Brain Connectivity in Attention Deficit Hyperactivity Disorder (ADHD)

Overview

This study investigates whether a relationship exists between pre-treatment brain characteristics and treatment response in adults with Attention Deficit Hyperactivity Disorder (ADHD).

Full Title of Study: “Brain Connectivity in Attention Deficit Hyperactivity Disorder (ADHD): a Biomarker to Predict Treatment Response”

Study Type

  • Study Type: Interventional
  • Study Design
    • Allocation: Non-Randomized
    • Intervention Model: Crossover Assignment
    • Primary Purpose: Other
    • Masking: Single (Participant)
  • Study Primary Completion Date: January 15, 2015

Detailed Description

There is a pressing need in psychiatry to offer more individualised treatments, and to improve outcomes from clinical trials. This 'individualised medicine' approach requires the development of biomarkers of treatment response. 60 adults with ADHD are recruited from the Adult ADHD Clinic at the Maudsley Hospital, London, United Kingdom. The study is developed over three sessions, two at baseline (DAY 1 and DAY 2) and one after two months of treatment (follow-up). The first two sessions are conceived as a single-blind non-randomised placebo-controlled cross-over experiment. The first 30 participants enrolled in the study receive a placebo tablet (ascorbic acid 50 mgs) on DAY 1 before the behavioural assessment and magnetic resonance imaging (MRI) scan. The behavioural assessment and the functional MRI measurements are repeated two days after (DAY 2), under a clinically effective dose (20 mgs) of short-acting methylphenidate (MPH). The order of the tablets is reverted for the remaining 30 participants to balance any potential expectation and practice effect between the two conditions. Placebo and medication are over-encapsulated with the same red opaque capsules by the pharmacy team. Also, the protocol followed during the two sessions is absolutely identical in respect of timing and tests administered in order to keep the participants blind to the drug condition (medication or placebo). After the scanning sessions, all the participants receive the same prescription of a long-acting formulation of MPH, according to the clinical guidelines adopted by the Maudsley Hospital. Treatment response is evaluated clinically and behaviourally after 2 months of treatment (follow-up). Pre-treatment brain characteristics are tested as potential predictors (biomarkers) of treatment response.

Interventions

  • Drug: MPH
    • Participants undergo behavioural tests and brain scanning twice, once under placebo and once under an acute dose of MPH, before starting long-term treatment with a long-acting formulation of MPH used routinely at the Adult ADHD Clinic.

Arms, Groups and Cohorts

  • Experimental: Placebo, MPH
    • Dose order: placebo, methylphenidate (MPH) Participants receive a placebo tablet (ascorbic acid 50 mgs) on DAY 1 and a clinically effective dose of short-acting MPH (20 mgs) on DAY 2.
  • Experimental: MPH, Placebo
    • Dose order: methylphenidate (MPH), placebo Participants receive a clinically effective dose of short-acting MPH (20 mgs) on DAY 1 and a placebo tablet (ascorbic acid 50 mgs) on DAY 2.

Clinical Trial Outcome Measures

Primary Measures

  • Diffusion imaging-based measurements as statistically significant predictors of treatment response (i.e. of participants’ performance on adult ADHD rating scale at follow-up as compared to baseline).
    • Time Frame: In the month 2-3 following the last scan.
    • Diffusion based measurements include specific measures of anatomical connectivity of pathways originating in the frontal lobes, such as the fronto-striatal pathways and the superior longitudinal fasciculus. According to previously published criteria, treatment response is defined as a symptomatic improvement of at least 30%, as measured by participants’ performance on adult ADHD rating scale at follow-up as compared to baseline.

Secondary Measures

  • Functional connectivity measurements as statistically significant predictors of treatment response (i.e. of participants’ performance on adult ADHD rating scale at follow-up as compared to baseline).
    • Time Frame: In the month 4-5 following the last scan.
    • Functional connectivity measurements include the strength of functional connectivity along pathways originating in the frontal lobes, such as the fronto-striatal pathways and the attentive networks. Treatment response is defined as in outcome 1.
  • Diffusion imaging-based measurements as statistically significant predictors of treatment response defined by a data-driven approach.
    • Time Frame: In the month 6-7 following the last scan.
    • A categorical approach (data-driven analysis using multivariate k-mean clustering) is used to define treatment response on the basis of clinical and behavioural characteristics at follow-up. Clinical characteristics include participants’ performance on adult ADHD rating scale at follow-up as compared to baseline, whereas behavioural characteristics include participants’ performance on the Qb test at follow-up as compared to baseline.
  • Functional connectivity measurements as statistically significant predictors of treatment response as defined by a data-driven approach.
    • Time Frame: In the month 8-9 following the last scan.
    • Treatment response is defined as in outcome 3.

Participating in This Clinical Trial

Inclusion Criteria

  • males – aged 18-45 years old – intelligent quotient (IQ) > 70 (as measured by WASI) – diagnosis of ADHD confirmed through clinical assessment (Adult ADHD Clinic) – non-medicated (stimulant medication-naive or not taking stimulant medication for at least 4 weeks) Exclusion Criteria:

  • no other brain disorders other than ADHD – no condition precluding MRI scanning (e.g., metallic implants, claustrophobia)

Gender Eligibility: Male

Minimum Age: 18 Years

Maximum Age: 45 Years

Are Healthy Volunteers Accepted: No

Investigator Details

  • Lead Sponsor
    • King’s College London
  • Collaborator
    • Shire
  • Provider of Information About this Clinical Study
    • Sponsor
  • Overall Official(s)
    • Declan Murphy, MD, PhD, Study Director, King’s College London

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