Ethical approval
This randomised clinical feasibility trial was approved by the Scientific-Ethics Committee of the Capital Region (H-16041794) and is registered on www.clinicaltrials.gov (ClinicalTrials.gov identifier: NCT02924649); the trial protocol has been published in Trials [1]. The project manager (CGR) is responsible for collecting and storing data and all correspondence. After a patient is found to be eligible for the trial, informed consent from the proxy and a trial guardian (a physician not involved in the trial) is obtained by CGR. The trial is carried out in accordance with the principles of the Helsinki Declaration [9].
Primary research questions
Is an early head-up tilt protocol feasible in patients with severe traumatic brain injury, in terms of the number of participants who are successfully included, number of exercise sessions performed in the experimental group, and the number of patients with serious adverse events (SAE) and non-serious adverse events (AE) and serious adverse reactions (SAR) and non-serious adverse reactions (AR)?
Exploratory research questions
- Does early head-up tilt with stepping reduce the number of AE, AR, SAE, and SAR compared with standard care after severe traumatic brain injury?
- Does early head-up tilt with stepping improve the level of consciousness (Coma Recovery Scale – Revised) after four weeks, early functional abilities (Early Functional Ability scale) after three months, or functional independence (Functional Independence Measure) after three months, compared with standard care after severe traumatic brain injury?
- Does head-up tilt with stepping improve the level of consciousness (Coma Recovery Scale – Revised), early functional abilities (Early Functional Ability scale), or functional independence (Functional Independence Measure) after one year compared with standard care in patients with severe traumatic brain injury?
Main trial design
The present statistical analysis plan describes our planned analyses for the feasibility trial, investigating head up tilt with stepping versus standard care in patients with severe traumatic brain injury. As described in the published protocol the sample size (n=60)) has been chosen as a realistic number to reach for this feasibility trial [1].
The trial is a randomised clinical feasibility trial with a pragmatic stratification according to the Glasgow Coma Score at inclusion (3-6 compared to 7-10 points). The patients are randomised in a 1:1 ratio by the Copenhagen Trial Unit using a central web-based randomisation system.
Besides standard care, the experimental intervention group receives daily (Monday to Friday) mobilisation on a tilt-table to the standing position for up to 20 minutes per session. This orthostatic exercise continues for four weeks from randomisation or until the patient can stand from a chair or bed with assistance. The tilt-table has a build in stepping device that increases the venous return of blood to the heart and thereby counteracts orthostatic hypotension and increases standing time [10,11]. The control group receives standard care. Standard care is decided in collaboration between doctors, nurses, and physiotherapists and will be monitored
during the trial. Only a small amount of time is used on mobilising the patient to either the edge of the bed or to a wheelchair whilst admitted to the neurologic ICU. The focus of the physiotherapist is on respiratory function and in bed positioning to avoid bedsores.
Additional exploratory physiological outcomes are blood pressure, blood flow velocity of the middle cerebral artery (MCAv), and electrocardiography, which were all measured in the supine position and during head-up tilt at two weeks and four weeks after randomisation. Furthermore, continuous electrocardiography was recorded for up to five days from randomisation in the trial. It is our intention to analyse and publish data on the heart rate variability frequency domain and time domain indices. The statistical analysis plan for these outcomes will be made public in a separate report.
Primary feasibility outcomes
Our primary feasibility outcomes are as follows:
The lower limit of the confidence interval of the inclusion ratio (the proportion of included participants randomised compared to all eligible patients). For example, if 44 of 60 eligible patients agree to participate, then the proportion will be 73% with a 95% confidence interval (95% CI) between 60% and 84%. The lower limit for this feasibility outcome is set at 60%; if the lower limit of the confidence interval of the gathered data of the HUT-TBI Trial is at 60% or higher, then the trial is considered to be successful in terms of inclusion. This is equivalent to a one-sided test (please see statistical section below).
The lower limit of the confidence interval of the intervention success rate defined as the proportion of participants allocated to the experimental intervention who received at least 60% of the planned exercise sessions. For example, if 21 of 30 participants (70%) randomised to the experimental intervention group receive 60% of the exercise sessions, the lower limit of the confidence interval will be 52%. Accordingly, if the lower limit of the confidence interval of the gathered data of the HUT-TBI Trial is at or above 52%, the trial will be successful in terms of exercise completeness.
Both the inclusion ratio and the intervention success rate limits are arbitrary limits decided together with the clinical staff at the department. It therefore emphasizes clinical reality on the validity of the data.
Our safety outcomes are defined as either proportion of participants with either an SAE, SAR, AE or AR not considered serious [12]. SAEs are defined as any undesirable event that result in death, is life-threatening, requires prolongation of existing hospitalisation, results in persistent or significant disability or incapacity, or requires intervention to prevent permanent impairment or damage, whether considered related to the trial intervention or not [12]. AEs are defined as any undesirable event not considered serious occurring to a participant during the trial. The proportion of participants with at least one SAE, SAR, AR, or AE during the intervention period will be compared between the two intervention groups. The proportion of SAE will be assessed through inspection (descriptive analysis) and through statistical analysis (see below).
Exploratory clinical outcomes
For the exploratory clinical outcomes, we have chosen three outcomes: The Coma Recovery Scale - Revised (CRS-R) [13], the Early Functional Ability scale (EFA) [14,15], and the Functional Independence Measure (FIM) [16,17], all of which are scored at baseline and after four-weeks, three-months and one-year. The CRS-R reflects changes in consciousness and will be analysed at the four-week time point (end of intervention period) comparing the two intervention groups and was scored by assessors blinded to the intervention allocation. The EFA evaluates early functional changes and the FIM evaluates the ability to independently perform functions and activities of daily living. Both will be evaluated at the three-month time point. Secondly, the data for all three exploratory clinical outcomes will be presented as longitudinal data in a figure (error bar plot) showing the mean and the 95% CI for each group. At the one-year follow up, the same three outcome scales are used and supplemented by the Glasgow Outcome Scale – Extended (GOSE); the latter is used routinely at the department for the one-year follow-up.
Exploratory physiological outcomes
For exploratory physiological outcomes we have measured the haemodynamic response to a head-up tilt at baseline, after two weeks, and after four weeks in both groups. From these data we will calculate the cerebral autoregulation index (Mxa) measured by transcranial Doppler ultrasound of the middle cerebral artery at each time point. In short, mean arterial blood pressure and mean MCAv are correlated using a Pearson correlation coefficient. Correlations are calculated during 300 seconds in the supine position (rest) and 300 seconds during head up tilt with 70 degrees head elevation. The Mxa will then principally be considered dichotomously in order to reflect intact cerebral autoregulation of blood flow, with a correlation equal to or below 0.3 or impaired if it is above 0.3 [18]. Data at four weeks will be compared between groups. Secondarily, we will analyse the Mxa as a continuous variable and we will utilise other methods such as the Gosling Pulsatile index, or the cerebrovascular resistance index.
Statistical analyses
Statistical analysis will be handled using STATA (StataCorp, College Station, Texas, USA).
All baseline characteristics will be presented for each intervention group. Continuous variables will be summarised using means and standard deviations or medians and interquartile range depending on distribution of data. Discrete variables will be presented as frequencies, proportions, and percentages.
Timing of outcome assessments can be found in the published protocol in figure 1 [1].
Regarding the feasibility outcome, we will not adjust for multiplicity since all three outcomes should be achieved for the trial to be considered feasible. That is, the inclusion ratio and exercise success rate should be above the decided limits and the adverse events should not be significantly different in favour of the standard care group. We have decided to use a one-sided test for the feasibility outcomes corresponding to the description above. In these analyses, a significance level of 2.5% will be used.
All our analyses will primarily be intention-to-treat, i.e. all randomised participants will be included in the primary analyses and analysed as randomised. We will secondly perform per protocol analyses including the participants allocated to the intervention who received at least 60% of the planned exercise sessions compared to the patients in the standard care group.
If we do not reach the desired number of participants in the trial, we will consider to analyse our data using Trial Sequential Analysis [19,20]. In this case, we will use the prespecified standard deviations and minimal relevant differences described in supplementary table 1 for continues outcome and the proportion in the control group for dichotomised outcomes. The calculations will be based on an alpha of 5% and a beta of 10%. Trial Sequential Analysis reduces the risk of type I and type II errors due to small sample size and multiple outcome testing [20].
Analysis will start after the last three-month follow-up has been collected and after submission of this statistical analysis plan (end of March 2019). The analysis of the one-year follow-up data will start after data from the last patient has been collected in late December 2019.
Feasibility outcomes
The first two primary feasibility outcomes will be derived from the trial with the above-mentioned lower limits of the proportions. For the intervention to be feasible, both feasibility outcomes should be achieved, and the early orthostatic intervention group should not have an overrepresentation of SAE, AE, SAR, AR or suspected unexpected serious adverse reactions (SUSAR).
All analysis described below using general linear regression, logistic regression, or mixed-model linear regression will be adjusted for the protocol specified stratification variable (high or low GCS).
We will use inspection of data (descriptive analysis) to evaluate adverse events due to the low power. Secondly, we will use logistic regression to compare the proportions of participants with one or more SAEs, SARs, ARs, and AEs between the two groups [1]. Accordingly, we will use an alpha of 5%. Each patient with at least one SUSAR during the intervention period will be analysed as exploratory feasibility outcome also using logistic regression analysis. Where appropriate, we will present data with a 95% CI.
Exploratory clinical outcomes
All exploratory clinical outcomes and physiological outcomes are on a continuous interval scale.
The exploratory clinical outcomes will primarily be compared between allocation groups at specified time points. The CRS-R will be analysed at the four-week time point and EFA and FIM will be analysed at the three-month time point using general linear regression analysis. As a sensitivity analysis, longitudinal data will be analysed using mixed model linear regression with each participant as a random effect and the time points as the fixed effect for analysis of longitudinal data over multiple time points.
Each outcome, with the corresponding minimal relevant difference, standard deviation and power level can be found in Supplementary table 1. The one-year follow up data for CRS-R, EFA, and FIM will be analysed in the same way. Furthermore, for the one-year analysis the Glasgow outcome scale extended will be compared between groups using general linear regression and adjusting for stratification-specific variables.
In case the regression models described above (linear regression and mixed model) cannot be fitted due to breach of their underlying assumptions (e.g. skewed distribution of data/residuals), non-parametric methods (e.g. Van Elteren test) taking the stratified randomisation into account will be employed. Analysis will in all cases be conducted at the prespecified time points as stipulated above. As described in our protocol, we have still reported that all results will be interpreted as hypothesis generating.
Exploratory physiological outcomes
The exploratory physiological outcomes measuring cerebral autoregulation will be compared at the 4-week time point (or end of intervention). To do this, we will use logistic regression with the Mxa as a binary outcome (above 0.3), as the dependent variable and with further adjustment for age and sex. The Mxa will also be tested as a continuous variable (ranging from -1 to 1) using mixed-model linear regression and Fischer’s Z transformation with each participant as a random effect for analysis of longitudinal data over multiple time points. The latter is used as a sensitivity analysis. The same approach will be used for the Gosling Pulsatile index and the cerebrovascular resistance index.
Missing data
Trials conducted in the ICU are at high risk of missing data alone on the account of the patient´s condition [21]. If data are missing, we will consider using multiple imputation according to the recommendations by Jakobsen and colleagues [22]. These recommendations states that up to 40% of missing data can be imputed, but the method of choice depends on the outcomes, whether the dependent variable has missing data only at baseline, etc. [22]. If multiple imputation is used the following variables will be incorporated in the analysis: baseline value of the dependent variable, stratification variable (GCS), end of post traumatic amnesia, and days to first mobilisation. For all continuous clinical outcomes, we will analyse survivors, and in a sensitivity analysis impute the lowest possible value for participants who died or dropped out as well as the best possible value. We will present the results of both analyses.
Trial status and profile
The inclusion period ended in December 2018 with only 38 patients included during a two-year period. End of the three-month follow-up period will be in March 2019 and the one-year follow up will be in December 2019. Flow of patients will be presented in a CONSORT diagram as reported in the protocol [1]. We will report the number of screened patients, the number of included patients, and the main reason for exclusion of eligible patients. Furthermore, we will present the number of patients who died within the four-week intervention period, within the first three months from randomisation, and within the first year.
Publication strategy
We plan to publish the following papers:
- The primary feasibility outcomes and the analyses of the exploratory clinical outcomes will be published separately to establish feasibility of the intervention and the sample size of a larger multicentre study (publication I).
- Analysis of the exploratory outcomes with the focus of investigating a specific physiological effect on cerebral autoregulation after a series of orthostatic exercises during head up tilt (publication II).
Presentation of results in tables and figures
Publication I: The CONSORT flow chart diagram will be presented as Figure 1 (not shown here). To assess the balance of our randomisation, description of baseline characteristics will be presented in a table (Table 1). Variables will be summarized as either frequencies and percentages or as continues or ordinal variables as mean with standard deviations (SD) or median and interquartile range (IQR) (see Appendix 1).
The primary feasibility outcome will be presented in Table 2 and Table 3. The first table will consist of the proportion of patients included in the trial as well as the number of patients who successfully received more than 60% of the intended interventions. Table 3 will present and describe the AE seen during the intervention period as well as the logistic regression analysis.
The exploratory clinical outcome will be presented in a figure showing each outcome over the four time points, with the absolute numbers of each outcome at each time point in a Supplementary table 2. Furthermore, the longitudinal analysis will be presented in a figure showing each time point with confidence intervals (not illustrated).
Publication II: The second publication will present Table 1 as a demographic table. The results from the haemodynamic measurements (heart rate, mean arterial pressure and MCAv) will be presented in a figure with included table (Figure 1). The figure will consist of three graphs (A, B and C) with data summarized beneath, showing Δ-values between supine position and during head up tilt at baseline, after 2 weeks and after 4 weeks. As supplementary material we will present a spaghetti-plot of each of the above variables in supine and in standing (Supplementary figure 3, not shown here). Table 4 shows the Mxa values in supine and in standing for both groups at the end of the intervention period. Alongside this, a Figure 3 (not shown here) will illustrate the time line for Mxa, with Mxa on the y-axis and time on the x-axis, showing a mean with confidence intervals for each time point (baseline, 2 weeks, 4 weeks). Figure 2A will illustrate Mxa in the supine and Figure 2B in standing. Lastly, a Table 5 will show the frequency of intact cerebral autoregulation in the two groups with P-values indicating group differences.