Trial of Enhanced Neurostimulation for Anorexia

Not Applicable

Recruiting

• Conditions: Anorexia Nervosa

• Registration Number: NCT05788042
• Lead Sponsor: The George Institute

Brief Summary

Preliminary open-label studies have suggested that non-invasive brain stimulation methods of both transcranial direct current stimulation (tDCS) and repetitive transcranial magnetic stimulation (rTMS) have clinical benefits for improving psychological and eating disorder related symptoms, which can persist at long-term follow ups after acute treatment (i.e., at 6 and 12 months).

Here the investigators propose to conduct the first double-blinded, randomised sham-controlled study to directly compare the therapeutic effectiveness and acceptability of both treatment modalities.

Participants will be recruited and treated at one inpatient setting (Northside Clinic, St Leonards, Sydney). This facility is one of the largest specialist eating disorder settings in Australia with approximately 130 new admissions every year (2019 data). All participants who give consent and who fulfill the eligibility criteria will be randomised to receive active tDCS, sham (placebo) tDCS, active rTMS or sham rTMS over 8 weeks. Trial participants, their treating psychiatrist, ward staff, and a study staff member (who will conduct blinded assessments of mood secondary outcome measures) will be blinded after assignment to intervention until the database is locked and the primary analysis completed. All participants will complete assessments of eating disorder symptoms, mood, psychological symptoms, neurocognition and functioning at baseline, end of week 4, 8 and 20.

Expected outcomes include data on the relative effectiveness and acceptability for both treatment modalities in the inpatient and at-home setting (i.e., for at-home tDCS). The investigators expect that both active treatment arms will produce clinical benefits and have high acceptability, and that clinical benefits will be maintained with long-term at-home tDCS continuation treatment. These outcomes have potential to assist in reducing hospital stay and emergency re-admissions and improving day to day functioning in participants. Health economic data for both treatment modalities will additionally have utility from a service perspective, given the disparity in resource requirements between the two treatments (TMS, tDCS) in terms of costs for patients and access to treatment for people living in remote and rural areas (i.e., for at-home tDCS).

Detailed Description

Not available

Study Timeline

• Study First Submitted: 2023-02-21
• Study First Submitted QC: 2023-03-15
• Study First Posted: 2023-03-28
• Status Verified: 2023-08
• Study Start: 2023-08-02
• Last Update Submitted: 2023-08-02
• Last Update Posted: 2023-08-07
• Primary Completion: 2025-04-01
• Study Completion: 2025-07-01

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 70

Inclusion Criteria

• Aged ≥16 years,
• A current Diagnostic and Statistical Manual of Mental Disorders (5th edition DSM-5) diagnosis of anorexia nervosa
• Willing and able to participate and comply with study requirements
• Worked or studied in a context requiring some proficiency in spoken English (to ensure validity of neuropsychological testing)
• Under ongoing care by his/her own treating psychiatrist (to ensure patient safety during the study)

Exclusion Criteria

• Inability to provide informed consent
• Contraindications to tDCS/rTMS
• Failed to respond to an adequate course or rTMS (4 weeks) within the current illness course
• Had ECT in the last 3 months
• MoCA score of <26
• Significant risk of significant self harm or suicide as assessed by study psychiatrist(s)
• Currently enrolled in another interventional clinical trial or using an investigational device/product

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Primary Outcome Measures

Name	Time	Method
Acceptability	8 weeks	Number of completed sessions for active tDCS and active rTMS in the acute 8 week RCT period.
Effectiveness - Eating Disorder Examination Questionnaire (EDE Q)	Change from baseline at 8 weeks	Self-report instrument that measures eating disorder behaviors and attitudes. Eating Disorder Examination Questionnaire; 28-items; rating scale 0 - 6; Higher scores on the global scale and subscales indicate more problematic eating behaviours and attitudes.

Secondary Outcome Measures

Name	Time	Method
Neurocognition - STROOP Colour Word Test (response inhibition).	Change from baseline at 20 weeks	The STROOP task assesses inhibitory control, which has been shown to be reduced in people with eating disorders.
Number of re-admissions as reported by clinical staff.	From date of randomization until the date of study completion, assessed up to 20 weeks.	Number of re-admissions as reported by clinical staff
Duration of inpatient hospital stay as recorded by clinical staff	Through study completion, an average of 20 weeks	Duration of inpatient hospital stay as recorded by clinical staff
Change in Circumplex Scales of Interpersonal Efficacy (CSIE-32)	Change from baseline at 20 weeks	Change in Circumplex Scales of Interpersonal Efficacy: 32-items; scale 0-10; Higher score indicate confidence that one can engage in variety of interpersonal behaviours.
Neurocognition - Trail Making Test parts A and B (TMT: attention and cognitive flexibility)	Change from baseline at 20 weeks	Deficits in set shifting has been found to be common in people with AN.
Neurocognition - Embedded Figures Test (EFT: field dependence vs independence).	Change from baseline at 20 weeks	This task assesses central coherence, or the degree of focus on details in processing information. Poor central coherence is a potential etiologic or maintaining factor for people with eating disorders.
Weight	Change from baseline at 20 weeks	Change in Body Mass Index. Weight status in AN is considered a key determinant of remission from illness.
Mood - Montgomery Asberg Depression Rating Score (MADRS)	Change from baseline at 20 weeks	Depressive symptomology is a common psychiatric comorbidity of AN and both tDCS and rTMS significantly improve mood symptoms. 10-items; rating scale 0- 6; Higher score indicates more severe depression.
Neurocognition - Wisconsin Card Sorting Test (WSCT: perseveration).	Change from baseline at 20 weeks	This task has been found to be sensitive to set shifting deficits in people with AN.
Psychological Symptoms - Depression Anxiety and Stress Scale (DASS-21)	Change from baseline at 20 weeks	Self reported questionnaire designed to measure the severity of a range of symptoms common to both Depression and Anxiety. 21-items; rating scale 0- 3; Higher scores on subscales indicate more severe depression, anxiety and stress.
Cost of psychology sessions	Through study completion, an average of 20 weeks	Cost of psychology sessions in $ AUD
Functioning - The Assessment of Quality of Life Instrument (AQoL-4D)	Change from baseline at 20 weeks	Measures quality of life for independent living, mental health, relationships, and senses. It as chosen as measures can be used for economic evaluation based on Quality Adjusted Life Years (QALYs). 12-items; scale 1-4; Higher score indicates lower health-related quality of life.
Total cost of costs of rTMS and tDCS administration	Through study completion, an average of 20 weeks	Total cost of costs of rTMS and tDCS administration
Number of psychology sessions	Through study completion, an average of 20 weeks	Number of psychology sessions

Trial Locations

Locations (1)

Northside Clinic; 🇦🇺 Sydney, New South Wales, Australia