Switching Patients with Schizophrenia from Intramuscular Paliperidone Palmitate Once Monthly to TV-46000, a Long-Acting Subcutaneous Antipsychotic: Population Pharmacokinetic–Based Strategies

Document Type

Article

Publication Title

Advances in Therapy

Abstract

Introduction: Pharmacokinetic differences between long-acting injectable antipsychotic (LAI) formulations, combined with a lack of clinical switch studies, contribute to clinician uncertainty when transitioning between LAIs. This analysis employed a population pharmacokinetic (popPK) modeling approach to characterize dosing conversions and switching strategies from intramuscular paliperidone palmitate once monthly (PP1m) to TV-46000, a long-acting subcutaneous formulation of risperidone, once monthly (q1m), with a secondary analysis of PP1m to TV-46000 every 2 months (q2m). Methods: For PP1m and TV-46000, concentration–time profiles for paliperidone and TV-46000 total active moiety (TAM; risperidone + paliperidone) were simulated on the basis of published popPK models with virtual populations of 5000 patients. TAM exposure following oral administration served as a comparison benchmark. Results: When switching from PP1m 234 mg at steady state (comparable to 6 mg/day oral risperidone), the most comparable switch involved initiating TV-46000 125 mg q1m 4 weeks after the last PP1m dose. Ratios of TV-46000 to PP1m for maximum, minimum, and average plasma concentration (Cmax, Cmin, and Cavg, respectively) post switch ranged from 1.0 to 1.4 after the first dose and 1.0–1.3 at steady state. Switching from other PP1m doses to TV-46000 q1m (comparable to 2–4 mg daily oral risperidone) using a 4-week interval demonstrated comparable TAM exposures. When switching from PP1m 234 mg to TV-46000 250 mg q2m, Cmax was higher and Cmin lower than that of q1m, though Cavg remained comparable to 5/6 mg daily oral risperidone. Conclusion: Switching to TV-46000 125 mg q1m 4 weeks after the last PP1m 234-mg injection yielded generally comparable pharmacokinetic parameters at steady state. The same was true for other TV-46000 q1m or q2m dosages and equivalent dosages of PP1m. Clinician discretion will ultimately determine how to switch on the basis of factors such as patient preference, convenience, and concerns about tolerability or symptom breakthrough.

First Page

5564

Last Page

5577

DOI

10.1007/s12325-025-03329-x

Publication Date

11-1-2025

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