An Open-Label Extension Study Assessing the Long-Term Safety and Efficacy of Viloxazine Extended-Release Capsules in Adults with Attention-Deficit/Hyperactivity Disorder.

An Open-Label Extension Study Assessing the Long-Term Safety and Efficacy of Viloxazine Extended-Release Capsules in Adults with Attention-Deficit/Hyperactivity Disorder.

Publication date: Oct 07, 2024

Viloxazine ER (extended-release capsules; Qelbree) is a nonstimulant medication that has been approved by the United States Food and Drug Administration (FDA) for treatment of attention-deficit/hyperactivity disorder (ADHD) in children (> 6 years old) and adults. This phase 3 open-label extension to a pivotal phase 3, double-blind trial evaluated the long-term safety and continued efficacy of viloxazine ER in adults with ADHD. This was a multicenter, flexible-dose, open-label extension to a phase III, double-blind, placebo-controlled trial (NCT04016779). Viloxazine ER was initiated at 200 mg/day and adjusted (between 200 and 600 mg/day) to achieve optimal efficacy and tolerability. Trial enrollment was halted temporarily (24 March 2020 to 23 July 2020) due to the coronavirus disease 2019 (COVID-19) pandemic. Participants completing double-blind treatment during that time were offered delayed enrollment upon trial requalification. Safety outcomes were the primary objectives. Secondary objectives were efficacy outcomes, including the ADHD Investigator Symptom Rating Scale (AISRS), and were assessed relative to double-blind baseline (or trial re-entry baseline for those whose enrollment was delayed by the COVID-19 pandemic). Overall, 159 participants (133 immediate and 26 delayed rollover) received viloxazine ER, with a mean exposure of 265 +/- 254. 9 days. Adverse events (AEs) included (> 10% incidence) insomnia (13. 8%), nausea (13. 8%), headache (10. 7%), and fatigue (10. 1%). AEs led to discontinuation for 17. 6% of participants [most commonly insomnia (2. 5%), nausea (2. 5%), and fatigue (1. 9%)]. AISRS total score [baseline mean +/- standard deviation (SD): 37. 9 +/- 6. 3] improved by the first follow-up visit (-11. 4 +/- 9. 5; week 2) with continued improvement at subsequent visits (last on-study visit: -18. 2 +/- 11. 54). Similar patterns of improvement were seen for other measures of efficacy, including quality of life and executive function. Following initial dose optimization, most participants (73%) used viloxazine ER doses ≥ 400 mg/day, with 36% using doses of 600 mg/day. Long-term viloxazine ER use was well tolerated, with no new long-term safety findings. Improvements in ADHD symptoms and associated measures were sustained throughout trial participation. In total, 73% percent of adult participants in this long-term study used viloxazine ER doses of 400 mg or more during maintenance treatment. Clinicaltrials. gov Identifier: NCT04143217.

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Concepts Keywords
Clinicaltrials Adhd
Coronavirus Blind
Food Day
July Double
Efficacy
Extension
Label
Long
Mg
Open
Participants
Safety
Term
Trial
Viloxazine

Semantics

Type Source Name
drug DRUGBANK Viloxazine
pathway REACTOME Release
disease MESH ADHD
disease MESH coronavirus disease 2019
disease IDO symptom
disease MESH insomnia
disease IDO quality
drug DRUGBANK Trestolone
disease MESH impulsivity
disease MESH educational achievements
drug DRUGBANK Coenzyme M
disease MESH depression
disease IDO history
drug DRUGBANK Epinephrine
drug DRUGBANK Atomoxetine
drug DRUGBANK Dopamine
drug DRUGBANK Reboxetine
disease MESH Suicide
disease MESH seizure
disease MESH syncope
disease MESH tic
disease MESH myoclonus
disease MESH muscle spasms
drug DRUGBANK Caffeine
pathway REACTOME Metabolism
disease IDO disposition
drug DRUGBANK Medical Cannabis
pathway REACTOME Vitamins
drug DRUGBANK Ibuprofen
drug DRUGBANK Acetaminophen
drug DRUGBANK Cetirizine
drug DRUGBANK Loratadine
drug DRUGBANK Diphenhydramine
drug DRUGBANK Pentaerythritol tetranitrate
drug DRUGBANK Methylphenidate
drug DRUGBANK Amphetamine
disease MESH deep vein thrombosis
disease MESH pulmonary embolism
disease MESH anxiety
disease MESH sinusitis
disease MESH irritable bowel syndrome
disease MESH somnolence
drug DRUGBANK Alkaline Phosphatase
disease IDO blood
disease MESH hypertension
drug DRUGBANK Sulpiride
disease MESH sleep disorder
disease MESH migraine
disease MESH aura
disease MESH tension headache
disease MESH Erectile dysfunction
disease MESH Upper respiratory tract infection
disease MESH nasopharyngitis
disease MESH pharyngitis
disease MESH Coronavirus infection
disease MESH Tachycardia
disease MESH Apathy
disease MESH Restlessness
disease MESH Urinary tract infection
disease MESH sinus arrhythmia
disease MESH arrhythmia
disease MESH weight gain
disease MESH suicidal ideation
disease MESH restless leg syndrome
drug DRUGBANK Methionine
disease MESH comorbidity
pathway KEGG Caffeine metabolism
disease MESH abnormalities
disease MESH weight loss
disease MESH uncertainty
disease IDO site
disease IDO production
drug DRUGBANK Tromethamine
drug DRUGBANK Efavirenz
pathway REACTOME Reproduction
disease MESH mental disorders
drug DRUGBANK L-Citrulline
drug DRUGBANK Serotonin
drug DRUGBANK Norepinephrine
drug DRUGBANK Lisdexamfetamine
drug DRUGBANK Modafinil
drug DRUGBANK Ranitidine
disease MESH Drug induced liver injury
disease MESH Kidney Diseases

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