Multicentre, single-blind randomised controlled trial comparing MyndMove neuromodulation therapy with conventional therapy in traumatic spinal cord injury: a protocol study.

INTRODUCTION: This protocol is describing a multicentre, single-blind randomised controlled trial. The objective is to compare the efficacy of MyndMove therapy versus conventional therapy (CT) in improving upper extremity function in individuals with C4-C7 traumatic, incomplete spinal cord injury (SCI). It is being conducted in two US and two Canadian SCI rehabilitation centres. METHODS AND ANALYSIS: Sixty people aged 18 years or older with a C4-C7 incomplete (AIS B-D) SCI between 4 months and 8 years postinjury are randomised to receive 40 sessions of MyndMove neuromodulation therapy or CT within a 14-week period of time. Therapy sessions are 1 hour in duration with a dose of 3-5 sessions per week. Assessments occur prior to randomisation, after 20 sessions, after 40 sessions and 10 weeks after the last session. The primary outcome measure is the efficacy of MyndMove therapy versus CT in improving upper extremity function as measured by Spinal Cord Independence Measure III: Self-Care subscore after 40 sessions. Secondary outcomes include: (1) improvements in the SCIM mobility subscore; (2) upper limb functions measured by Graded Redefined Assessment of Strength, Sensibility and Prehension and (3) Toronto Rehab Institute Hand Function Test; (4) To assess safety as measured by serious and non-serious adverse events recorded for participants in both groups of the study population over the duration of the study; (5) to compare the change in quality of life as measured by the Spinal Cord Injury-Quality of Life; and (6) to evaluate the impact on healthcare resource utilisation. ETHICS AND DISSEMINATION: All ethical approvals were obtained prior to enrolling any participants. Dissemination of the results of the study will be made at peer-reviewed academic meetings and through peer-reviewed medical journals TRIAL REGISTRATION NUMBER: NCT03439319. © Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.

RCT Entities:   Population Interventions Outcomes

A strength of this study is that it is a properly powered randomised controlled trial designed to detect functionally meaningful change in participants with tetraplegia.

This therapy requires the use of a device that is not currently part of standard rehabilitation for spinal cord injury and, as a result, the participant and treating therapist are not blinded.

The assessing therapist is blinded to reduce the risk of bias.

The statistical analysis team is blinded to the study group.

Introduction

Spinal cord injury (SCI) is a devastating, life-altering event that can lead to significant disability, in addition to socioeconomic challenges for the individual, family and community at large. A survey of people with SCI revealed that the majority of people with tetraplegia (which constitutes more than 50% of individuals with SCI) rated recovery of hand function as their highest priority.1 2 Currently, various approaches to improve hand function after SCI are used, for example: exercises, biofeedback, robotic therapy, task-specific movement therapy, reconstructive surgeries and functional electrical stimulation (FES) therapy. To date, FES therapy has been found to be one of the most promising approaches in improving voluntary hand function.3–18 One school of thought proposes that FES can be used as a short-term therapeutic intervention to help improve voluntary grasping function. A number of FES systems have been used for this application, for example: NESS H2004–6; the Bionic Glove and its newer version HandEstim Wireless Hand Stimulator8 9; and the complex motion system.12 18 Emerging evidence in tetraplegia suggests that electrical stimulation and FES therapy improve arm and hand function more than conventional therapy (CT), particularly when provided in combination with various types of CT. Recently, a study demonstrated that the functional benefits of massed practice of CT were greater when augmented by sensory stimulation.19 Another study demonstrated that exercise therapy combined with FES produced greater functional improvements compared with exercise therapy combined with traditional electrical stimulation.20

MyndMove therapy is a non-invasive FES neuromodulation therapy designed to restore voluntary reaching and grasping movements in individuals paralysed by SCI or stroke. It is based on FES principles and therapeutic interventions21 to provide clinically meaningful gains in both upper extremity function and self-care functional independence.22 The MyndMove system promotes development and re-establishment of neural pathways within the central nervous system (CNS) and between CNS and the upper extremities by engaging neuroplasticity following neurological injury.23 Therapists use the device with surface electrodes to deliver proprietary electrical stimulation sequences to induce targeted muscle contractions leading to functional movements. Over multiple sessions, the treatments are thought to reconnect the signal from the brain to the muscles, restoring voluntary use of their arms and hands. MyndMove therapy is approved for sale by Health Canada (licence number 93158) and has been confirmed by the FDA (510(k) Number K170564). MyndMove therapy has also been confirmed by FDA to be a non-significant risk device and exempt from an Investigational Device Exemption (IDE; reference file Q131135).

A pilot study comparing the effectiveness of FES neuromodulation therapy to CT has been conducted in individuals with cervical, incomplete SCI.24 In that study, a small number of participants with chronic C4–C7 American Spinal Injury Association Impairment Scale (AIS) B-D SCI were randomised to FES neuromodulation therapy or CT and received 39 hours of therapy over 13–16 weeks. The FES neuromodulation therapy group improved fivefold on the primary outcome measure (Toronto Rehabilitation Institute-Hand Function Test) compared with the CT group. However, because there were only eight people enrolled and the study was open label, a larger randomised controlled trial (RCT) with blinded assessments was needed to definitively compare the effectiveness of the two interventions.

The protocol for this multicentre RCT in people with tetraplegia following traumatic SCI aims to: (1) confirm the FES neuromodulation treatment effect as delivered by the MyndMove device across multiple investigational sites, (2) characterise the long-term benefits and retention of function by including long-term follow-up assessments and (3) compare the efficacy of MyndMove therapy to an equivalent number of hours of CT. The study will also evaluate the impact of MyndMove therapy on the quality of life for people with traumatic SCI (C4–C7) over the course of 24 weeks. Ultimately, the data from these studies will assist in redefining clinical best practices in SCI rehabilitation.

Methods and analysis

Trial design and setting

This study is designed as a multicentre, parallel group, two-arm, single-blind, RCT to compare the clinical outcomes of MyndMove therapy to CT for individuals with C4–C7 traumatic incomplete SCI with upper extremity paresis. See figure 1 for the study flow chart. The study is being conducted at four regional rehabilitation medical centres, in Canada and the USA, that specialise in providing neurorehabilitation to people with SCI. The first participant was enrolled in June 2019. It is estimated that the final participant will be enrolled by December 2020, but this may be negatively impacted by COVID-19.

Figure 1

CONSORT diagram of study flow chart. CONSORT, Consolidated Standards of Reporting Trials.

Recruitment and retention

Each of the investigational sites has experience in recruiting individuals with SCI for clinical studies, and each investigational site has a study coordinator assigned to the study who routinely reviews charts to identify potential study participants and to increase awareness of the planned clinical study within their community. Recruitment strategies include outreach to advocacy and support groups for individuals with SCI. Study coordinators will enhance retention of participants by developing rapport with them during the active portion of the trial, then periodically communicating with participants during the follow-up portion of the trial.

Eligibility criteria

Inclusion criteria:

Traumatic incomplete (AIS B-D) C4–C7 SCI.

Paralysis or paresis in both upper extremities.

At least 4 months (120 days) and less than 96 months (2920 days) post-traumatic SCI.

Baseline Spinal Cord Independence Measure III: Self-Care (SCIM-SC) ≤10.

From an inpatient (such as skilled nursing facility) or outpatient care setting.

Able to understand and follow instructions.

Able to tolerate being in a seated position for a least 1 hour required to deliver upper limb therapy.

Willing to attend treatment sessions and all assessment sessions.

Able to understand and provide informed consent.

Male and female participants ≥18 years of age at the time of enrolment.

Exclusion criteria:

Previous history of any other neuromuscular disorder or conditions that may affect motor response.

Upper extremity injury or condition prior to SCI that limits the function of the hand or arm.

Malignant skin lesion on the affected upper extremity.

Rash or open wound at any potential electrode site.

History of seizure disorder not effectively managed by seizure medications.

An implanted metallic part (eg, plates, screws or joint replacement) or electrical device (eg, implantable cardiac defibrillator, pacemaker and spinal stimulation). (Note: if the participant has passive metallic implants, the therapy can be delivered if the implants are located in an area other than where the electrical stimulant is to be delivered.)

Complete denervation of muscles that are targeted by MyndMove such that MyndMove is unable to elicit tetanic muscle contraction when upper limits of stimulation intensity (of the device) for the targeted muscle are applied.

Poorly controlled autonomic dysreflexia (as determined by the local site physician).

History of psychiatric illness requiring hospitalisation within past 24 months.

Active drug treatment for dementia.

Life expectancy of less than 12 months due to other illness.

In the judgement of the medical provider, participant has medical complications that may interfere with the execution of the study.

Currently enrolled in another upper limb intervention study and/or has received MyndMove therapy within the past 3 months.

Enrolled, in the past 6 months, in a clinical study involving drugs or biologicals.

Currently dependent on a ventilator.

Botulinum toxin injection into affected upper extremity and the muscle targeted by MyndMove therapy within 6 months prior to the study start. No botulinum toxin injections in the upper extremity during the study treatment and follow-up period.

Women who are pregnant or planning to become pregnant in the duration of the trial.

Regional disorder of the upper extremities such as fracture, dislocation or joint contractures to less than 50% of expected range of motion.

Sample size

The sample size calculation is based on the test of the research hypothesis that the mean difference in SCIM-SC in the MyndMove intervention group is better than CT control group. The primary measure of effect is the difference in function measured using SCIM-SC at 14 weeks. The criterion for significance (alpha) has been set at 0.05. The test is two tailed, which implies that a mean difference in either direction will be interpreted. The sample was calculated using the power procedure in SAS V.9.2. With the proposed sample size of 30 in each of the two groups (ie, assuming a 1:1 allocation ratio) (ie, total sample size of 60), the study will have power of at least 80% to yield a statistically significant result using t-test (assuming an intention-to-treat principle for the analysis) of the difference between mean SCIM-SC scores at 14 weeks adjusting for baseline SCIM-SC scores at alpha=0.05. It is important to note that using the assumption of a t-test is more conservative in that an analysis of variance (ANCOVA) will lead to better power. This computation assumes that SCIM-SC scores are normally distributed, the mean difference is 3 points and the common within-group SD is 4.05. These estimates are modified estimates from the pilot study,24 which account for the type of intervention planned for in this study. The assumed minimal clinically important difference is considered to correspond to a substantially meaningful improvement on the SCIM-SC, approximately 3 points,25 26 and also represents a moderate effect of the intervention.

Allocation and blinding

Study participants will be stratified by rehabilitation site and will be allocated in a 1:1 ratio to the following two treatment arms:

MyndMove therapy: participants will receive a minimum–maximum of 36–40 1-hour sessions per day of MyndMove therapy within a 14-week period of time.

CT: participants will receive upper-limb CT of equivalent frequency, intensity and duration to MyndMove therapy (ie, a minimum-maximum of 36–40 1-hour sessions per day of CT within a 14-week period of time).

The randomisation schedule will be generated and maintained by a statistician at the Biostatistics Unit. A 1:1 allocation occur as per a computerised randomisation schedule stratified by site (to account for variation in rehabilitation programmes between Canada and the USA) using permutated blocks of random sizes and to ensure equal assignment of the MyndMove and the CT at each site. The block sizes will not be disclosed to ensure concealment. Sufficient randomisation sequence allocation, prior to study activation, will be generated to permit the enrolment and drop-out of at least 40% of the total sample size.

Participants who provide signed informed consent, meet all inclusion/exclusion criteria for the study and complete the baseline visit will be randomly assigned to one of the two treatment arms requested directly from REDCap system. Through REDCap, the randomisation allocation will be provided to the study coordinator. The study coordinator will then provide the information about treatment allocation to the participant and treating therapist. The therapist who is the outcome assessor will be blinded to the treatment allocation. All therapists (whether treating or assessing) will be licenced in physical or occupational therapy.

Intervention

Participants randomised to the MyndMove therapy group will receive FES therapy bilaterally at the therapist discretion based on clinical presentation/dominance and participant’s goals. Treatment will be provided in 1-hour sessions per day for a minimum–maximum of 36–40 sessions delivered no less than three times per week and up to five times per week within a 14-week period of time. Over the course of the sessions, the participants will progress through various movement sequences aimed at regaining natural, unassisted voluntary movements in the affected limb(s). The proposed volume of therapy is guided by discussions with clinicians experienced with delivery of MyndMove therapy along with previous clinical research studies.27

The type and frequency of protocols used will follow a standardised regimen in order to minimise cointervention variation across sites.27 Training for MyndMove will be provided prior to the initiation of the study. Guidance regarding protocol selection, sequence and frequency of repetition will be provided as a part of the training by MyndTec. The selection of protocols used during each treatment session will be captured. During each treatment session, therapists will select from a menu of preprogrammed stimulation protocols to facilitate various task-specific movements (table 1). Movement practice may be massed or distributed, depending on the tolerance of the participant (ie, muscle fatigue).

Table 1

Example MyndMove protocols

Movement practised*	Muscles stimulated with MyndMove†
Palmar grasp‡	Flexor digitorum superficialis and profundus. Thenar muscles. Extensor digitorum.
Lateral pinch grasp‡	Flexor digitorum superficialis and profundus. Thenar muscles. Extensor digitorum.
Pinch grasp‡	Thenar muscles. Extensor digitorum. First lumbrical.
Lumbrical grasp	Thenar muscles. Extensor digitorum. First, second and third lumbricals.
Tripod grasp	Flexor digitorum superficialis. Thenar muscles. Extensor digitorum. Second dorsal interosseous.
Side reach with finger extension	Biceps. Triceps. Middle deltoid. Extensor digitorum. Extensor carpi radialis longus. Extensor carpi ulnaris.
Forward reach and grasp	Biceps. Triceps. Posterior deltoid. Anterior deltoid. Extensor digitorum. Extensor carpi radialis longus. Extensor carpi ulnaris. Flexor digitorum superficialis and profundus. Thenar muscles.
Hand to mouth	Biceps. Triceps. Anterior deltoid.

*The movement is demonstrated for the participant by the therapist. The therapist then instructs the participant to voluntarily attempt the movement for about 10 s, after which electrical stimulation is provided with the appropriate MyndMove protocol.39

†Muscles not listed in order of stimulation.

‡Unilateral or bilateral stimulation may be used.

The CT intervention serves as an active control group and will use conventional rehabilitative therapy with control for the schedule, form and intensity of participant–therapist interactions and therapeutic activities in the MyndMove therapy group. During each treatment session, participants will receive CT of equivalent duration to the 1-hour sessions per day of MyndMove therapy. The type and frequency of interventions used will follow a standardised regimen developed by consensus across the centres for the CT in order to minimise intervention variation across sites. Conventional upper limb rehabilitation therapy, at the local institution, may include any or all of the following: (A) facilitation of reaching or prehension movements; (B) bilateral task-specific movement practice (distributed or massed, dependent on participant tolerance); (C) range of motion and mobilisation of joints; (D) splinting; (E sensorimotor stimulation (eg, TENS, acupuncture, muscle stimulation and biofeedback); (F) electrical stimulation (for strength, not function); and (G) reduction of oedema, if needed. The use of other FES devices during the course of the study will not be permitted. The Tempate for Intervention Description and Replication (TiDieR) checklist will be used to report results.

All other rehabilitation services will be provided throughout the intervention and follow-up period. This concomitant care, which may influence outcomes, will be captured throughout the study by self-report through the use of a healthcare resource utilisation questionnaire, provided to the participant and confirmed by the study staff. During the intervention period, the questionnaire will be completed by the participant to record any rehabilitation services and provide a categorical description of the treatment provided and duration of treatment sessions. This information will be reviewed by study staff and verified with the participant.

For all treatment arms, adherence to therapy will be captured to document any missed research therapy visits. This will allow for the assessment of the effectiveness of the treatment and the practicality of daily administration of the treatment. A per-protocol analysis will be completed using only data from those participants completing at least 30 treatments, which corresponds to 75% of allocated treatments.

Data collection and management

The Biostatistics Unit will provide data management and analysis for the study. All data will be deidentified to maintain confidentiality and captured on paper case report forms. Key data will be entered at each site directly into the electronic database created in REDCap.

An independent research monitor will be appointed, with expertise consonant with the nature of risk(s) identified within the research protocol. The duties, authorities and responsibilities of the independent research monitor will include: observation of recruitment and enrolment procedures and the consent process for individuals, overseeing study interventions and interactions, reviewing monitoring plans and unanticipated problems involving risk to subjects or others reports; and overseeing data matching, data collection and analysis. Monitoring activities will be performed both on-site and off-site according to Good Clinical Practices (GCP) guidelines. A MyndTec Study Monitor will conduct the site initiation visit, periodic site visits (with the independent research monitor) and a close-out visit for each site.

Schedule of data collection

A schedule of assessments and data collection is provided in table 2.

Table 2

A summary of assessments and data collection

Events	Screening visit	Baseline visit	Randomisation	Treatment period		Early termination assessment
				Interim assessment (after 20th treatment session)	End-of-treatment assessment (after 40th treatment session/14 weeks post first treatment visit)	End-of-study follow-up assessment (24 weeks post first treatment visit)
Consent
Informed consent form	×
Eligibility
Inclusion/exclusion criteria	×
Enrolment			×
Interventions
MyndMove therapy
Intensive conventional therapy
Assessments
Demographics and social status		×
General health history		×
History of injury event		×
Neurological	×	×
Blood pressure	×	×*		×*	×*	×*
Functional assessments
SCIM	×	×		×	×	×
GRASSP		×		×	×	×
TRI-HFT		×			×	×
Participation and quality of life
AE/SAE				×	×	×
SCI-QOL		×			×	×
Healthcare resource utilisation questionnaire		×		×	×	×
End of Therapy Questionnaire					×

×*=blood pressure is only required if the measurement is deemed abnormal or up to investigator’s discretion.

AE, adverse event; GRASSP, Graded Redefined Assessment of Strength, Sensibility and Prehension; SAE, serious adverse event; SCIM, Spinal Cord Independence Measure III; SCI-QOL, Spinal Cord Injury-Quality of Life; TRI-HFT, Toronto Rehab Institute Hand Function Test.

Adverse events (AEs) and serious adverse events (SAEs)

All AEs will be recorded and used to assess participant safety. AE will be recorded on the appropriate case report forms from the time written informed consent is obtained until completion of the study or until resolution of the reportable event. Information to be collected includes the description of the AE, date and time of onset, severity, duration, causality, outcome and relationship to the study procedure.

An AE or suspected AE is considered ‘serious’ if, in the view of either the investigator or sponsor, it results in any of the following outcomes: (1) leads to death, (2) is life threatening, or places the participant at immediate risk of death, (3) requires or prolongs inpatient hospitalisation, (4) results in a significant, persistent or permanent change, impairment, damage or disruption in the participant’s body function/structure, physical activities and/or quality of life, (5) results in congenital anomaly/birth defect or (6) any other serious or important event that may jeopardise the participant and may require medical or surgical intervention (treatment) to prevent one of the other outcomes.

All AEs and SAEs will be followed until: (1) AE is resolved, (2) AE is declared clinically insignificant, (3) AE has stabilised, (4) participant is lost to follow-up or withdraws consent, (5) participant completes study, including required follow-up visits or (6) study closure.

MyndTec Inc shall reimburse all reasonable and necessary expenses incurred for medical care received by study participants, including hospitalisation, in the treatment of any injury or illness sustained by a clinical trial participant as a result of receiving treatment with MyndMove therapy in the study.

Outcomes

Primary outcome

The primary outcome for the study is the change in SCIM-SC between baseline and end of treatment (14 weeks). This is the basis for the a priori sample size and sensitivity estimates. The SCIM is a disability scale that has been specifically developed to evaluate the functional outcomes of people with traumatic and non-traumatic SCI.28

Secondary outcomes

Additional secondary analyses of the SCIM self-care and mobility subscales will be performed at the interim, end-of-treatment assessment and end-of-study assessments (see table 2 schedule of assessments). The GRASSP test29–31 is a multimodality test designed to assess the integration of sensorimotor hand and upper limb impairment and function. The baseline scores for each of the GRASSP subscales will be compared with the scores at interim, end-of-treatment assessment and end-of-study assessment. The TRI-HFT32 was developed to evaluate improvements in the gross motor function of the unilateral grasp due to FES for reaching and grasping treatment. The baseline scores for each of the TRI-HFT subscales will be compared with the scores at the end-of-treatment assessment and end-of-study assessments. The SCI-QOL measurement system is a multifaceted system of measuring participants reported outcomes across a wide variety of functioning specifically targeted for individuals with SCI.33 Participants will complete 9 out of 22 areas of measure in the SCI-QOL (table 3). The baseline scores for each of the SCI-QOL subscales will be compared with the scores at the end-of-treatment assessment and end-of-study assessment. A healthcare resource utilisation questionnaire to capture inpatient, outpatient and community-based rehabilitation and healthcare services during the follow-up period will also be collected. The total number of minutes used from baseline to the end-of-study assessment will be compared between groups. Participants will be asked to complete an end-of-therapy questionnaire that consists of three open-ended questions to understand their acceptance and impression of the therapy they received in the trial. See table 3 for the analysis plan for each secondary outcome.

Table 3

Summary of the analysis for each objective, outcome and corresponding hypothesis

Variable/outcome	Hypothesis	Outcome measure (type of outcome)	Methods of analysis
1. Primary Upper extremity function.	FES intervention (I) is better than conventional therapy control (C).	SCIM-SC subscale score.	ANCOVA.
2. Secondary Limb function.	I is better than C.	SCIM mobility subscale score.	ANCOVA.
Upper limb function.	I is better than C.	GRASSP subscales:Strength total score.Sensibility total score.Qualitative prehension total score.Quantitative prehension total score.	ANCOVA.
Upper limb function.	I is better than C.	TRI-HFT subscales:Object manipulation score.Wooden block score.Cylinder torque.Credit card force.Wooden bar displacement length.	ANCOVA.
QoL.	I is better than C.	SCI-QOL subscales:Basic mobility score.Fine motor score.Manual wheelchair score.Power wheelchair score.Self-care score.Independence score.Pain behaviour score.Pain interference score.Satisfaction with social roles and activities score.	ANCOVA.
Safety.	I is better than C.	Serious and non-serious adverse events, total number of each per group.	Descriptive.
Healthcare resource utilisation.	Reduced healthcare resource utilisation with I compared with C.	Healthcare resource utilisation questionnaire, total number of minutes.	ANCOVA.
3. Sensitivity analyses: Per-protocol. Missing data based imputed based on LOCF. Adjusted analysis with key baseline characteristics: age, baseline function and QoL.	Results of analysis of primary analysis will remain robust.	SCIM-SC score.	ANCOVA with multivariable analysis for adjusted analysis.
Important remarks: In all analyses, results will be expressed as coefficient, SEs, corresponding 95% and associated p values. Goodness-of-fit will be assessed by examining the residuals for model assumptions and χ2 test of goodness-of-fit.

ANCOVA, analysis of covariance; C, control; FES, functional electrical stimulation; GRASSP, Graded Redefined Assessment of Strength, Sensibility and Prehension; I, intervention; LOCF, last observation carried forward; QOL, quality of life; SCIM, Spinal Cord Independence Measure III; SCIM-SC, Spinal Cord Independence Measure III self-care sub-scale; SCI-QOL, Spinal Cord Injury-Quality of Life; TRI-HFT, Toronto Rehab Institute Hand Function Test.

Participant and disease characteristics (demographics and SCI info)

The following participant characteristics will be captured: AIS grade and neurological level, concomitant medications, biological sex, age, race, ethnicity, marital status, number of members in household, years of education, primary occupation, family income range, handedness, international SCI upper extremity basic data set, general medical history, cause of SCI, current medical complications related to SCI, surgical history, current medical symptoms, smoking status and alcohol consumption.

Data analysis plan

The analysis and reporting of the results with follow the Consolidated Standards of Reporting Trials guideline (www.consort-statement.org). The statistician/data analyst will be blinded to the study group. The process of participant selection and flow throughout the study will be summarised using a flow diagram. The analysis results of participant demographics and baseline outcome variables (both primary and secondary) will be summarised using descriptive summary measures: expressed as mean (SD) or median (IQR) for continuous variables and number (per cent) for categorical variables. We will adopt an intention-to-treat principle to analyse all outcomes. We will also use multiple imputation to handle missing outcome data.34 Research has shown that this is the most optimal strategy for handling missing outcome data in trials under the assumption of missing at random.35 All statistical tests will be performed using two-sided tests at the 0.05 level of significance. The overall level of significance will not be adjusted for multiple testing for secondary outcomes because these are exploratory. We will use ANCOVA for the analyses of both primary and secondary outcomes, with treatment group as an independent variable and baseline values of each outcome as a covariate. For all models, the results will be expressed as mean difference, corresponding two-sided 95% CIs and associated p values. P values will be reported to three decimal places with values less than 0.001 reported as <0.001. We will conduct some sensitivity analyses to assess the robustness of the results: (1) per-protocol analysis: this analysis will be based only on participants with complete data that completed study procedures as per-protocol; (2) using last observation carried forward (LOCF) for missing data: this analysis will use the LOCF to impute missing data; (3) adjusted analysis: this analysis will adjust for some baseline variables that we think may impact the results if not balanced. These include age, time postinjury, baseline function, baseline quality of life and, potentially, site. To the extent that these sensitivity analyses yield similar results to the main analysis, inferences about the primary outcome will be strengthened.36 37 Goodness-of-fit will be assessed by examining the residuals for model assumptions and χ2 test of goodness-of-fit. Please see table 3 for a summary of the analysis for each objective, outcome and corresponding hypothesis. All analyses will be performed using SAS V.9.2.

Patient and public involvement

Patients were not involved in the design of this protocol. Collaborations will be developed with SCI community organisations to codevelop lay descriptions of the results of the trial for the public.

Ethics and dissemination

The study design is described according to the Standard Protocol Items: Recommendations for Interventional Trials reporting guidelines.38 This study has ethics approval from: MetroHealth System Institutional Review Board (IRB18-0751); University Health Network Research Ethics Board (REB17-6029); University of Texas Health Science Center IRB (HSC-MS-18–0862); Advarra IRB for HealthTech Connex Centre for Neurology Studies (Pro00030094); as well as approval from the US Army Medical Research and Materiel Command, Office of Research Protections and Human Research Protection Office. Any changes to the protocol will not be implemented until ethics approvals have been obtained. Amendments will be numbered in a sequential manner and assigned an amendment date and version.

Data collected as a part of the study will be maintained at Biostatistics Unit on behalf of the investigators. The initial evaluation of the clinical study results will be provided to the investigators and to MyndTec Inc. MyndTec Inc will not prevent publication of the results regardless of the outcome of the study. Dissemination of the results of the study will be made at peer-reviewed academic meetings and through peer-reviewed medical journals. Participant confidentiality will be maintained in all analyses and presentations.