Your search keyword '"Lisa Kamen"' showing total 5 results

1. Human Milk and Plasma Pharmacokinetics of Single-Dose Rimegepant 75 mg in Healthy Lactating Women

Author

Teresa E. Baker, Robert Croop, Lisa Kamen, Patty Price, David A. Stock, Andrea Ivans, Rajinder Bhardwaj, Matt S. Anderson, Jennifer Madonia, Joseph Stringfellow, Richard Bertz, Vladimir Coric, and Thomas W. Hale

Subjects

Adult, Adolescent, Milk, Human, Pyridines, Health Policy, Infant, Newborn, Infant, Obstetrics and Gynecology, Pediatrics, Young Adult, Breast Feeding, Piperidines, Maternity and Midwifery, Humans, Lactation, Female

Published

2022

2. Oral rimegepant for preventive treatment of migraine: a phase 2/3, randomised, double-blind, placebo-controlled trial

Author

David Kudrow, Lisa Kamen, Vladimir Coric, Charles M. Conway, Richard B. Lipton, Elyse Stock, David A. Stock, Peter J. Goadsby, and Robert Croop

Subjects

Adult, Male, medicine.medical_specialty, Pyridines, Migraine Disorders, Placebo-controlled study, Administration, Oral, 030204 cardiovascular system & hematology, Placebo, law.invention, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, Double-Blind Method, Piperidines, law, Calcitonin Gene-Related Peptide Receptor Antagonists, Internal medicine, medicine, Clinical endpoint, Humans, 030212 general & internal medicine, Adverse effect, business.industry, General Medicine, medicine.disease, Clinical trial, Treatment Outcome, Tolerability, Migraine, Drug Evaluation, Female, business

Abstract

Summary Background Rimegepant is a calcitonin gene-related peptide receptor antagonist that has shown efficacy and safety in the acute treatment of migraine. We aimed to compare the efficacy of rimegepant with placebo for preventive treatment of migraine. Methods We did a multicentre, phase 2/3, randomised, double-blind, placebo-controlled trial at 92 sites in the USA. Adults with at least a 1-year history of migraine were recruited. After a 4-week observation period, eligible participants were randomised using an interactive web response system to oral rimegepant 75 mg or matching placebo every other day for 12 weeks (double-blind treatment phase). The primary efficacy endpoint was change from the 4-week observation period in the mean number of migraine days per month in the last 4 weeks of the double-blind treatment phase (weeks 9–12). Participants who received at least one dose of their assigned study medication and who had 14 days or more of data in the observation period and 14 days or more of data for at least one 4-week interval during the double-blind treatment phase were analysed for efficacy. Those who received at least one dose of study medication were analysed for safety. This study is registered with ClinicalTrials.gov, NCT03732638. Findings Between Nov 14, 2018, and Aug 30, 2019, 1591 participants were recruited and assessed for eligibility, of whom 747 were randomly allocated either rimegepant (n=373) or placebo (n=374). 695 participants were included in the analysis for efficacy, of whom 348 were assigned rimegepant and 347 were allocated placebo. Rimegepant was superior to placebo on the primary endpoint of change in the mean number of migraine days per month during weeks 9–12. The change from the observation period in mean number of migraine days per month during weeks 9–12 was −4·3 days (95% CI –4·8 to –3·9) with rimegepant and −3·5 days (–4·0 to –3·0) with placebo (least squares mean difference −0·8 days, 95% CI −1·46 to −0·20; p=0·0099). 741 participants received study medication and were included in the safety analysis. 133 (36%) of 370 patients who received rimegepant reported an adverse event, compared with 133 (36%) of 371 who received placebo. Seven (2%) participants who received rimegepant and four (1%) who received placebo discontinued the study due to an adverse event; no patients died. Interpretation Taken every other day, rimegepant was effective for preventive treatment of migraine. Tolerability was similar to that of placebo, and no unexpected or serious safety issues were noted. Funding Biohaven Pharmaceuticals.

Published

2020

3. A Placebo-Controlled, Fixed-Dose Study of Aripiprazole in Children and Adolescents With Irritability Associated With Autistic Disorder

Author

William H. Carson, Lisa Kamen, Robert D. McQuade, Ronald N. Marcus, Michael G. Aman, Randall Owen, and George Manos

Subjects

Male, Pediatrics, medicine.medical_specialty, Adolescent, medicine.drug_class, Aripiprazole, Atypical antipsychotic, Child Behavior Disorders, Quinolones, Personality Assessment, Irritability, Placebo, Partial agonist, Drug Administration Schedule, Piperazines, law.invention, Double-Blind Method, Randomized controlled trial, law, Developmental and Educational Psychology, medicine, Adverse Drug Reaction Reporting Systems, Humans, Autistic Disorder, Child, Psychiatry, Psychomotor Agitation, Dose-Response Relationship, Drug, medicine.disease, Irritable Mood, Psychiatry and Mental health, Treatment Outcome, Tolerability, Autism, Female, medicine.symptom, Psychology, Self-Injurious Behavior, Antipsychotic Agents, medicine.drug

Abstract

To evaluate the short-term efficacy and safety of aripiprazole in the treatment of irritability in children and adolescents with autistic disorder.Two hundred eighteen children and adolescents (aged 6-17 years) with a diagnosis of autistic disorder, and with behaviors such as tantrums, aggression, self-injurious behavior, or a combination of these symptoms, were randomized 1:1:1:1 to aripiprazole (5, 10, or 15 mg/day) or placebo in this 8-week double-blind, randomized, placebo-controlled, parallel-group study. Efficacy was evaluated using the caregiver-rated Aberrant Behavior Checklist Irritability subscale (primary efficacy measure) and the clinician-rated Clinical Global Impressions-Improvement score. Safety and tolerability were also assessed.At week 8, all aripiprazole doses produced significantly greater improvement than placebo in mean Aberrant Behavior Checklist Irritability subscale scores (5 mg/day, -12.4; 10 mg/day, -13.2; 15 mg/day, -14.4; versus placebo, -8.4; all p.05). All aripiprazole doses demonstrated significantly greater improvements in mean Clinical Global Impressions-Improvement score than placebo at week 8. Discontinuation rates due to adverse events were as follows: placebo 7.7%, aripiprazole 5 mg/day 9.4%, 10 mg/day 13.6%, and 15 mg/day 7.4%. The most common adverse event leading to discontinuation was sedation. There were two serious adverse events: presyncope (5 mg/day) and aggression (10 mg/day). At week 8, mean weight change (last observation carried forward) was as follows: placebo +0.3 kg, aripiprazole 5 mg/day +1.3 kg, 10 mg/day +1.3 kg, and 15 mg/day +1.5 kg; all p.05 versus placebo.Aripiprazole was efficacious and generally safe and well tolerated in the treatment of children and adolescents with irritability associated with autistic disorder.

Published

2009

4. Aripiprazole in the treatment of irritability in pediatric patients (aged 6-17 years) with autistic disorder: results from a 52-week, open-label study

Author

Lisa Kamen, William H. Carson, Raymond Mankoski, Ronald N. Marcus, Patricia K. Corey-Lisle, George Manos, Michael G. Aman, Randall Owen, and Robert D. McQuade

Subjects

Male, Pediatrics, medicine.medical_specialty, Adolescent, Aripiprazole, Quinolones, Placebo, Irritability, Piperazines, law.invention, Open label study, Randomized controlled trial, law, medicine, Humans, Pharmacology (medical), Autistic Disorder, Psychiatry, Child, Psychiatric Status Rating Scales, Follow up studies, Irritable Mood, Clinical trial, Psychiatry and Mental health, Treatment Outcome, Tolerability, Pediatrics, Perinatology and Child Health, Female, medicine.symptom, Psychology, medicine.drug, Antipsychotic Agents, Follow-Up Studies

Abstract

To report the long-term efficacy of aripiprazole in the treatment of irritability in children and adolescents (ages 6-17 years) with autistic disorder.This was a 52-week, open-label, flexible-dose (2-15 mg/day) study of aripiprazole for the treatment of children and adolescents with irritability associated with autistic disorder. Eligible subjects were enrolled from two 8-week randomized trials or were enrolled as de novo subjects. "Prior aripiprazole" subjects had received treatment with aripiprazole for 8 weeks before entering this study. Evaluation of efficacy, a secondary objective after evaluation of safety and tolerability in this study, was conducted using the caregiver-rated Aberrant Behavior Checklist-Irritability subscale and the clinician-rated Clinical Global Impression-Improvement score.Three hundred thirty subjects received treatment (de novo, n = 86; prior aripiprazole, n = 174; prior placebo, n = 70) and 199 subjects (60.3%) completed 52 weeks of treatment. At their last study visit, 38.2% of subjects were receiving concomitant central nervous system medications (commonly antidepressants, 13.4%; psychostimulants, 11.5%; antiepileptics, 5.9%). At week 52 (observed cases data set), the mean change from baseline in Aberrant Behavior Checklist Irritability subscale scores was -8.0 in de novo subjects and -6.1 in prior placebo subjects; prior aripiprazole subjects maintained symptom improvement that was achieved with treatment in the prior study. At endpoint, the majority of subjects had a Clinical Global Impressions-Improvement score of 2 (much improved) or 1 (very much improved).Aripiprazole reduced symptoms of irritability associated with autistic disorder in pediatric subjects ages 6-17 years who were studied for up to 1 year.

Published

2011

5. Safety and tolerability of aripiprazole for irritability in pediatric patients with autistic disorder: a 52-week, open-label, multicenter study

Author

Raymond Mankoski, Ronald N. Marcus, Robert L. Findling, William H. Carson, Lisa Kamen, George Manos, Robert D. McQuade, and Randall Owen

Subjects

Male, medicine.medical_specialty, Psychomotor agitation, Adolescent, Aripiprazole, Quinolones, Irritability, Akathisia, Weight Gain, Piperazines, law.invention, Randomized controlled trial, Extrapyramidal symptoms, Basal Ganglia Diseases, law, Internal medicine, Medicine, Humans, Aspartate Aminotransferases, Autistic Disorder, Adverse effect, Child, business.industry, Alanine Transaminase, Drug Tolerance, Irritable Mood, Aggression, Psychiatry and Mental health, Tolerability, Anesthesia, Female, medicine.symptom, business, medicine.drug, Antipsychotic Agents

Abstract

Objective Evaluate the long-term safety and tolerability of aripiprazole in the treatment of irritability in pediatric subjects (6-17 years) with autistic disorder. Method A 52-week, open-label, flexibly dosed (2-15 mg/d) study of the safety and tolerability of aripiprazole in outpatients with a DSM-IV-TR diagnosis of autistic disorder who either had completed 1 of 2 antecedent, 8-week randomized trials or were enrolled de novo (ie, not treated in the randomized trials). Safety and tolerability measures included incidences of adverse events, extrapyramidal symptoms, weight, metabolic measures, vital signs, and other clinical assessments. Results Subjects were enrolled between September 2006 and June 2009. Three hundred thirty subjects entered the treatment phase: 86 de novo, 174 prior aripiprazole, and 70 prior placebo. A total of 199 (60.3%) subjects completed 52 weeks of treatment. Adverse events were experienced by 286/330 subjects (86.7%). Common adverse events included weight increase, vomiting, nasopharyngitis, increased appetite, pyrexia, upper respiratory tract infection, and insomnia. Discontinuations due to adverse events occurred in 35/330 randomized subjects (10.6%)-most commonly aggression and weight increase. One patient discontinued from the study due to a laboratory-related adverse event (moderately increased alanine transaminase and aspartate transaminase). Nine subjects experienced serious adverse events-most frequently aggression. Extrapyramidal symptoms-related adverse events occurred in 48/330 subjects (14.5%)-most commonly tremor (3.0%), psychomotor hyperactivity (2.7%), akathisia (2.4%), and dyskinesia (not tardive, 2.4%). At > 9 months' aripiprazole exposure (n = 220), mean change in body weight z score was 0.33 and body mass index z score was 0.31. The percentages of subjects with clinically significant fasting metabolic abnormalities at > 9 months were 2% for glucose, 5% for total cholesterol, 7% for low-density lipoprotein cholesterol, 30% for high-density lipoprotein cholesterol, and 5% for triglycerides. Conclusions Aripiprazole was generally safe and well tolerated in the long-term treatment of irritability associated with autistic disorder in pediatric subjects. Weight should be proactively monitored during long-term treatment. Trial registration clinical trials.gov Identifier: NCT00365859.

Published

2009