Vitamin D as a Therapeutic Adjunct in the Stimulant Treatment of ADHD: a Proof-of-concept Tele-health Study of Stimulant-induced Improvement in Neurocognitive Functioning.

Study Description

Brief Summary

The purpose of this study is to assess vitamin D as a therapeutic adjunct in the stimulant treatment of ADHD.

Detailed Description

The specific aim of this study is to determine whether acute calcitriol (vitaminD) administration (compared to placebo) enhances the neurocognitive effects of of current stimulant medications as measured by tasks of vigilance/attention, spatial working memory, and reversal learning in individuals with (attention deficit hyperactivity disorder (ADHD) using a randomized, double-blind, placebo controlled, within-subject, two-day study design.

Primary Hypothesis: It is hypothesized that calcitriol (versus placebo) administration will enhance positive neurocognitive effects of current stimulant medications in individuals with ADHD.

Seconday (Exploratory) Hypothesis: It is hypothesized that calcitriol (versus placebo) administration alone will also enhance neurocognitive performance on tasks of attention/vigilance and/or spatial working memory.

Study Design

Outcome Measures

Primary Outcome Measures

1. Enhanced positive neurocognitive effects on the CPT-IP [Up to 5 hours]

   On the Continuous Performance Task (CPT-IP) subjects are shown a random sequence of different numbers and are instructed to press a button as quickly and accurately as possible upon detection of two identical pairs of numbers, and to withhold their response to any other sequence of letters. Outcomes will be measured by d prime.

2. Enhanced positive neurocognitive effects on the Spatial working memory task [Up to 5 hours]

   The spatial working memory task is a measure of working memory. As part of the task, stimuli will be projected onto the computer screen and target stimuli can be spatial locations, different visual stimuli, sound or text. Outcomes will be measured by percent correct.

3. Enhanced positive neurocognitive effects on the PRLT [Up to 5 hours]

   The Probabilistic Reversal Learning Task (PRLT) measures subjects' perseverative responding in the context of changing reward contingencies / cues. Outcomes will be measured by numbers of reversal achieved, total points, and error types.

Secondary Outcome Measures

1. Enhanced positive neurocognitive effects on the CPT-IP- hits [Up to 5 hours]

   Enhanced positive neurocognitive effects on the CPT-IP will be measured by counts of hits, false alarms, and random errors.

2. Enhanced positive neurocognitive effects on the CPT-IP- false alarms [Up to 5 hours]

   Enhanced positive neurocognitive effects on the CPT-IP will be measured by counts of hits, false alarms, and random errors.

3. Enhanced positive neurocognitive effects on the CPT-IP- random errors [Up to 5 hours]

   Enhanced positive neurocognitive effects on the CPT-IP will be measured by counts of hits, false alarms, and random errors.Enhanced positive neurocognitive effects on the CPT-IP will be measured by counts of hits, false alarms, and random errors.Enhanced positive neurocognitive effects on the CPT-IP will be measured by counts of hits, false alarms, and random errors.

4. Spatial working memory task- reaction time [Up to 5 hours]

   Enhanced positive neurocognitive effects be measured by reaction time on the spatial working memory task.

5. Enhanced positive neurocognitive effects on the PRLT - win-switch / lose-stay rate [Up to 5 hours]

   Enhanced positive neurocognitive effects on the PRLT will be measured by win-switch / lose-stay rate.

Eligibility Criteria

Criteria

Inclusion Criteria:

• Age 18-50 years

• Voluntary, written, informed consent

• Physically healthy by medical and psychiatric history

• DSM-5 diagnosis of ADHD

• Point of Care Test results for Vitamin D equal or higher than 20 ng/ml

• English speaking

Exclusion Criteria:

• Medical contraindication to calcitriol administration (e.g., history of hypersensitivity to calcitriol or any component of the formulation, hypercalcemia or vitamin D toxicity)

• History of substance dependence (e.g., alcohol, opiates, sedative hypnotics), except for nicotine

• A primary major DSM-V psychiatric disorder (e.g., schizophrenia, bipolar disorder, major depression, etc.) as determined by the Structured Clinical Interview for DSM-V (SCID), except ADHD

• A history of significant medical (e.g., cardiovascular, diabetic/metabolic) or neurological (e.g., cerebrovascular accidents, seizure, traumatic brain injury) illness

• Current use of psychotropic and/or potentially psychoactive prescription medications, except prescribed stimulants

• Use of any prescription medications and/or over-the-counter medications, vitamins (including vitamin D) and/or herbal supplements which could have a negative clinical interaction with calcitriol or which could confound scientific results of the study, within 2 weeks prior to each test day (e.g., thiazide diuretics, Mg based antiacids, digoxin, etc,).

• Levels of 25(OH)D3 below 20 ng/ml .

• History of kidney stones within the past 5 years

• History of renal failure

• History of parathyroid disorder (hyper or hypoparathyroidism)

• History of osteoporosis or any pathologic fractures

• Vitamin D supplementation in any form in the past 3 months

• Known hypersensitivity to calcitriol

• Malabsorption syndromes (i.e. Celiac sprue)

Contacts and Locations

Locations

Sponsors and Collaborators

• Yale University

Investigators

• Principal Investigator: Marc Potenza, MD, Yale University

Study Documents (Full-Text)

More Information

Publications