A proposal for reducing maximum target doses of drugs for psychosis: Reviewing dose–response literature

O’Neill, James R.; Jameson, Adam; McLean, Samantha L.; Dixon, Michael; Cardno, Alastair G.; Lawrence, Christopher

doi:10.1177/02698811241239543

J Psychopharmacol

2024

DOI: 10.1177/02698811241239543

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A proposal for reducing maximum target doses of drugs for psychosis: Reviewing dose–response literature

James R. O’Neill,

Adam Jameson,

Samantha L. McLean

et al.

Abstract: Background: Presently, there is limited guidance on the maximal dosing of psychosis drugs that is based on effectiveness rather than safety or toxicity. Current maximum dosing recommendations may far exceed the necessary degree of dopamine D2 receptor blockade required to treat psychosis. This may lead to excess harm through cognitive impairment and side effects. Aims: This analysis aimed to establish guidance for prescribers by optimally dosing drugs for psychosis based on efficacy and benefit. Methods: We us… Show more

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2024

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Cited by 2 publications

References 85 publications

(122 reference statements)

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Augmenting clozapine with antipsychotics—Correspondence

Mukherjee,

Sazhin,

Cho

2024

Australas Psychiatry

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Augmenting clozapine with antipsychotics—Correspondence

Mukherjee,

Sazhin,

Cho

2024

Australas Psychiatry

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Using in silico methods to determine optimal tapering regimens for decanoate-based long-acting injectable psychosis drugs

O’Neill,

Taylor,

Horowitz

2024

Therapeutic Advances in Psychopharmacology

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Background: Reducing the dose of psychosis drugs in a gradual hyperbolic manner may minimise withdrawal effects and risk of relapse. There is presently limited guidance on tapering decanoate-based long-acting injectable dopamine antagonists (LIDAs). Objectives: We aimed to apply hyperbolic principles of tapering to the decanoate-based LIDAs flupentixol, zuclopenthixol and haloperidol to develop withdrawal regimens. Design: We used in silico methodology to predict plasma drug levels and D2 occupancy for different LIDA regimens. Methods: Existing pharmacokinetic and receptor occupancy data from nuclear neuroimaging studies were used to power modelling. Abrupt discontinuation was examined as a potential strategy, and dose reduction was modelled with pre-defined constraints used in similar work of 10 (fast regimens), 5 (moderate) and 2.5 (slow) percentage points of D2 occupancy change per month. Results: Abrupt discontinuation of decanoate-based LIDAs leads to excessive change in D2 occupancy which violated our pre-defined constraints, potentially resulting in withdrawal symptoms and increased risk of relapse. Reduction of LIDA dose allowed hyperbolic reduction in plasma level consistent with imposed constraints on receptor occupancy reduction rate. For equivalent per-weekly LIDA dosing, more frequent administration allowed a more gradual reduction of D2 occupancy. However, switching to oral forms is required to continue hyperbolic tapering to full discontinuation; reduction to zero using only LIDA produces too large a reduction in D2 occupancy. Guidance for reduction and cessation of LIDAs according to slow, moderate and fast criteria is provided. Conclusion: Abrupt cessation of decanoate LIDAs is not consistent with gradual hyperbolic tapering, despite their longer half-lives compared with oral formulations. Reduction to the point of full discontinuation can only be achieved by switching to oral therapy to complete the taper. These results are limited by the in silico and theoretical nature of the study, and there is a need to confirm these findings through real-world observational and interventional studies.

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A proposal for reducing maximum target doses of drugs for psychosis: Reviewing dose–response literature

Cited by 2 publications

References 85 publications

Augmenting clozapine with antipsychotics—Correspondence

Augmenting clozapine with antipsychotics—Correspondence

Using in silico methods to determine optimal tapering regimens for decanoate-based long-acting injectable psychosis drugs

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