during exertion, the recent ‘Long Term Oxygen Therapy’ (LOTT) trial showed no reduced mortality [7], and a Cochrane metaanalysis reported some effect on breathlessness but not on health related quality of life (HRQoL) [8].

LTOT is associated with considerable logistic challenges, costs and side effects [9, 10]. Being connected to oxygen equipment is associated with feelings of shame, restrictions of daily activities, and social isolation [11, 12]. Thus, continuous LTOT may pose an unnecessary burden and limitation for many patients compared with treatment 15 h/day, where they can be free of their oxygen for 9 h/day. The longer the duration of daily therapy, the less likelihood of adherence to treatment. Low-flow oxygen therapy has been associated with oxidative stress and inflammation [13], which could potentially contribute to increased morbidity and negative health effects [14, 15]. Moreover, the validity of the NOTT and MRC trials for current practice is questionable as the studies included mainly men and people younger than 70 years without significant comorbidity. Of note, treatment for COPD and cardiovascular disease has also improved in recent decades [5, 9]. The results of the NOTT and MRC trials are also generally applied for all conditions with secondary hypoxemic respiratory failure, although intervention studies of LTOT in pulmonary fibrosis, heart failure and pulmonary hypertension are lacking. Thus, improved evidence-based LTOT is needed.

The Registry-based randomized controlled trial (R-RCT) is a recent scientific paradigm shift that can facilitate large interventional trials with adequate power and low cost [16] to detect clinically important patient outcomes pragmatically in the real world setting [17]. The trial design was pioneered by Swedish cardiologists in the TASTE study of thrombus aspiration using the Swedish Coronary Angiography and Angioplasty Registry, which enabled inclusion of a large nationally representative sample, and the study was highly cost-effective [16].

This paper presents the protocol for a Swedish national multisite R-RCT; REgistry based randomized controlled trial of treatment Duration and mortality in long-term OXygen therapy (REDOX), to test the primary research hypothesis that LTOT 24 h/day does not reduce all-cause mortality compared with LTOT 15 h/day in patients with oxygen-dependent COPD. Secondary outcomes include cause-specific mortality, hospitalizations, health-related quality of life, symptoms, effects in other underlying diseases, and effects by the level of hypoxemia at baseline.

This is the first study to compare effectiveness of LTOT duration of 24 and 15 h/day on clinical outcomes in people with chronic respiratory failure, with a potential direct impact on research and clinical management. LTOT is used commonly as it is one of few interventions that can affect prognosis in COPD, but there has been no trial of LTOT in severe hypoxemia since the 1970s [3, 4]. Research in LTOT has been held back by problems and high cost of recruitment and follow-up of patients with advanced disease, and challenges with ethical justification to withhold oxygen 24 h/day in patients with severe hypoxemia for the purpose of conducting a clinical trial even though there is no clear evidence of difference in outcomes between shorter and longer duration LTOT. This study will be by far the largest study in LTOT to date, and the first R-RCT in respiratory medicine. The R-RCT design is a paradigm shift and enables a large-scale, randomized trial in a representative sample of people with very advanced disease, with complete follow-up of main endpoints. This will be the first trial investigating whether LTOT 24 h/day improves important patient outcomes − survival time, risk of hospitalization, levels of symptoms, oxygen side effects, and HrQoL compared with LTOT 15 h/day, or whether LTOT 24 h/day might unnecessarily constraint and burden patients. This study will also for the first time evaluate effects of LTOT by the degree of hypoxaemia and in people with disease other than COPD. Further, evaluating the effect on the risk of hospitalization is crucial as hospitalization is a major driver of health care costs [34]. If COPD hospitalizations can be reduced by LTOT 24 h/day compared with 15 h/day, increased use of long term oxygen treatment could be cost-effective, which will be evaluated in a comprehensive health economic analysis. The trial will also examine the effect of LTOT prescribed 24 h/day compared with 15 h/day on survival and other outcomes, several of which were not assessed in the LOTT trial of patients with moderate hypoxemia [7]. The study will investigate effectiveness of the prescription of LTOT in clinical care. No objective measurement of oxygen use will be used, as there is no accepted, user-friendly objective means of collecting usage data. However self-reported actual oxygen duration will be collected.

If LTOT 24 h/day is found to be non-superior to 15 h/day, this will confirm that patients safely can be free of supplemental oxygen for up to nine hours per day. If not, LTOT 24 h/day may be superior which implies the importance of oxygen therapy in chronic respiratory failure and the relevance of implementing services to facilitate and optimize the daily duration of LTOT. The trial design will provide robust, detailed data using validated instruments that enable correlational analyses of factors influencing the adherence to and net clinical effectiveness of LTOT in patients with respiratory failure in current clinical practice. The study also aims to take forward an infrastructure for randomized trials that can be used to facilitate research and improved evidence-based treatment in patients with chronic respiratory failure.