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Review
. 2023 Sep 13:13:20451253231198463.
doi: 10.1177/20451253231198463. eCollection 2023.

Implementing gradual, hyperbolic tapering of long-acting injectable antipsychotics by prolonging the inter-dose interval: an in silico modelling study

Affiliations
Review

Implementing gradual, hyperbolic tapering of long-acting injectable antipsychotics by prolonging the inter-dose interval: an in silico modelling study

James R O'Neill et al. Ther Adv Psychopharmacol. .

Abstract

Gradual, hyperbolic tapering has been proposed as a method to reduce the risk of withdrawal effects and potential relapse of an underlying condition by minimising disruption of existing equilibria. We applied hyperbolic tapering principles in silico to long-acting aripiprazole to generate regimens for withdrawal in clinical practice. We derived thresholds for taper rates using existing studies and consensus. Using pharmacokinetic data for aripiprazole long-acting injectable antipsychotic (ALAI), we conducted in silico modelling to examine the impact of abrupt cessation of long-acting injectable antipsychotic (LAI) medication and the effect of prolonging inter-dose interval on plasma aripiprazole levels and consequent D2 occupancy. We also modelled transitions from LAI medication to oral medication. Regimens were designed to afford a rate of reduction between 5 and 12.5 percentage points of D2 occupancy per month. Abrupt discontinuation of ALAI was shown to lead to a maximal D2 occupancy reduction of 16.8 percentage points per month; prolongation of the inter-dose interval of ALAI produced a slower reduction. Specifically, hyperbolic tapering was afforded by prolongation of a 400 mg ALAI inter-dose interval from 4 to 7 weeks, before reducing the dose to 300 mg ALAI. This could then be administered at up to 4-week (for 6% maximal D2 occupancy change), 6-week (9% change) or 7-week (11% change) intervals. Switching to oral medication - 5, 2.5 and 1.25 mg for the three regimens, respectively - is required for ALAI to complete full cessation to prevent too rapid a reduction in D2 occupancy. Oral medication should probably be maintained at a consistent dose for 3-6 months before further reductions to account for residual LAI being concurrently eliminated. Hyperbolic dose tapering is possible with ALAI through prolongation of the inter-dose interval and may reduce the risk of relapse compared to abrupt discontinuation of LAI medication.

Keywords: antipsychotic withdrawal; depot tapering; discontinuation; hyperbolic tapering; long-acting injectable antipsychotic; pharmacokinetic; stopping.

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Conflict of interest statement

JO’N has no conflicts of interest that are directly relevant to the content in this article. DMT has received research funding from Janssen Pharmaceuticals and Lundbeck but no sources of funding were received for the preparation of this article. He has also received speaking honoraria from Janssen, Otsuka, Viatris, Lundbeck, Sunovion and Recordati. MAH is the clinical research fellow on the NIHR-funded RADAR study examining reduction and discontinuation of antipsychotic medication in people with psychotic disorders, including depot medication. He is an unpaid associate of the International Institute of Psychiatric Drug Withdrawal and a member of the Tapering Antipsychotics and Evaluating Recovery (TAPER) group consisting of international psychiatric researchers.

Figures

Figure 1.
Figure 1.
Graphs demonstrating (a) the elimination of LAI medication from plasma peak levels (time = 0) following abrupt cessation, (b) the effect that increasing the plasma level of medication has in occupying D2 receptors and (c) the combined effects of the phenomena illustrated in part labels a and b which demonstrates the decrease in D2 occupancy as LAI medications are eliminated from plasma. LAI, long-acting injectable antipsychotic.
Figure 2.
Figure 2.
Pictorial representation of how the rate of decreasing D2 occupancy was assessed, in terms of both overall and terminal reductions.
Figure 3.
Figure 3.
Effect of abrupt cessation of a 300 mg ALAI, in terms of both (a) plasma concentration levels and (b) occupancy of D2 receptors. ALAI, aripiprazole long-acting injectable.
Figure 4.
Figure 4.
Pictorial representation of how residual drug from previous ALAI administration affects the choice of dose for subsequent oral medications. This is reflected in both (a) plasma aripiprazole level and (b) the effect on changing D2 occupancy. ALAI, aripiprazole long-acting injectable.
Figure 5.
Figure 5.
Pictorial representations of how the proposed (a) ‘slow’, (b) ‘moderate’ and (c) ‘fast’ regimes would affect both (i) plasma aripiprazole level and (ii) D2 receptor occupancy.

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