Prospective dose selection and acceleration of paliperidone palmitate 3-month formulation development using a pharmacometric bridging strategy.

AIMS: To prospectively select the dose of the paliperidone palmitate 3-month (PP3M) formulation, using a pharmacometric bridging strategy based on the paliperidone palmitate 1-month (PP1M) formulation previously approved for schizophrenia treatment. METHODS: Pharmacokinetic (PK) data from a 6-month interim analysis of a single dose PP3M Phase I clinical trial was integrated with a previously developed PP1M population-PK model. The model was updated to incorporate formulation as a covariate on absorption parameters and to explore the most critical design element of the Phase III study: the PP1M-to-PP3M dose multiplier for patients switching formulations. Plasma paliperidone concentrations were measured at predetermined intervals during Phase III, enabling comparison of the multiple-dose PK between PP1M and PP3M. Exposure matching was assessed graphically to determine whether paliperidone plasma concentrations from the two formulations overlapped. RESULTS: Prospective steady-state PK simulations revealed that a 3.5 multiple of the PP1M dose would yield a corresponding PP3M dose with comparable exposure. The prospective pharmacometric simulation and observed Phase III PK data agreed closely. Phase III results confirmed the hypothesis that efficacy of PP3M was noninferior to that of PP1M. The similarity in exposures between the two formulations was likely a key determinant of the equivalent efficacy between the two products observed in the Phase III study. CONCLUSIONS: Successful prospective PP3M Phase III clinical trial dose selection was achieved through the use of pharmacometric bridging, without conducting a Phase II study and using only limited Phase I data for PP3M. We estimate that this strategy reduced development time by 3-5 years and may be applicable to other drug development projects.

Rapidly disintegrating risperidone in subjects with schizophrenia or schizoaffective disorder: a summary of ten phase I clinical trials assessing taste, tablet disintegration time, bioequivalence, and tolerability.

BACKGROUND: Schizophrenia and schizoaffective disorder are severe and chronic psychiatric illnesses for which treatment compliance is important in the prevention of relapse. Atypical antipsychotic drugs, such as risperidone, have been found to be effective in the treatment of a range of psychiatric disorders. Although the oral route of administration is generally preferable to injection, some patients (eg, elderly patients or children) find swallowing physically difficult and thus refuse oral treatments. Rapidly disintegrating (RD) oral formulations of these drugs have been developed to improve their acceptability to patients and thus improve compliance. OBJECTIVE: The aim of this report was to describe the results from clinical studies that have assessed the taste, time to disintegration, and tolerability of RD risperidone tablets, and bioequivalence of RD risperidone tablets (2 x 0.5 mg, 2 mg, and reduced-size 4 mg) versus conventional (CV) risperidone tablets. METHODS: This study used data from 10 clinical trials conducted between 1996 and 2003. Eight trials were open-label, crossover trials; 2 were pilot trials, and all of the trials were short-term. The results from 2 trials were published previously; the remainder are unpublished trials. Taste, time to dissolution, and tolerability of RD risperidone tablets were assessed, and bioequivalence (based on the guidelines from the European and US health care evaluation agencies) of RD versus CV risperidone tablets were determined for risperidone, the active metabolite (9-hydroxy-risperidone), and the total antipsychotic fraction (sum of risperidone and the active moiety, 9-hydroxy-risperidone). RESULTS: In total, these trials included 264 subjects(160 patients with schizophrenia or schizoaffective disorder, 104 healthy volunteers; 173 men, 91 women; age range, 20-61 years). The taste of the RD risperidone tablets was rated as "nice" in 54.2% of subjects compared with 18.3% of subjects who rated CV risperidone as "nice." Totals of 28.8% and 49.2% of subjects described the RD risperidone tablets as "sweet" or "other taste" (commonly mint), respectively. A total of 66.7% of subjects rated the 4-mg RD risperidone tablets as "acceptable, but could be improved," while 85.7% rated the lower-dose RD risperidone tablets as "good." The median time to complete disintegration of the RD risperidone tablet was 38.0 seconds. The mean plasma concentration-time profiles of risperidone and the active moiety of RD or CV risperidone tablets were similar, and these 2 risperidone formulations were found to be bioequivalent. The RD and CV risperidone tablets were well tolerated; there were no serious adverse events reported. CONCLUSIONS: In the 10 studies analyzed, the taste of RD risperidone tablets was found to be acceptable in the majority of healthy subjects and patients with schizophrenia or schizoaffective disorder. In addition, RD risperidone tablets were found to be bioequivalent to CV risperidone tablets.

Sustained drug delivery optimizes long-term treatment of patients with schizophrenia.

Chronic disorders such as schizophrenia require long-term treatment programs in order to maintain patients at the lowest level of symptomatology, reduce the likelihood of psychotic relapse, and support achievement of remission and recovery. Evidence suggests that treatment with long-acting injectable antipsychotics reduces the impact of partial compliance and provides predictable release of medication, assuring continuous therapeutic coverage. Until recently, only conventional antipsychotic agents were available in long-acting formulations, thereby foregoing the advantages of the atypical class. Atypical agents which are given orally have been shown to provide long-term efficacy and tolerability benefits compared with conventional agents, but are limited by the need for daily administration. The most recent pharmacological strategy to achieve optimal maintenance treatment has been to combine the benefits of an atypical antipsychotic with delivery in a water-based long-acting formulation. The first antipsychotic to achieve this combination - long-acting risperidone - may thus represent an important advance in the optimization of long-term treatment outcomes in patients with schizophrenia.