Pharmacogenetically-guided Escitalopram Treatment for Pediatric Anxiety: Aiming to Improve Safety and Efficacy (PrEcISE)
Overview
- Phase
- Phase 4
- Intervention
- Escitalopram
- Conditions
- Anxiety
- Sponsor
- University of Cincinnati
- Enrollment
- 132
- Locations
- 1
- Primary Endpoint
- Pediatric Anxiety Rating Scale severity score
- Status
- Recruiting
- Last Updated
- last year
Overview
Brief Summary
This double-blind, 12-week study will consist include132 anxious youth who are randomized (1:1) to standard or pharmacogenetically-guided escitalopram dosing. Block randomization (1:1) will be stratified by sex and metabolizer status.
Detailed Description
This randomized, controlled trial compares pharmacogenetically-guided and standard dosing of escitalopram in adolescents (12-17 years of age) with anxiety disorders. In this study, the investigators will examine these two dosing strategies in terms of efficacy (Aim 1) and tolerability (Aim 2). The investigators propose to recruit 132 adolescents (age 12-17 years, inclusive) with generalized, separation and/or social anxiety disorder (pediatric anxiety trial).1 This will allow investigators to evaluate whether pharmacogenetically-guided escitalopram dosing improves efficacy and tolerability in outpatient adolescents aged 12-17 years with anxiety disorders. Eligible patients will be randomized to: (1) standard escitalopram dosing or (2) pharmacogenetically-guided dosing for 12 weeks.
Investigators
Jeffrey Strawn, MD
Principal Investigator
University of Cincinnati
Eligibility Criteria
Inclusion Criteria
- •Written, informed assent and consent.
- •Patients, parent/guardian must be fluent in the English.
- •12 to 17 years of age, inclusive, at Visit
- •Patients must meet DSM-512 criteria for generalized, social and/or separation anxiety disorder, confirmed by the MINI-KID.
- •PARS score ≥15 at Visit 1 and Visit
- •No initiation of psychotherapy within 8 weeks of screening (Visit 1). Current therapy much be stable for ≥2 months prior to baseline (Visit 2).
- •Clinical Global Impressions-Severity (CGI-S) score ≥4 at Visits 1 \&
- •Caregiver who is willing to consent to be responsible for safety monitoring of the patient, provide information about the patient's condition, oversee the administration of the investigational product.
- •No clinically significant abnormalities on physical examination and EKG.
- •Negative pregnancy test at Visit 1 in females.
Exclusion Criteria
- •Co-occurring DSM-5 mood disorder (except persistent depressive disorder, unspecified depressive disorder, provided that the primary diagnosis is an anxiety disorder), eating, bipolar or psychotic disorders.
- •A lifetime diagnosis of an intellectual disability.
- •A significant history of trauma exposure.
- •A history of SSRI treatment within 12 weeks of baseline or current treatment with a medication with psychiatric effects that requires \>5 half-lives for washout History of non-response to \>2 SSRIs.
- •Allergy, intolerance, non-response or hypersensitivity to escitalopram. Major neurological or medical illness or head trauma with ≥5 minutes loss of consciousness.
- •Alcohol or substance use disorder within the past 6 months (nicotine use is permitted).
- •Psychotherapy initiated within 8 weeks of screening (Visit 1), or plans to initiate/change therapy during the study.
- •Pregnant, breastfeeding, lactating, and/or planning to become pregnant during the study or within 30 days following the end of study participation.
- •Positive urine pregnancy test.
- •A positive urine drug screen.
Arms & Interventions
Standard dosing
Patients randomized to standard dosing (std) will initiate escitalopram at 5 mg daily and will then increase to 20 mg/day at week 4.
Intervention: Escitalopram
Pharmacogenetically-guided escitalopram dosing
Patients randomized to PGx-guided treatment, escitalopram titration will be based on CYP2C19 phenotype and predicted escitalopram exposure. In poor metabolizers (PM), escitalopram will be initiated at 5 mg daily and increased to 10 mg daily at week 4.
Intervention: Escitalopram
Outcomes
Primary Outcomes
Pediatric Anxiety Rating Scale severity score
Time Frame: Baseline to Week 12/Early Termination
Change from Baseline in Pediatric Anxiety Rating Scale (PARS) severity score. The PARS is a clinician-rated instrument for assessing the severity of anxiety symptoms associated with common anxiety disorders in children and adolescents. The PARS score is derived by summing 5 of the 7 severity/impairment/interference items (2, 3, 5, 6, and 7)
Secondary Outcomes
- Tolerability-Activation(Baseline to Week 12/Early Termination)