Asenapine pharmacokinetics and tolerability in a pediatric population

Peter Dogterom; Robert Riesenberg; Rik de Greef; Justin Dennie; Martin Johnson; Venkatesh Pilla Reddy; André Mm Miltenburg; Robert L Findling; Abhijeet Jakate; Timothy J Carrothers; Matthew D Troyer

doi:10.2147/DDDT.S171475

Asenapine pharmacokinetics and tolerability in a pediatric population

Drug Des Devel Ther. 2018 Aug 30:12:2677-2693. doi: 10.2147/DDDT.S171475. eCollection 2018.

Affiliations

¹ Early Stage Development, Merck Sharp and Dohme, Oss, the Netherlands, peter.dogterom@qps.com.
² Atlanta Center for Medical Research, Atlanta, GA.
³ Merck, Kenilworth, NJ.
⁴ Kennedy Krieger Institute, Johns Hopkins University, Baltimore, MD.
⁵ Allergan, Madison, NJ, USA.

Abstract

Purpose: This study aimed to characterize the pharmacokinetic (PK) properties, safety, and tolerability of asenapine, and to develop a population PK model in pediatric patients with schizophrenia, bipolar disorder, or other psychiatric disorders.

Methods: Two Phase I multiple ascending-dose studies were conducted to evaluate the PK, safety, and tolerability of sublingual asenapine in pediatric patients (age 10-17 years) with schizophrenia or bipolar I disorder. Patients received asenapine 1-10 mg twice daily for up to 12 days. PK parameters (maximum concentration [C_max], area under the curve from 0 to 12 hours [AUC_0-12], time to C_max [T_max], and half-life) were summarized for asenapine with descriptive statistics, and safety parameters were collected. A population PK model, which included the two Phase I studies and two additional Phase III efficacy studies (asenapine 2.5-10 mg twice daily for up to 8 weeks, age 10-17 years), was developed using nonlinear mixed-effect modeling based on a previously developed adult PK model. The final model was used in simulations to obtain asenapine-exposure estimates across pediatric subgroups and to determine if intrinsic covariates warrant dose adjustments.

Results: The PK of asenapine showed rapid absorption (T_max ~1 hour) with an apparent terminal half-life between 16 and 32 hours. Increases in mean C_max and AUC_0-12 appeared to be dose-proportional in one study and near dose-proportional in the second study. Steady state was attained within 8 days. The most frequently occurring treatment-emergent adverse events were dysgeusia, sedation, and oral hypoesthesia. Simulation-based estimates of C_max and AUC_0-12 were similar for pediatric and adult patients; age, body-mass index, race, and sex were not associated with changes in asenapine exposure.

Conclusion: Asenapine was generally safe and well tolerated in pediatric patients aged 10-17 years. PK and safety data were similar to that observed in the adult population. Intrinsic factors had no significant impact on asenapine exposure, indicating there is no need for dose adjustments in the pediatric population.

Keywords: asenapine; atypical antipsychotic; bipolar disorder; child and adolescent; pharmacokinetics; schizophrenia.

Publication types

Clinical Trial, Phase III
Randomized Controlled Trial

MeSH terms

Adolescent
Antipsychotic Agents / administration & dosage
Antipsychotic Agents / adverse effects*
Antipsychotic Agents / pharmacokinetics*
Child
Dibenzocycloheptenes
Female
Heterocyclic Compounds, 4 or More Rings / administration & dosage
Heterocyclic Compounds, 4 or More Rings / adverse effects*
Heterocyclic Compounds, 4 or More Rings / pharmacokinetics*
Humans
Male
Mental Disorders / drug therapy*
Mental Disorders / metabolism*

Substances

Antipsychotic Agents
Dibenzocycloheptenes
Heterocyclic Compounds, 4 or More Rings
asenapine