Physical Fitness Training in Patients with Subacute Stroke (PHYS-STROKE): multicentre, randomised controlled, endpoint blinded trial
BMJ 2019; 366 doi: https://doi.org/10.1136/bmj.l5101 (Published 18 September 2019) Cite this as: BMJ 2019;366:l5101Linked Opinion
Null but not void—the effectiveness of aerobic exercise following subacute stroke
- Alexander H Nave, neurological research fellow1 2 3 4,
- Torsten Rackoll, research scholar1 5,
- Ulrike Grittner, biostatistician4 6,
- Holger Bläsing, neurologist7,
- Anna Gorsler, neurologist5,
- Darius G Nabavi, professor of neurology8,
- Heinrich J Audebert, professor of neurology1 2,
- Fabian Klostermann, professor of neurology2,
- Ursula Müller-Werdan, professor of geriatrics9,
- Elisabeth Steinhagen-Thiessen, professor of geriatrics9,
- Andreas Meisel, professor of neurology1 2 10,
- Matthias Endres, professor of neurology1 2 3 4 10 11,
- Stefan Hesse, professor of neurology12,
- Martin Ebinger, professor of neurology1 12,
- Agnes Flöel, professor of neurology1 13 14
- 1Centre for Stroke Research Berlin, Charité–Universitätsmedizin Berlin, Berlin, Germany
- 2Klinik und Hochschulambulanz für Neurologie, Charité–Universitätsmedizin Berlin, Berlin, Germany
- 3German Center for Cardiovascular Research, partner site Berlin, Germany
- 4Berlin Institute of Health, Berlin, Germany
- 5Kliniken Beelitz, Beelitz-Heilstätten, Germany
- 6Institute of Biometry and Clinical Epidemiology, Charité–Universitätsmedizin Berlin, Berlin, Germany
- 7Median Klinik Grünheide, Grünheide, Germany
- 8Vivantes Klinikum Neukölln, Klinik für Neurologie, Berlin, Germany
- 9Evangelisches Geriatriezentrum Berlin, Berlin, Germany
- 10NeuroCure Clinical Research Center, Charité–Universitätsmedizin Berlin, Berlin, Germany
- 11German Center for Neurodegenerative Diseases, partner site Berlin, Germany
- 12Medical Park Berlin Humboldtmühle, Berlin, Germany
- 13Department of Neurology, University Medicine Greifswald, Ferdinand-Sauerbruch-Strasse, 17475 Greifswald, Germany
- 14German Center for Neurodegenerative Diseases, partner site Rostock/Greifswald, Germany
- Correspondence to: A Flöel agnes.floeel{at}med.uni-greifswald.de
- Accepted 23 July 2019
Abstract
Objective To determine the safety and efficacy of aerobic exercise on activities of daily living in the subacute phase after stroke.
Design Multicentre, randomised controlled, endpoint blinded trial.
Setting Seven inpatient rehabilitation sites in Germany (2013-17).
Participants 200 adults with subacute stroke (days 5-45 after stroke) with a median National Institutes of Health stroke scale (NIHSS, range 0-42 points, higher values indicating more severe strokes) score of 8 (interquartile range 5-12) were randomly assigned (1:1) to aerobic physical fitness training (n=105) or relaxation sessions (n=95, control group) in addition to standard care.
Intervention Participants received either aerobic, bodyweight supported, treadmill based physical fitness training or relaxation sessions, each for 25 minutes, five times weekly for four weeks, in addition to standard rehabilitation therapy. Investigators and endpoint assessors were masked to treatment assignment.
Main outcome measures The primary outcomes were change in maximal walking speed (m/s) in the 10 m walking test and change in Barthel index scores (range 0-100 points, higher scores indicating less disability) three months after stroke compared with baseline. Safety outcomes were recurrent cardiovascular events, including stroke, hospital readmissions, and death within three months after stroke. Efficacy was tested with analysis of covariance for each primary outcome in the full analysis set. Multiple imputation was used to account for missing values.
Results Compared with relaxation, aerobic physical fitness training did not result in a significantly higher mean change in maximal walking speed (adjusted treatment effect 0.1 m/s (95% confidence interval 0.0 to 0.2 m/s), P=0.23) or mean change in Barthel index score (0 (−5 to 5), P=0.99) at three months after stroke. A higher rate of serious adverse events was observed in the aerobic group compared with relaxation group (incidence rate ratio 1.81, 95% confidence interval 0.97 to 3.36).
Conclusions Among moderately to severely affected adults with subacute stroke, aerobic bodyweight supported, treadmill based physical fitness training was not superior to relaxation sessions for maximal walking speed and Barthel index score but did suggest higher rates of adverse events. These results do not appear to support the use of aerobic bodyweight supported fitness training in people with subacute stroke to improve activities of daily living or maximal walking speed and should be considered in future guidelines.
Trial registration ClinicalTrials.gov NCT01953549.
Introduction
Despite encouraging advances in the early treatment of stroke,1 at least one third of the 10 million people worldwide with new stroke each year2 remain functionally dependent and as a result experience impairments in activities of daily living.34 The number of stroke survivors with impairments in activities of daily living is increasing, leading to more people with stroke who are dependent on rehabilitation interventions.5 To date, no drug treatments are available to enhance rehabilitation. Treadmill based physical fitness training constitutes a non-drug approach in stroke rehabilitation that might not only prevent deconditioning but also show associated benefits on activities of daily living, such as walking and climbing stairs.678
A meta-analysis of small randomised controlled trials showed improvements in speed and tolerance of walking after physical fitness training in stroke survivors.6 The studies have, however, varied in type and intensity of exercise, timing of initiation after stroke, and control groups.791011 The American Heart Association/American Stroke Association currently recommends aerobic exercise for stroke survivors, with three to five sessions weekly lasting 20 to 60 minutes and at a heart rate of 55-80% of the maximum. Applied in the subacute stage after stroke, aerobic exercise is thought to promote neuroplasticity and to have beneficial effects on functional outcomes.7 So far, nine randomised controlled trials (n=324) have compared the effects of aerobic physical fitness training on maximal walking speed—an important indicator of mobility in everyday life6—with a control intervention. However, only two of these studies (n=73) enrolled participants within the first six weeks after stroke, and these participants showed improvement in maximal walking speed post-intervention.6 For activities of daily living and disability, two small randomised rehabilitation trials (n=199) that applied 400-540 minutes of physical fitness training in the early and late subacute stage after stroke found an increase in the Barthel index score, a disability scale widely used in the clinical setting to measure activities of daily living.1213 Meta-analyses have, however, indicated that the evidence for improvement in Barthel index scores after physical fitness training is still inconclusive.6
Previously, the larger Locomotor Experience Applied Post-Stroke (LEAPS) trial randomised 408 participants to treadmill based locomotor training either two or six months after stroke, or to a progressive exercise programme at home, and did not detect a difference in treatment effects.11 LEAPS did not, however, apply an aerobic physical fitness training early after stroke.
We performed a multicentre, randomised controlled trial in adults with stroke in the early subacute phase (days 5-45 after stroke) to determine the efficacy of aerobic treadmill based, physical fitness training on maximal walking speed and activities of daily living compared with relaxation as a control intervention.
Methods
Study design
The study protocol for the multicentre, randomised controlled, endpoint blinded Physical Fitness Training in Patients with Subacute Stroke (PHYS-STROKE) trial is available online (https://doi.org/10.1186/1745-6215-15-45) and has been published previously.14 All participants provided informed consent. Adults were enrolled at seven inpatient rehabilitation sites in Berlin, Germany, and the surrounding area. A medical monitoring and independent data safety and monitoring board was appointed by the Centre for Stroke Research Berlin. Guidance of study centre representatives was maintained by regular telephone contact and study visits by members of the coordinating trial centre at the Centre for Stroke Research Berlin. To determine eligibility for the trial, trained trial physicians screened people with an imaging confirmed diagnosis of ischaemic or haemorrhagic stroke who had been admitted to hospital within a recruiting centre.
Participants
People were eligible for the trial if they were aged at least 18 years, were in the subacute phase of ischaemic or haemorrhagic stroke (days 5-45 after stroke onset), were able to sit unsupported for at least 30 seconds, were considered able to perform aerobic exercise by the responsible trial physician, and had a Barthel index score of 65 or less at the time of enrolment. The Barthel index measures activities of daily living based on 10 items, with scores ranging from 0 to 100 points—higher scores indicating less dependence.15 Key exclusion criteria were intracranial haemorrhage from a ruptured aneurysm or arteriovenous malformation, inability to perform required physical exercise, assisted walking before stroke, or severe cardiac or psychiatric comorbidities. If study requirements were met, trial physicians assessed information on stroke type and medical conditions after written informed consent was obtained. The supplementary file lists the inclusion and exclusion criteria.
Randomisation and blinding
Participants were stratified by age (≤65 years, >65 years), functional ambulation category (scores ≤3, >3), and centre and were randomised using a web based tool in a 1:1 ratio to receive aerobic physical fitness training or relaxation sessions (control group) in addition to standard care.16 The functional ambulation category is a six point scale that assesses dependency on walking aids, with higher scores indicating less dependency. Trained study assessors (physiotherapists, occupational therapists) collected information on participant characteristics and clinical data from chart reviews at baseline visits and carried out outcome assessments at baseline and follow-up. Study assessors and the trial statistician were blinded to the intervention allocation.
Interventions
Therapists at each rehabilitation site performed interventions according to standardised protocols taught by a manual and two day training course. The study interventions were applied during inpatient stay at the rehabilitation centre, in addition to standard rehabilitation therapy according to German guidelines (www.bar-frankfurt.de). The supplementary file provides detailed information on the amount and content of standard care. Each study session was for 50 minutes (therapist led), comprising 25 minutes of core intervention (training aimed at target heart rate or relaxation time), and took place five times weekly over four weeks (20 sessions in total). The start and end of each intervention session as well as the duration of the core intervention were documented for each participant. An intervention period of four weeks was chosen to ensure intervention sessions were applied during the length of the inpatient stay at the rehabilitation centres. This also enabled the assessment of short term outcomes at three months after stroke.
The supplementary appendix provides a detailed description of the aerobic physical fitness training and relaxation interventions. Briefly, the aerobic physical fitness training sessions included treadmill based, bodyweight supported training at a cardiorespiratory active (aerobic) level to reach a target heart rate for 25 minutes. The target heart rate was calculated by the formula 180 minus years of age, a pragmatic decision, which resembles conventional approaches for calculation of target heart rate that is 50-60% of each participant’s maximum heart rate (see supplementary appendix). If participants used β blockers, we reduced the target heart rate by 10 beats per minute. Participants used a bodyweight supported treadmill (Multi-disk treadmill Callis, Model Therapie; Sprintex Trainingsgeräte, Kleines Wiesental, Germany; Reha-Stim, Berlin, Germany) if their functional ambulation category score was 3-5 or an electromechanical gait trainer (Gait Trainer GT1; Reha-Stim, Berlin, Germany) if their score was 0-2. The amount of bodyweight support was applied as required. If necessary, one or two therapists assisted with leg movement, such as extending hip and knee, shifting body weight, or setting the paretic leg in the case of severe paresis of the peroneus muscles. Participants used the same orthoses during the intervention as during standard care physiotherapy. Each training session, including preparation time and a warm-up and cool-down phase, lasted 50 minutes and comprised 25 minutes of active training at aimed target heart rate, depending on each participant’s ability, as recommended in current guidelines.7 To ensure target heart rate was maintained, heart rate during training was controlled through a pulse sensor (Polar FT1 HRM, Polar Electro Oy, Kempele, Finland) and a screen attached to the treadmill or gait trainer. Reduction of bodyweight support and an increase of belt speed or increase of inclination, or both was used to reach the target heart rate throughout the four week intervention, and thus to constantly induce aerobic training effects. The trainers documented changes of these variables during the intervention period and individual perceived exertion after each training session in intervention diaries. To prevent falls, participants were equipped with a modified parachute harness (Belt system; Reha-Stim, Berlin, Germany).
Relaxation sessions were performed as an active control and focused on contraction and relaxation of muscle groups in the face, arms, shoulders, back, and abdomen for 25 minutes. Participants were instructed to contract the muscles for five to 10 seconds then to relax for 30-40 seconds and were encouraged to pay attention to the feelings of warmth and heaviness. Sessions aimed to promote mental and physical relaxation and avoid any cardiovascular stress. Participants’ heart rates were monitored during the relaxation sessions, and ratings of perceived exertion were assessed at the end of each session. Participants in both groups received individual attention during each session to achieve comparability.
No specific treatment policy was prescribed after the intervention period. If participants stopped the intervention prematurely, we continued clinical follow-up at set time points. Participants were analysed in the per protocol analysis if they received 75% or more of the scheduled intervention sessions, had not suspended the intervention for more than five consecutive days, and had participated in the follow-up visit three months after stroke.
Outcome measures
Study visits for outcome assessment were performed before and after the intervention period as well as three and six months after stroke. The primary outcome measures were change in maximal walking speed (assessed in m/s) and change in Barthel index scores three months after stroke compared with baseline in the intention-to-treat analysis. Maximal walking speed was assessed in a 10 m walk test.17 Participants were asked to walk at maximal speed for 14 m—2 m for acceleration and 2 m for deceleration, with markings on the floor for starting point, at 2 m (start of measurement) and 12 m (end of measurement). The time taken for the walk was measured manually using an electronic time watch for all participants and was additionally controlled with a light beam to trigger an additional watch (Wilhelm Köster Ingenieur für Zeitmessung, Ditzingen, Germany). The test was performed twice and mean speed calculated to avoid test-retest error. Prespecified secondary outcomes included the six minute walk test (in metres), Rivermead mobility index18 (range 0-15, with higher scores indicating better mobility), actigraphy for 24 hours (in steps daily, assessed with GT3x; Actigraph, Pensacola, FL), modified Rankin scale (mRS) score (a scale assessing disability after stroke; ranging from 0 for no symptoms to 6 for death), as well as measures of cognition, motor function, spasticity, mood, and sleep at follow-up compared with baseline. Additionally, in a per protocol dataset we analysed changes in maximal walking speed and Barthel index score three months after stroke compared with baseline. Prespecified biomarker and imaging outcome measures will be analysed separately within an accompanying study,19 as described in the statistical analysis plan. The supplementary appendix describes the assessments of secondary outcomes. Main prespecified subgroup analyses included dichotomisation of impairment scores (National Institutes of Health stroke scale (NIHSS)20 assessed on days 3-5 after stroke, a scale that measures neurological deficits, ranging from 0 to 42 points, with higher values indicating more severe strokes, and functional ambulation category), type of stroke, time of study inclusion, and age and sex of participants. We carried out additional post hoc exploratory analyses of differential treatment effects for continuous variables using splines.21
Primary safety outcomes included the serious adverse events of recurrent cardiovascular events, including stroke, admission to an acute care hospital, or death within three months after stroke. Trial physicians reported these outcomes to the coordinating trial centre within 24 hours. The adverse events of self reported pain, fatigue, dizziness, and number and nature of falls during the intervention period were recorded after each intervention session. We reported adverse events to the data safety monitoring board on a regular basis.
Statistical analysis
To show the superiority of the aerobic physical fitness training over relaxation intervention, the study was powered on the primary outcome measures to detect a clinically meaningful difference of 0.13 m/s in maximal walking speed (common standard deviation of 0.25 m/s) or 10 points in Barthel index score (common standard deviation of 21 points).14 Assumptions were based on reported clinical differences from a previous study of another working group (n=155).13 Overall, 172 participants (86 in each group) were needed to provide 80% power to detect a statistically significant treatment effect for each of the primary endpoints (maximal walking speed and Barthel index score at three months compared with baseline; two sided significance level α=0.025 for each primary outcome, two sample t test). Accounting for a 20% dropout rate, we planned a total sample size of 215 participants. The predefined analyses have been performed as described in the statistical analyses plan of the trial (version 1.0, available online) and were conducted using SPSS, STATA, and R statistical software.222324
All randomised participants were included in the full dataset for the intention-to-treat analysis. Group differences for each primary outcome were analysed using two separate analyses of covariance, with baseline measures as covariates and an additional random effect (random intercept model) to account for clustering of participants in centres. The primary outcomes at follow-up (maximal walking speed and Barthel index score three months after stroke) were the dependent variables in these analyses, and baseline scores and intervention group were independent variables. Additionally, we adjusted the analyses for age, sex, and functional impairment (as assessed by the functional ambulation category test). We imputed missing data because of attrition by using multivariate imputation by chained equations (mice) based on 10 imputed datasets and relevant information generated by the R package mice.25 The supplementary appendix provides detailed descriptions of data imputation and handling missing data. If we were unable to assess data on mobility measures at baseline because of severe impairment, reasonable single value imputation was carried out by using half the speed of the slowest participant in the group. Analyses of safety endpoints were done using Poisson regression models, which account for the time each participant is at risk and allows incidence rate and incidence rate ratios with confidence intervals to be calculated.
Prespecified subgroup analyses for the primary outcomes were exploratory for sex, age groups, type of stroke, impairment measured by NIHSS and functional ambulation category, and time from stroke to start of intervention. For each subgroup analysis, we tested the interaction between treatment allocation and subgroup to test whether any difference in treatment effect between subgroups was substantial. For each subgroup we also provided mean treatment effects and 95% confidence intervals.
Secondary outcome measures were analysed using a three level mixed model where the repeated measures were nested in participants and participants were nested in centres. We used baseline variables of outcomes as covariates. Models were additionally adjusted for age, sex, and baseline functional ambulation category. In all models we included interaction terms for time point and treatment group. Reported effect estimates were calculated using post-estimation procedures. All models (except for mRS and functional ambulation category) are based on 10 imputations with chained equations and groupwise imputation (see supplementary table S3). For the mRS and functional ambulation category, we used an ordinal logistic mixed regression model including respective covariates for adjustment and random intercept to account for repeated measures. The group variable for centre was entered as fixed covariate in the ordinal mixed models to avoid instability of models. Variables with non-normal distribution were log transformed before analyses. All secondary analyses were carried out in an exploratory framework. No adjustment for multiple testing was applied for secondary analyses.
Patient and public involvement
Before and during the trial, a patient representative appointed by the Berlin Stroke Alliance participated in meetings of the trial’s executive steering committee. A member of the trial centre informed the Berlin Stroke Alliance (including participants and family members) about the progress of the trial on a regular basis. After the last trial visit, each participant received a summary of his or her personal outcome measures and blood test results. Findings of the trial will be shared with all participants by providing access to the full manuscript. The supplementary appendix provides a section for participants and carers who provided additional information.
Results
From 26 September 2013 to 30 April 2017, a total of 12 866 adults were screened of whom 200 were included in the trial and underwent randomisation (105 were assigned to aerobic physical fitness training and 95 to relaxation sessions (control group) in addition to standard care (fig 1). The main reasons for exclusion were a Barthel index score greater than 65, stroke onset more than 45 days before screening, and presence of comorbidities at the time of screening (mainly cardiac). The full analysis set entered the intention-to-treat analysis. The mean age of the study cohort was 69 (SD 12) years and 41% were women. The median NIHSS score was 8 (interquartile range 5-12) points at days 3-5 after stroke. Baseline personal and clinical characteristics were similar in both study groups, except for the six minute walk test and Rivermead mobility index, which were higher in the relaxation group. Table 1 lists the baseline characteristics. The amount of physiotherapy applied during inpatient and outpatient standard care between baseline and follow-up visit three months after stroke was similar between groups (see supplementary table S14).
The median time from stroke onset to start of intervention was 28 (interquartile range 17-40) days. Adherence to the study protocol was good to moderate (fig 2). The mean delta heart rate (pre-post intervention) was 15 (SD 9) beats per minute (bpm) in participants assigned to aerobic physical fitness training compared with −2 (SD 3) bpm in participants assigned to relaxation. Among participants randomised to aerobic physical fitness training, the median percentage of training sessions performed at target heart rate was 70% (interquartile range 23-100%) with improved adherence towards the end of the intervention period (fig 2). The amount of therapy applied during standard care was similar for severely impaired participants (functional ambulation category 0-1) compared with less severely impaired participants (>1), indicating similar treatment conditions (see supplementary table S7). Participants in the aerobic physical fitness training group received a mean of 16 (SD 6) sessions with a mean duration of the core intervention of 21 (SD 4) minutes, compared with a mean 17 (SD 5) sessions and mean duration of 24 (SD 3) minutes in the relaxation group. Eighteen participants in the aerobic physical fitness training group (17%) did not reach the required amount of 15 intervention sessions, compared with 11 participants (12%) in the relaxation group. Main reasons for termination of the intervention were early transfer to a non-participating hospital (n=4, each group) and a serious adverse event (n=5 in aerobic physical fitness training group; n=3 in relaxation group, see fig 1). At three months after stroke, 34 participants (17%) were lost to follow-up, and respective data were imputed for the intention-to-treat analysis using multiple imputation methods (see supplementary appendix for detailed description). The prespecified per protocol analysis comprised data for 151 participants (76% of the full analysis set), 80 participants in the aerobic physical fitness training group and 71 in the relaxation group.
Table 2 lists the primary efficacy outcomes. The adjusted mean change of maximal walking speed from baseline to three months after stroke was 0.4 m/s (95% confidence interval 0.3 to 0.4 m/s) in the aerobic physical fitness training group and 0.3 m/s (0.2 to 0.4 m/s) in the relaxation group, resulting in an adjusted treatment effect of 0.1 m/s (0.0 to 0.2 m/s; P=0.23, primary efficacy outcome). The adjusted mean change in Barthel index score three months after stroke was 30 points (95% confidence interval 24 to 36) in the aerobic physical fitness training group compared with 30 points (23 to 36) in the relaxation group, resulting in an adjusted treatment effect of 0 (95% confidence interval −5 to 5; P=0.99, primary efficacy outcome). Figure 3 shows the change in maximal walking speed and Barthel index score during the trial.
In the per protocol analysis, the mean change in maximal walking speed was 0.4 m/s (95% confidence interval 0.3 to 0.5 m/s) in the aerobic physical fitness training group and 0.3 m/s (0.2 to 0.4 m/s) in the relaxation group, resulting in a treatment effect of 0.1 m/s (95% confidence interval −0.1 to 0.2 m/s). The mean increase in Barthel index score after three months was similar in both groups: aerobic physical fitness training 32 (95% confidence interval 28 to 37) versus relaxation 31 (27 to 35); treatment effect 1 (95% confidence interval −4 to 6). Figure 4 shows the results for the prespecified subgroup analyses. Exploratory subgroup analysis for maximal walking speed suggested a greater treatment effect in women than in men: 0.3 (95% confidence interval 0.1 to 0.5) v 0.0 ( −0.2 to 0.1); P=0.01 for interaction. Figure 5 and supplementary figure S2 show the results for subgroup analyses of continuous variables using splines.
All secondary analyses were done in an exploratory framework. Overall, no substantial differences in maximal walking speed or Barthel index score between groups were observed at the end of intervention or at follow-up six months after stroke (table 3).
The six minute walk test showed a mean adjusted difference of 27 m (95% confidence interval 0 to 54 m) in favour of aerobic physical fitness training compared with relaxation at three months after stroke (adjusted for baseline, age, sex, and functional ambulation category). Other exploratory secondary analyses did not show substantial differences between study groups three months after stroke. At follow-up six months after stroke, the relaxation group showed greater improvements in the resistance to passive movement scale sum score (treatment effect 2.6 (95% confidence interval 0.6 to 4.5)) and the Rivermead mobility index subtest arm (treatment effect −1.1 (−2.0 to 0.0)) compared with aerobic physical fitness training (table 3).
The aerobic physical fitness training group had a higher rate of serious adverse events (n=22) than the relaxation group (n=9) at three months after stroke (incidence rate ratio 1.81, 95% confidence interval 0.97 to 3.36). Fourteen participants in the aerobic physical fitness training group were admitted to acute hospitals compared with five in the relaxation group (2.53, 0.91 to 7.04). Recurrent strokes occurred in eight participants in the aerobic physical fitness training group and in three participants in the relaxation group (2.41, 0.64 to 9.10). No serious adverse events occurred during intervention sessions. Self reported falls during the intervention period occurred more often in the aerobic physical fitness training group (2.34, 1.26 to 4.34) and self reported dizziness occurred more often in the relaxation group (0.33, 0.12 to 0.90, table 4).
Discussion
In adults with moderate to severe subacute stroke receiving standard inpatient rehabilitation therapy, a four week intervention of additional aerobic physical fitness training was not superior to a control intervention based on relaxation in improving activities of daily living and maximal walking speed three months after stroke. Analysis of safety showed an increased risk of falls during the treatment period and suggested a higher number of acute hospital admissions and recurrent strokes in participants randomised to aerobic physical fitness training. For clinical practice, the results of this pragmatic trial26 do not support the use of aerobic physical fitness training in moderately or severely affected adults in the subacute phase of stroke.
Comparison with other studies
The treatment effects in mobility outcomes observed in the current study are in line with results reported in the latest Cochrane Collaboration meta-analysis of physical fitness trials after stroke6 and randomised trials of circuit class training interventions.2728 In our trial, however, neither the intention-to-treat analysis nor the per protocol analysis showed a substantial difference in maximal walking speed between study groups. This finding contrasts with that of previously published trials reporting beneficial effects of fitness training on maximal walking speed.293031 Interventions in these previous trials were compared with usual care only, however, and the reported improvements were in smaller cohorts comprising participants with late subacute or chronic stroke and less severe disability. As recently endorsed by the Stroke Recovery and Rehabilitation Roundtable taskforce, trials should focus on the early subacute phase of stroke (days 7-90 after stroke)10; in the present trial more than 99% of participants were recruited in this subacute phase. This phase is thought to be a critical time for neuroplasticity32 and therefore might serve as an important period for rehabilitation to harness endogenous neural repair. Despite early enrolment of participants to our trial, we were not able to show enhanced treatment effects. Interestingly, a recent meta-analysis of randomised controlled trials on bodyweight supported treadmill training after stroke concluded that participants who walked independently (functional ambulation category score >2) improved in walking speed and walking endurance, whereas those who were not able to walk independently (score 0-2) did not improve with treadmill training.33 This fact could explain why our trial failed to show a statistically significant improvement in primary outcome measures, given that about 75% of the study cohort had functional ambulation category scores between 0 and 2 at baseline. However, no interaction between functional ambulation category score and treatment effect was observed in the respective subgroup analysis (fig 4 and supplementary figure S2). No treatment effect was observed with activities of daily living three months after stroke, which contrasts with the findings of smaller, previous trials including participants in the early and late subacute stage of stroke.1213 Until now, evidence that physical fitness reduces disability after stroke has been inconclusive for activities of daily living, and positive effects on disability after stroke could primarily derive from improvements in mobility.6 Aerobic physical fitness training compared with relaxation had no beneficial effect on scores on the Barthel index, functional ambulation category, or modified Rankin scale (see tables 2 and 3). Current outcome measures of activities of daily living differ in sensitivity, and the Barthel index might not be sensitive enough to capture small but clinically meaningful differences in activities of daily living related to aerobic training after stroke. Exploratory analyses of secondary outcome measures suggested small beneficial effects in fitness measures for participants randomised to aerobic physical fitness training at three months after stroke, as reflected in the six minute walk test (see table 3). This was a secondary exploratory finding, however, and cannot be used for inferences on treatment effects. Thus, adequately powered trials need to confirm whether bodyweight supported, treadmill based, aerobic physical fitness training improves measures of endurance at a clinically important level in this stroke population.
No safety concerns were reported for aerobic physical fitness training in the early subacute phase in two smaller previous studies comprising survivors of mild to moderate stroke.3435 However, in the large randomised controlled LEAPS trial, the proportion of participants with multiple falls was higher in the early locomotor training group (starting two months after stroke) compared with the late locomotor training group (starting six months after stroke).11 Similarly, in the current trial, falls occurred more often in the aerobic physical fitness training group than in the relaxation group during the intervention period. In contrast, participants in the relaxation group reported dizziness more often than participants in the aerobic physical fitness training group (see table 4). People with stroke are at increased risk for repeat falls, and fall prevention programmes are needed.36 Hence, and in opposition to current guideline recommendations,7 treadmill based aerobic physical fitness training should be administered with caution early after moderate to severe stroke. A Very Early Rehabilitation Trial after stroke (AVERT) mobilised participants within 24 hours after stroke and found a worse outcome after three months, but no differences were observed in walking related outcome measures.37 Although AVERT, LEAPS, and the present trial differ in terms of study population, timing after stroke, and type of intervention, these studies did not replicate the previously reported beneficial effects of specific rehabilitation interventions in small cohorts, while at the same time detecting a larger number of relevant adverse events and serious adverse events.
Strengths and limitations of this study
This is a randomised controlled, multicentre stroke rehabilitation trial assessing the efficacy and safety of an aerobic, bodyweight supported fitness intervention compared with relaxation in adults with subacute stroke. Compared with previous post-stroke fitness trials,6 our trial recruited a substantially larger sample size comprising adults with moderate to severe stroke and assessed a broad spectrum of patient centred outcome measures. The study does, however, have limitations. Firstly, recruitment took place between days 5 and 45 after stroke, therefore variations in early neurological recovery could have increased differences in outcome measures and might have affected current conclusions. However, the impact of the additionally induced variations is limited because almost all participants were recruited within the time window of early subacute stroke,10 and subgroup analyses (see fig 4) could not detect differences in treatment effects for participants receiving the intervention early after stroke (<2 weeks) compared with late after stroke (>2 weeks). Secondly, despite random allocation, the aerobic physical fitness training group was more severely affected at baseline, but we adjusted for baseline values in statistical analyses. Thirdly, findings are only applicable to moderately to severely affected adults with subacute stroke and are not generalisable to the stroke population, especially not to people with chronic stroke. Fourthly, less than 4% of the screened adults with stroke were included in the trial, and the severity of impairment might have resulted in a substantial proportion of participants terminating the intervention prematurely; a limitation often observed in early stroke rehabilitation trials.91138 Fifthly, the intervention period of four weeks could have been too short to show additional benefits compared with a relaxation control intervention; and the lack of a control arm for usual care only limits the understanding of the treatment effects of relaxation therapy.
Clinical implications and future research
Our trial provides evidence that an aerobic physical fitness training intervention with bodyweight support cannot be generally endorsed in adults after subacute stroke and should be administered with caution when applied early after moderate or severe stroke. Carers should closely monitor people with stroke for recurrent cardiovascular events and provide additional support after training to prevent falls. Despite these findings, aerobic physical fitness could still be an invaluable part of stroke rehabilitation—for example, in people with chronic stroke or mildly affected with subacute stroke.
Based on our results, trials should investigate if longer intervention periods are necessary to capture major changes in activities of daily living, assess the treatment effects of relaxation programmes compared with usual care, and recruit participants at fixed time points after stroke to reduce variance in outcome measures.1039 Future trials might also evaluate whether the observed sex specific difference in change of maximal walking speed or the effects on endurance measures can be replicated.
Conclusion and policy implications
A four week intervention of a bodyweight supported, treadmill based, aerobic physical fitness training in adults in the subacute phase of moderate to severe stroke is not superior to relaxation sessions with regard to maximal walking speed and activities of daily living. The risk of falls was higher in participants randomised to aerobic physical fitness training. Compared with current guideline recommendations,7 these results do not appear to support the use of aerobic bodyweight supported fitness training in this stroke population.
What is already known on this topic
Current guidelines endorse cardiorespiratory training within post-stroke rehabilitation programmes
Large randomised controlled trials of this recommendation are scarce, resulting in inconclusive data on efficacy for disability (activities of daily living) and safety of physical fitness training after stroke
What this study adds
Results suggest that in adults with moderate to severe subacute stroke, in addition to standard rehabilitation care, aerobic, bodyweight supported, treadmill based fitness training did not improve maximal walking speed or activities of daily living compared with relaxation
The rate of serious adverse events was higher in the aerobic physical fitness training group than relaxation group
Compared with current guideline recommendations, these results do not appear to support the use of aerobic, bodyweight supported, treadmill based fitness training in this stroke population
Acknowledgments
We thank the participants and their family members for participating in the trial, and the Berlin Stroke Alliance for non-financial support of the trial planning and conduction.
This study was presented in part at the 4th European Stroke Organisation Conference in Gothenburg, Sweden, on 17 May 2018.
Footnotes
Contributors: AHN, TR, MEb, and AF contributed equally to the study. AF, MEb, AHN, TR, AM, and SH conceived or designed the study. All authors were responsible for acquisition of data, data analysis, or interpretation of data. AHN drafted the manuscript. AF, AHN, MEb, and TR had full access to all the data in the study and take responsibility for the integrity of the data and the accuracy of the data analysis. AHN, TR, MEb, and AF contributed equally to the final manuscript. UG and TR performed statistical analyses. AF, MEb, ME obtained funding. AM and ME provided administrative, technical, or material support. AF, AHN, MEb, and TR supervised the study. All authors critically revised the manuscript for important intellectual content and gave final approval of the version to be published. AF is the guarantor of the paper and takes responsibility for the integrity of the work from inception to published article. The corresponding author attests that all listed authors meet authorship criteria and that no others meeting the criteria have been omitted. SH died before publication of the study.
Funding: This trial was supported by the German Ministry for Health and Education (01EO0801) through Center for Stroke Research Berlin grant G.2.15. The funder had no role in study design; data collection, analysis, or interpretation; or writing manuscript. AHN, AF, TR, MEb, and UG had full access to all the data in the study and the corresponding author had final responsibility for the decision to submit for publication.
Competing interests: All authors have completed the ICMJE uniform disclosure form at www.icmje.org/coi_disclosure.pdf (available on request from the corresponding author) and declare: German Ministry for Health and Education (01EO0801) through Center for Stroke Research Berlin grant G.2.15; no financial relationships with any organisations that might have an interest in the submitted work in the previous three years; no other relationships or activities that could appear to have influenced the submitted work. AHN is participant in the Berlin Institute of Health BIH-Charité clinical scientist programme and reports grants from BIH during the conduct of the study. AM reports funding from Neurocure (German Research Foundation EXC257). MEn reports grant support from Bayer, the German Research Foundation, the German Federal Ministry of Education and Research, the German Center for Neurodegenerative Diseases, the German Centre for Cardiovascular Research, the European Union, Corona Foundation, and Fondation Leducq; fees paid to the Charité from Bayer, Boehringer Ingelheim, Bristol-Myers Squibb/Pfizer, Daiichi Sankyo, Amgen, GlaxoSmithKline, Sanofi, Covidien, Ever, Novartis, all outside the submitted work. AF reports grant support from the German Research Foundation, German Federal Ministry of Education and Research, European Union, Else Kröner Fresenius Stiftun, and Hannelore Kohl Stiftung; consultant fees from Novartis and Bayer, and honoriums for presentations in scientific symposia by Novartis and Bayer, all outside the submitted work. UMW reports honorariums for presentations in scientific symposia by Novartis and Bayer.
Ethical approval: This study was approved by the institutional review board of Charité–Universitätsmedizin Berlin (EA1/138/13). The trial was conducted in line with the CONSORT extension for non-drug treatments, and study procedures were carried out in accordance with the Declaration of Helsinki.
Data sharing: The statistical analysis plan is available at https://doi.org/10.6084/m9.figshare.5375026.v1. The raw trial data are provided by the authors on a secure online repository (see supplementary appendix for link). Data include anonymised individual patient variables for results reported here, a read-me file with data dictionary and analyses scripts used in this study. Data will be available three months after publication of the article. Further information can be shared on individual request addressed to the corresponding author.
The lead authors (AHN, TR, MEb, and AF) affirm that the manuscript is an honest, accurate, and transparent account of the study being reported; that no important aspects of the study have been omitted; and that any discrepancies from the study as planned (and, if relevant, registered) have been explained.
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