Attention Deficit Hyperactivity Disorder Clinical Trial
— ADHDOfficial title:
An Open-label, Flexible Dose, Single Site Study Evaluating the Safety, Efficacy and Tolerability of Cariprazine as an Adjunct to Psychostimulants in Adult Patients With ADHD Who Have Had an Inadequate Response to Psychostimulants Alone
According to the Canadian ADHD Practice Guidelines, psychostimulants are the preferred treatment of attention-deficit/hyperactivity disorder (ADHD), especially for those that require urgent care. Specifically, long-acting psychostimulants are considered the gold-standard pharmacological treatment for ADHD. Using extended-release formulations, long-acting psychostimulants provide an extended duration of daily symptom relief in addition to overall reductions in ADHD symptoms that are maintained over time. In accordance with these guidelines, clinicians may combine psychostimulants with other medications when it is considered necessary. For complex cases, psychostimulants alone are often inadequate for improving the effects of ADHD and are therefore prescribed in conjunction with other medications. At low doses, antipsychotics have been considered appropriate adjunctive medications. Studies show that most adult cases with ADHD that were undiagnosed or untreated in childhood result in the need for adjunctive medication in adulthood to enhance the effects of the psychostimulant. As a result, it is hypothesized that adjunct treatment with a low dose of cariprazine, an atypical antipsychotic, will enhance the effectiveness of standard ADHD treatment with a long-acting psychostimulant in a subset of the ADHD population that achieved little to no response on psychostimulants alone.
Status | Recruiting |
Enrollment | 15 |
Est. completion date | April 14, 2023 |
Est. primary completion date | December 30, 2022 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years to 70 Years |
Eligibility | Inclusion Criteria: 1. The participant has provided signed informed consent. 2. Males and/or females aged 18-70 (extremes included). 3. Participants with a primary diagnosis of ADHD according to DSM-5 (314.01) criteria (diagnosis to be made using the Mini-International Neuropsychiatric Interview (MINI) 7.0.2 and confirmed by the Diagnostic Interview for ADHD in Adults (DIVA 5.0). Participants with a comorbid anxiety and depressive disorder will be permitted, as long as ADHD is judged to be the primary diagnosis. 4. Participants who score an ASRS of = 4 in Part A at both Screening and Baseline, representing non-response to current stable psychostimulant treatment 5. Participants are on a stable dose (> 4 weeks) of their existing long-acting psychostimulant (any type) prior to entry into the study. 6. Participants are on a stable dose of any other psychotropic medication (> 8 weeks) to treat comorbid conditions, except antipsychotics. 7. On the basis of a physical examination, medical history and basic laboratory screening, the patient is, in the investigator's opinion, in a suitable condition. Basic laboratory screening includes: Chemistry: Electrolytes, ALT, Albumin, Alkaline Phosphatase, AST, Bilirubin Total protein, Creatinine, Urea (BUN), CK, GGT, Potassium, Sodium, Calcium, Glucose (Fasting), Bilirubin Direct, Bicarbonate, Chloride, Urate (for Uric Acid), LD, Magnesium, Phosphorus, Amylase CBC: Hematocrit, Hemoglobin, RBC, WBC + differential, abs. Platelet Count Drug Screen (urine-8 tests): amphetamines, benzodiazepines, barbiturates, methadone, cocaine, opiates, cannabinoids, PCP Standard Urinalysis Lipid Assessment: Cholesterol, HDL, LDL-calc, Triglycerides Prolactin 8. Willing and able to attend study appointments in the correct time windows. Exclusion Criteria: Participants meeting one or more of the following criteria cannot be selected for inclusion: 1. Any other primary mental health disorder in the previous six months. 2. Alcohol or drug abuse as defined in the DSM-5 criteria within the last six months. 3. Mania, hypomania as defined in the DSM-5 criteria. 4. Any psychotic disorder. 5. Eating disorders as defined in the DSM-5 criteria. 6. Any cognitive disorder or dementia within 3 months before the baseline visit. 7. A history of Seizure Disorder (Epilepsy or other). 8. Clinical interpretation of apparent suicide risk. 9. Commencement of formal psychotherapy for 4 weeks prior to entry into the study and/or during the course of the study. 10. Existing treatment with any antipsychotic as mono- or adjunct therapy at the time of the study. 11. Change in use of medications. 12. Laboratory values at screening or in medical history that may be considered through clinical interpretation to be significant, including positive drug and alcohol tests. 13. Diseases that could through clinical interpretation interfere with the assessments of safety, tolerability and efficacy of study treatment. 14. Serious illness: liver or renal insufficiency, cardiac, vascular, pulmonary, gastrointestinal, endocrine, neurological, infectious, neoplastic or metabolic disturbance. 15. If female, the subject is pregnant or lactating or intending to become pregnant before, during, or within 30 days after participating in this study, or intending to donate ova during such time period. 16. The participant has received electroconvulsive therapy, vagal nerve stimulation, or repetitive transcranial magnetic stimulation within 6 months prior to Screening. 17. The participant is, in the opinion of the investigator, unlikely to be able to comply with the clinical trial protocol or is unsuitable for any other reasons. 18. Contraindications and Warning Precautions as per the U.S. Product Monograph will be followed. Participants must discontinue the use of recreational drugs including cannabis for at least 2 weeks prior to entry into the study. Participants must limit alcohol intake to a maximum of 3 standard drinks per week during the study period. |
Country | Name | City | State |
---|---|---|---|
Canada | START Clinic for Mood and Anxiety Disorders | Toronto | Ontario |
Lead Sponsor | Collaborator |
---|---|
Dr. Martin A. Katzman |
Canada,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Mean changes in the ADHD Rating Scale (ADHD RS-5) | Remission cut off score is defined as less than or equal to 18 | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Barkley Adult ADHD Rating Scale IV (BAARS-IV) | Where response rate is defined at 50 percent improvement in symptoms | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Adult ADHD Self-Report Scale (ASRS) v1.1 | Where remission is greater than 14 | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Intolerance of Uncertainty Scale (IUS) | self-report measure of intolerance of uncertainty, where lower scores indicate greater capacity to tolerate ambiguity | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Clinical Global Impression - Severity (CGI-S) scale | where response rate is measured as 50 percent improvement on the CGI-S | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes in on the Time Sensitive ADHD Symptom Scale (TASS) | self-report inventory assessing severity of ADHD symptoms throughout the day | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Fawcett-Clark Pleasure Capacity Scale (FCPS) | Self-report inventory assessing anhedonia or hedonic tone | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the cognitive battery | Cambridge Health Sciences neuropsychological assessment battery including memory, reasoning, verbal ability, and concentration tasks | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Snaith-Hamilton Pleasure Scale (SHAPS) | Self-report inventory assessing anhedonia or hedonic tone | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Dimensional Anhedonia Rating Scale (DARS) | Self-report inventory assessing anhedonia | Pre treatment (screening, week 0) and post treatment (week 8) | |
Secondary | Mean changes on the Motivation and Energy Inventory (MEI) | self-report inventory assessing motivation and energy as a proxy measure for hedonic capacity | Pre treatment (screening, week 0) and post treatment (week 8) |
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