Deep Brain Stimulation in Children With Autism

Not Applicable

Completed

• Conditions: Autism Spectrum Disorder; Self-Injurious Behavior
• Interventions: Procedure: Deep Brain Stimulation; Device: DBS

• Registration Number: NCT03982888
• Lead Sponsor: The Hospital for Sick Children

Brief Summary

The purpose of this study is to evaluate the safety and possible effectiveness of deep brain stimulation (DBS) of the nucleus accumbens in children with autism spectrum disorder and treatment-refractory, repetitive self-injurious behavior. Six (6) patients will be recruited and enrolled in this pilot study and study duration for each patient will be one (1) year. All will undergo surgical implantation of the Medtronic DBS system and will receive stimulation of the nucleus accumbens (2 electrodes per patient).This will be an open, non-blinded, non-randomized, pilot, phase I trial.Expected study duration is 36 months.

Detailed Description

This is a phase I, non-blinded, non-randomized, pilot trial for safety and efficacy of deep brain stimulation for medically-refractory, repetitive self-injurious behaviours in children with ASD (i.e. secondary stereotypies). The trial will be conducted in compliance with the protocol, GCP and the applicable regulatory requirement(s).

Patients who meet inclusion and exclusion criteria will be identified and recruited the Neurosurgical Clinic at The Hospital for Sick Children. The study will proceed according to the schedule laid out below, and both patients and treating team will be aware of all treatment parameters at all times. Six (6) subjects will be enrolled in this study and study duration for each patient will be one (1) year. Previous phase I trials of DBS in psychiatric and Alzheimer's Disease populations have utilized 6 subjects per surgical target. Such a number is sufficient to demonstrate initial safety, as well as feasibility and clinical effectiveness.

Study Timeline

• Study First Submitted: 2019-06-03
• Study First Submitted QC: 2019-06-11
• Study First Posted: 2019-06-12
• Study Start: 2019-08-14
• Primary Completion: 2024-01-01
• Study Completion: 2024-01-31
• Status Verified: 2024-02
• Last Update Submitted: 2024-02-20
• Last Update Posted: 2024-02-22

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 6

Inclusion Criteria

• Female or Male patients between age 7-18
• Diagnosis of Autism Spectrum Disorder (as defined by the DSM-5).
• Failure or non eligibility of medical therapy with ongoing repetitive self-injurious behaviours, at 6 months or more after instigation of therapy. Failure is defined as a lack of improvement in self-injurious behaviours, as documented by objective evidence, including caregiver logs or clinician assessment, if the clinician has documented a baseline status prior to instigation of the medical therapy.
• Diagnosis of secondary stereotypies, based on clinical assessment of the treating physicians with evidence of self-injury, documented in the patient records.
• Parents or legal guardians, including caregivers, informed and able to give written consent.
• Able to comply with all testing, follow-ups and study appointments and protocols for 12 months following the end of the duration of the study.

Exclusion Criteria

• Substance dependence or abuse in the last 6 months, excluding caffeine and nicotine
• Any contraindication to MRI or PET scanning
• Likely to relocate away from the study site or move during the study's one year duration
• Presence of cardiac arrhythmias, or other cardiac, respiratory, renal or endocrine conditions that will result in significant risk from a surgical procedure.
• Pregnancy
• Unable to communicate adequately in English in order to complete the baseline and follow-up questionnaires.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: SINGLE_GROUP

Arm && Interventions

Group	Intervention	Description
DBS Treatment	Deep Brain Stimulation	Deep brain stimulation of both limbic and dysfunctional reward processing circuits for treatment of repetitive self injurious behaviours in children with ASD
DBS Treatment	DBS	Deep brain stimulation of both limbic and dysfunctional reward processing circuits for treatment of repetitive self injurious behaviours in children with ASD

Primary Outcome Measures

Name	Time	Method
Changes in abberant behaviour	1 year	The Aberrant Behavior Checklist (Aman, Singh, Stewart \& Field, 1985) will be used to measure changes in the extent that abberant behaviour is a problem pre and post intervention. The scale is scored from 0-3 as follows: 0= not at all a problem; 1. the behaviour is a problem but slight in degree; 2. the problem is moderately serious; 3. the problem is severe in degree Where the higher number indicates the behaviour is problematic. Questions are scored and totaled.; Measure will be completed at baseline (pre-surgery), weekly from weeks 2-6 post-surgery, bi-weekly from weeks 7-10 post surgery, monthly from weeks 11-51 post-surgery, and 1 year post surgery.
Changes in self-injurious behaviour	1 year	The Inventory of Statements about Self-Injury (ISAS; Klonsky \& Olino, 2008) will be used to measure changes in self-injurious behaviour pre and post intervention. The scale is scored from 0-2 as follows: 0= not relevant; 1. somewhat relevant; 2. very relavant Where a higher number indicates increased self-injurious behaviour. Questions are scored and totaled.; Measure will be completed at baseline (pre-surgery), weekly from weeks 2-6 post-surgery, bi-weekly from weeks 7-10 post surgery, monthly from weeks 11-51 post-surgery, and 1 year post surgery.
Changes in obsessive-compulsive thoughts	1 year	The Yale-Brown Obsessive Compulsive Scale (Y-BOCS; Goodman, Price, Rasmussen,1989) will be used to measure changes in the amount of interference of unwanted ideas, images, or impulses pre and post intervention. The scale is scored from 0-4, where 0 represents minimal interference and 4 represents substantial interference. Questions are scored and totaled.; Measure will be completed at baseline (pre-surgery), weekly from weeks 2-6 post-surgery, bi-weekly from weeks 7-10 post surgery, monthly from weeks 11-51 post-surgery, and 1 year post surgery.
Changes in repetitive behaviour	1 year	The Repetitive Behavior Scale-Revised (RBS-R; Bodfish, Symons, Parker \& Lewis, 2000) will be used to measure changes in repetitive behaviour pre and post intervention. The following sub-scales will be used: * Steretyped behaviour subscale; * Self-injurious behaviour subscale; * Compulsive behaviour subscale; * Ritualistic behaviour subscale; * Sameness behaviour subscale; * Restricted behaviour subscale; All subscales are scored from 0-3 as follows: 0 = behaviour does not occur; 1. behaviour occurs and is a mild problem; 2. behaviour occurs and is a moderate problem; 3. behaviour occurs and is a severe problem Where a higher number indicates increased repetitive behaviour.; Subscores are totaled and then an overall score is calculated.; Measure will be completed at baseline (pre-surgery), weekly from weeks 2-6 post-surgery, bi-weekly from weeks 7-10 post surgery, monthly from weeks 11-51 post-surgery, and 1 year post surgery.
Changes in quality of life	1 year	The Paediatric Quality of Life Inventory (PedsQL v. 4.0) will be used to measure changes in self-reported quality of life pre and post intervention. The statements are scored from 0-4 as follows: 0= it is never a problem; 1 = it is almost never a problem 2= it is sometimes a problem 3 = it is often a problem 4= it is almost always a problem Where a higher score indicates the statement is a problem. All items are scored and totaled.; Measure will be completed at baseline (pre-surgery), weekly from weeks 2-6 post-surgery, bi-weekly from weeks 7-10 post surgery, monthly from weeks 11-51 post-surgery, and 1 year post surgery.

Secondary Outcome Measures

Name	Time	Method
Changes in physical brain abnormalities	1 year	MR images will be analyzed pre and post intervention for the following to assess physical abnormalities of the brain, including type (focal cortical dysplasia, tumor, hippocampal sclerosis, hypothalamic hamartoma, gliosis, brain atrophy), side of abnormalities (left/right/ bilateral), and location (frontal, temporal, sylvian, parietal, occipital, multilobar).; MRI data will be collected at baseline, 6 weeks post-surgery, and 1 year post-surgery.
Changes in metabolic brain abnormalities	1 year	FDG-PET scans will be analyzed to measure changes in neurometabolism pre and post intervention, specifically indications of hypermetabolism in the frontal lobes, hippocampus, and lentiform nucleus.; FDG-PET data will be collected at baseline, 6 weeks post-surgery, and 1 year post-surgery.
Type of adverse events reported in caregiver logs	1 year
Changes in activity	1 year	Changes in activity pre and post intervention will be measured using the Actiwatch Spectrum, Phillips Respironics, Bend, OR. Actigraphy is the continuous measurement of an individual's movement. Actigraph data will be collected at baseline, 6 weeks post-surgery, and 1 year post-surgery. Actigraph data will be analyzed using MATLAB (Mathworks, Natick, MA). Measures analyzed will be maximum and minimum value amplitudes, peak to peak, variance, entropy fast fourier transform, discrete cosine function, z-transform, bispectrum.
Changes in number of complications pre and post intervention will be compared.	1 year

Trial Locations

Locations (1)

The Hospital for Sick Children; 🇨🇦 Toronto, Ontario, Canada