Cerebral Palsy Clinical Trial
Official title:
Enhancing Developmental Motor Plasticity After Perinatal Stroke With Transcranial Direct Current Stimulation
The purpose of this study is to test tDCS (transcranial direct current stimulation), a type
of non-invasive brain stimulation, to determine whether it can improve motor function in
children with perinatal stroke and hemiparesis. Children 6-18 years with imaging-confirmed
perinatal stroke and functional motor impairment will be recruited. Children will be
randomized (1:1) to receive sham or tDCS (20 minutes daily) during daily intensive,
goal-directed motor learning therapy (90 minutes). Motor outcomes will be repeated at
baseline, 1 week, and 2 months.
Aim 1: Establish the ability of tDCS to safely enhance motor learning in children with
perinatal stroke.
Hypothesis 1: tDCS is safe and well tolerated in children.
Hypothesis 2: Contralesional, cathodal tDCS increases motor functional gains measured by AHA
at 2 months in children with perinatal stroke.
Methods details not included elsewhere
Study: Randomized, sham-controlled, double blind, phase II clinical trial.
Patient Population. All children will be recruited through the Alberta Perinatal Stroke
Project (APSP); a large population-based perinatal stroke research cohort based at Alberta
Children's Hospital and directed by the PI. Prospective APSP ascertainment since 2007 is
combined with retrospective enrolment (1992-2007) with comprehensive International
Classification of Disease codes (ICD-9, ICD-10)237 and institutional databases. These are
fully characterized patients with confirmed diagnosis by modern neuroimaging assessed in
person in standardized APSP clinics. Recruitment will occur randomly from the population of
all children meeting the criteria below.
Inclusion/exclusion criteria - see below
Data Collection and Management. Candidate APSP families will be contacted with review of
consent/assent forms. Families residing outside Calgary will have equal opportunity to
participate through existing APSP support systems. All complimentary data from existing
studies is extractable from the APSP database (demographics, imaging, risk factors,
outcomes).13 Neuroimaging data will be managed through the ACH Pediatric Neuroimaging
Laboratory according to institutional protocols. Neurophysiology data will be collected at
the ACH Pediatric TMS Laboratory and securely stored centrally.107 The institutional
Clinical Research Unit is a database management unit designed for clinical research and
currently houses all APSP studies and trials. The research database platform encompasses
data capture utilities, management tools, and security measures (Health Canada-compliant).
Methods will adhere to the CONSORT guidelines and the study will be registered prior to
consent of the first patient (www.clinicaltrials.gov).
Intensive Motor Learning (all subjects). An evidence-based approach to upper extremity motor
learning therapy in children with hemiparetic CP will be employed. Protocols have been
designed by expert pediatric neurorehabilitation and occupational therapy co-investigators
based on best available evidence. All children will participate in the same child-centered,
age-appropriate, goal-directed, peer supported motor learning program. Designed as an "after
school program" to optimize efficiency, children will attend our hospital for 10 consecutive
weekdays over 2 weeks. Each session begins with a 30 minute social snack activity, providing
the opportunity for peer social interactions and "recharging" from the school day while
engaging their affected extremity in functional activity. Each subject then enters 90
minutes of goal-directed (see COPM in outcome measures) motor learning therapy with an
individualized occupational therapist.
Week 1 will employ constraint induced movement therapy (CIMT) according to current practice
guidelines. Each child will be custom fit with a removable, bivalved cast that will be worn
throughout all therapy sessions. Week 2 will transition to intensive bimanual therapy to
integrate gains into more practical bimanual functions. Intensive bimanual therapies are now
evidence-based, safe, valid, and effective motor learning strategies in children with
hemiparetic CP. Efficacy appears equal to CIMT but the absence of constraint facilitates
functional bimanual motor learning and removes the complications of casting. Bimanual tasks
will be graded and selected according to relative function with increasing complexity across
the relevant spectrum (e.g. passive assist to active manipulator). Tasks will be both
symmetrical and asymmetrical, geared to age-appropriate activities of daily living and
individual interests, and include active patient participation. Following the acute 10 day
intervention, all children receive a structured home program based on the same principles
with ongoing therapist support, surveillance, and documentation for 2 months.
Randomization and blinding. Children will be randomized 1:1 to tDCS or sham. The study
statistician will perform the randomization based on study number only, being blinded to all
subject details. Allocation will then be communicated to the study PI and tDCS
neurophysiologist only. The subject, parents, measuring and treating occupational
therapists, and all other study members will be blinded to treatment allocation. The
neurophysiologist will then program each subjects tDCS unit accordingly. All will experience
identical ramp-up of current to 1mA over 30 seconds and maintained stimulation for 120
seconds. Those randomized to treatment will have the same current maintained for 20 minutes
during therapy. The tDCS units of those randomized to sham will automatically ramp-down
gradually to off over 60 seconds following the initial 120 seconds of stimulation. These
sham procedures are well validated in adult tDCS trials. Blinding effectiveness will be
evaluated.
Intervention: TDCS - see below.
Outcome measures - see below
Interim Safety Analysis. Any possible major side effects will be immediately reported to the
IRB per policy. Minor side effects will be tracked by the safety outcomes specified. An
interim safety analysis will be performed after the first 2 camps (12 subjects) to ensure no
decrease in hand function has occurred in association with contralesional tDCS. This will be
evaluated by comparing change in affected (AHA, MA) and unaffected (GS, PS, BB) hands at
both 1 week and 2 months between tDCS and sham populations.
Sample Size. Variables were extrapolated from the most relevant literature, our previous
studies in the same population, and personal communication with AHA creators. Smallest
detectable difference for the AHA is estimated at 0.97 logit units or approximately 5
logit-based AHA units. Our previous trial in the same population found the proportion
achieving this change was approximately 25% with CIMT alone compared to 65% receiving both
CIMT and contralesional brain stimulation (rTMS). Therefore, for the primary hypothesis that
tDCS improves AHA gains at 2 months, significance level alpha=0.05, power of 90%, and no
drop-outs (100% completion in previous trials), 24 patients (12 per group) will be required.
This is comparable or larger than most pediatric CP trials and positive tDCS and rTMS adult
stroke trials.
Statistical Analysis. Co-investigator expertise in statistical methods (AN) and clinical
trial methodology (MH) are established. Primary analysis will examine change in AHA and
other outcome variables from baseline to final outcome at 2 months using simple ANOVA.
Secondary analysis will explore effects of time and severity using repeated measures ANCOVA
with deficit severity as a covariable to examine interactions across treatment groups (tDCS,
sham). Safety outcomes will compare changes in unaffected hand function (as above), adverse
event rates (tDCS vs sham) using Chi-square/Fisher exact and Mann-Whitney tests. Association
between treatment group and subject's estimation of treatment received will be determined to
evaluate sham effectiveness (Chi-square/Fisher exact). The sample is not large enough for
multivariable modelling. Analysis will be intention-to treat.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Double Blind (Subject, Caregiver, Outcomes Assessor), Primary Purpose: Treatment
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