The Dilemma of Polypharmacy in Psychosis: is It Worth Combining Partial and Full Dopamine Modulation?

Overview

Journal Int Clin Psychopharmacol

Specialty Pharmacology

Date 2022 Jul 11

PMID 35815937

Authors

Matteo Lippi

Giuseppe Fanelli

Chiara Fabbri

Diana De Ronchi

Alessandro Serretti

Affiliations

Soon will be listed here.

Abstract

Antipsychotic polypharmacy in psychotic disorders is widespread despite international guidelines favoring monotherapy. Previous evidence indicates the utility of low-dose partial dopamine agonist (PDAs) add-ons to mitigate antipsychotic-induced metabolic adverse effects or hyperprolactinemia. However, clinicians are often concerned about using PDAs combined with high-potency, full dopaminergic antagonists (FDAs) due to the risk of psychosis relapse. We, therefore, conducted a literature review to find studies investigating the effects of combined treatment with PDAs (i.e. aripiprazole, cariprazine and brexpiprazole) and FDAs having a strong D 2 receptor binding affinity. Twenty studies examining the combination aripiprazole - high-potency FDAs were included, while no study was available on combinations with cariprazine or brexpiprazole. Studies reporting clinical improvement suggested that this may require a relatively long time (~11 weeks), while studies that found symptom worsening observed this happening in a shorter timeframe (~3 weeks). Patients with longer illness duration who received add-on aripiprazole on ongoing FDA monotherapy may be at greater risk for symptomatologic worsening. Especially in these cases, close clinical monitoring is therefore recommended during the first few weeks of combined treatment. These indications may be beneficial to psychiatrists who consider using this treatment strategy. Well-powered randomized clinical trials are needed to derive more solid clinical recommendations.

Citing Articles

A systematic review and meta-analysis of the effects of combined aripiprazole on glycolipid metabolism in schizophrenia.

Wei T, Jiang L, Zhang R, Su H, Sun Z, Sun J Front Psychiatry. 2025; 15:1496986.

PMID: 39866685 PMC: 11757238. DOI: 10.3389/fpsyt.2024.1496986.

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