Hostname: page-component-78c5997874-j824f Total loading time: 0 Render date: 2024-11-17T06:32:24.726Z Has data issue: false hasContentIssue false

Population pharmacokinetic modeling and simulations of dopamine Dd2 receptor occupancy of long-acting intramuscular risperidone-ISM

Published online by Cambridge University Press:  23 March 2020

J. Llaudó
Affiliation:
Laboratorios Farmacéuticos Rovi-S.A., Medical Department, Madrid, Spain
L. Anta
Affiliation:
Laboratorios Farmacéuticos Rovi-S.A., Medical Department, Madrid, Spain
I. Ayani*
Affiliation:
Laboratorios Farmacéuticos Rovi-S.A., Medical Department, Madrid, Spain
J. Martínez-González
Affiliation:
Laboratorios Farmacéuticos Rovi-S.A., Medical Department, Madrid, Spain
I. Gutierro
Affiliation:
Laboratorios Farmacéuticos Rovi-S.A., R&D, Madrid, Spain
R. Faelens
Affiliation:
SGS Exprimo NV, Exprimo, Mechelen, Belgium
J. Winkler
Affiliation:
SGS Exprimo NV, Exprimo, Mechelen, Belgium
E. Snoeck
Affiliation:
SGS Exprimo NV, Exprimo, Mechelen, Belgium
*
* Corresponding author.

Abstract

Core share and HTML view are not available for this content. However, as you have access to this content, a full PDF is available via the ‘Save PDF’ action button.
Introduction

Risperidone-ISM is a new long-acting intramuscular formulation intended to achieve sustained plasma concentrations over 4 weeks without oral supplementation. The clinical efficacy to risperidone has been associated with 65–80% occupancy of dopamine D2 receptor (D2RO) and a mean Cmax between 7.5 ng/mL and 80 ng/mL.

Aim

Use a population PK/PD model to predict the PK and the D2RO for Risperidone-ISM in schizophrenic patients and to characterize the relationship among doses, in order to guide dose selection for a future Phase-III trial.

Methods

A population PK/PD analysis for Risperidone-ISM using Monolix software was conducted based on 6641 plasma samples from two Phase-I studies (17 healthy subjects and 31 schizophrenic subjects, respectively) and 1 Phase-II study (60 schizophrenic subjects). Simulations were subsequently undertaken predicting the steady state PK and D2RO after multiple Risperidone-ISM doses administered every 28 days for 12 weeks.

Results

Doses of 75 and 100 mg, administered either in gluteal or deltoid muscle, were predicted to result in median Cmax and Ctrough that stayed between 7.5 ng/mL and 80 ng/mL. At steady state 75 mg and 100 mg dose (gluteal) achieved a D2RO average [min–max] of 70.8% [61.4–80.4] and 74.3% [66.2–82.1], respectively; a 75-mg and 100-mg dose (deltoid) achieved a D2RO average [min–max] of 69.3% [56.5–80.3] and 73.0% [61.8–82.1], respectively. The model estimated that the 65% D2RO occurs within first 8 h after treatment.

Conclusions

Simulations were carried out supporting doses of 75 mg and 100 mg Risperidone-ISM to show the greatest efficacy and safety potential to be assessed in the future Phase-III trial.

Disclosure of interest

The authors have not supplied their declaration of competing interest.

Type
EV1133
Copyright
Copyright © European Psychiatric Association 2016
Submit a response

Comments

No Comments have been published for this article.