Dyspnea Clinical Trial
Official title:
Phase II Pilot Pragmatic Single-Blinded Fast Track Randomised Controlled Trial of the Breathlessness Intervention Service Versus Standard Care for Patients With Chronic Obstructive Pulmonary Disease
The aim of this study is to test the feasibility of conducting a pragmatic fast track Randomized Controlled Trial (RCT) of the Breathlessness Intervention Service (BIS) versus standard care for patients with COPD and their carers, and to begin testing the effectiveness of the intervention.
The aim of the study is to test the feasibility of conducting a pragmatic single-blinded
fast track RCT of BIS versus standard care for patients with COPD and their carers and to
begin testing the effectiveness of the intervention by: (1) Describing the referral patterns
and activity of the service; (2) Describing the experiences and views of the service by
people with breathlessness who have been referred to it and the experiences and views of
those informally involved in their care; (3) Identifying those aspects of the service which
are most useful to people with breathlessness, those informally involved in their care and
health care professionals.
The study consists of five components: (1) data relating to referral patterns and service
activity; (2) identification of components of the intervention; (3) a pilot pragmatic
fast-track randomised controlled trial (RCT) of BIS for COPD patients versus standard care;
(4) semi-structured interviews with referrers; (5) in-depth interviews with BIS staff. The
RCT is described below.
Although the BIS also receives referrals for patients with cancer and heart failure, COPD
patients make up the largest diagnostic group of referrals. The pilot trial therefore
focuses on a heterogeneous cohort of COPD/COAD patients.
The investigator will be blinded to the allocation of respondents until week 8. This will be
achieved by the investigator conducting the recruitment to the study and collecting baseline
measures, but then passing the process of randomisation and reporting of allocation (to the
patient and provider) over to a third party (clinical trials' nurses) using a random
sequence of opaque envelopes previously generated by a study administrator at King's
(independent of the service and the RCT). Subsequent to this, all data will be handled using
study identity numbers and group allocation identifiers will only be added at the analysis
stage. Outcomes are all self-assessed by patients and carers principally using structured
questionnaires but also incorporating a qualitative topic guide prior to randomisation and
then again at the end of the fast track group's exposure to BIS and the control group's
waiting period for BIS (at both of these measurement points structured questionnaires will
be completed prior to the qualitative interview).
Subsequent data collected from the control group once they are in receipt of BIS (after
their period on the waiting list when their group allocation was blinded to the
investigator) will be treated as before/after data and not RCT data. This will allow the
collection of qualitative data at the midpoint of using the service as the investigator will
no longer be blinded to their group allocation, nor will she be required to be at this
stage.
Measurement points: 'measures' (quantitative and qualitative) will be taken for all
respondents (FT and CC) at baseline (t1), prior to randomisation. They will be repeated for
the fast-track group (FC) during the intervention (4 weeks post commencement of the
intervention (FTt2) - quantitative only) and for control condition group at the same time
(CCt2 - quantitative only), and then again after discharge for the fast track group (8 weeks
post commencement of intervention (FTt3)). As well as being measured at t1 (randomisation)
and t2 (mid-point between randomisation and intervention - quantitative only), the control
condition group (CC) will also be measured just prior to the commencement of their
intervention (CCt3), repeated during the intervention (4 weeks post commencement of the
intervention (CCt4)) and then again after discharge (8 weeks post commencement of
intervention (CCt5)). Using this measurement strategy should make it possible to identify
whether or not the condition of respondents in the control group deteriorated whilst they
awaited their intervention and whether or not this then had an impact on final outcomes for
this group.
Measures will be collected by means of audio-taped structured/semi-structured interviews
(with respondents' permission). It is proposed that at each measurement point patients and
carers are interviewed separately as this found to be important in the pilot study
interviews. This will be managed by means of requesting that carers complete any
self-complete measures whilst the interview is being conducted with the patient. Interviews
with carers will then be conducted on a separate, but temporally close, occasion (e.g. up to
2 days later), at the carer's convenience (e.g. in the evening if required). Careful
attention will be paid to the needs of the patient and carer in terms of fatigue.
Determining the sample size for a pilot/exploratory trial of this type is difficult. As no
trials have been conducted before with this particular intervention, or for this type of
intervention with this patient group (i.e. COPD patients), there is a lack of data (e.g.
identification of primary outcome measures and their data) to support the power calculations
usually used to estimate the required sample size of a definitive RCT (i.e. the number of
participants needed to ensure the study is scientifically sound). In addition, those trials
that do exist relating to interventions for patients with COPD (e.g. trials of pulmonary
rehabilitation rather than breathlessness intervention services) have focused primarily on
physiological outcomes such as clinical measures of breathlessness. However, as a result of
our earlier work at the Pre-Clinical phase and Phase I, we became aware of the need to look
beyond such physiological measures and consider other outcomes (e.g. distress due to
breathlessness, ability to choose to participate in social events).
Thus the pilot/exploratory trial (Phase II) will itself provide vital information to inform
the power calculations for a future planned definitive RCT (Phase III). The aims of this
current pilot/exploratory trial therefore include testing the intervention (the BIS) but
also establishing the feasibility of conducting a definitive RCT by testing the trial method
(i.e. the pragmatic fast-track design), randomisation procedures and the identification of
appropriate primary outcome measures. It is envisaged that the most likely primary patient
outcomes will be 'distress due to breathlessness' and mastery of breathlessness; the most
likely primary carer outcome is 'carer distress due to breathlessness'. For both patients
and carers 'distress due to breathlessness' will be measured using a Visual Analogue Scale
(VAS; 0-10cm); a difference between the baseline and follow up measurements of 1cm on this
scale could be regarded as clinically significant for patients with intractable
breathlessness. This pilot/exploratory RCT will provide the data to confirm or refute these
outcomes, and so enhance the design of future definitive trials.
Based on clinical experience, data published from other studies and case reports (e.g.
Corner et al, 1996), and on expert advice, we have made some tentative estimates of the
likely changes we may expect the intervention to have. We could expect a change in score of
severe distress due to breathlessness of 2.2 (SD 1.8) on a 10 point scale. This difference
would be detected, using a Mann Whitney U test, with 11 patients in each group (22 in
total), with 80% power and a significance of p=0.05. A change in the proportion of patients
with severe or very severe distress due to breathlessness from 90% to 40% would be detected
at 80% power and a significance of p<0.05 by 14 patients in each group (28 patients in
total). Therefore we will aim to recruit at least 30 (or 28) patients to the trial.
A number of subjective measures, exercise tolerance measures and physiological measures are
already collected or recorded by the BIS itself (e.g. VAS, modified BORG, MRC grading of
dyspnoea symptoms etc.). These will continue to be collected and will be utilised by both
the service and the evaluation. In accordance with the aims of the evaluation, other
outcomes to be assessed within the trial will relate to patient and carer satisfaction with
the service, patient and carer quality of life, patient and carer anxiety, patient mastery,
caregiver burden, patients' breathlessness, patient and carer distress due to
breathlessness, aspects of the service most useful to users (patients and carers) and other
service use.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Investigator), Primary Purpose: Supportive Care
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