Abstract
BackgroundAntipsychotics are used in Parkinson disease (PD) to treat psychosis, mood, and behavioral disturbances. Commonly used antipsychotics differ substantially in their potential to worsen motor symptoms through dopaminergic receptor blockade. Recent real-world data on the use and continuation of antipsychotic therapy in PD are lacking. The objectives of this study are to (1) examine the continuation of overall and initial antipsychotic therapy in individuals with PD and (2) determine whether continuation varies by drug dopamine receptor blocking activity.MethodsWe conducted a retrospective cohort study using U.S. commercially insured individuals in Optum 2001–2019. Adults aged 40 years or older with PD initiating antipsychotic therapy, with continuous insurance coverage for at least 6 months following drug initiation, were included. Exposure to pimavanserin, quetiapine, clozapine, aripiprazole, risperidone, or olanzapine was identified based on pharmacy claims. Six-month continuation of overall and initial antipsychotic therapy was estimated by time to complete discontinuation or switching to a different antipsychotic. Cox proportional hazards models evaluated factors associated with discontinuation.ResultsOverall, 38.6% of 3566 PD patients in our sample discontinued antipsychotic therapy after the first prescription, 61.4% continued with overall treatment within 6 months of initiation. Clozapine use was too rare to include in statistical analyses. Overall therapy discontinuation was more likely for those who initiated medications with known dopamine-receptor blocking activity (adjusted hazard ratios 1.76 [95% confidence interval 1.40–2.20] for quetiapine, 2.15 [1.61–2.86] for aripiprazole, 2.12 [1.66–2.72] for risperidone, and 2.07 [1.60–2.67] for olanzapine), compared with serotonin receptor-specific pimavanserin. Initial antipsychotic therapy discontinuation also associated with greater dopamine-receptor blocking activity medication use – adjusted hazard ratios 1.57 (1.28–1.94), 1.88 (1.43–2.46), 2.00 (1.59–2.52) and 2.03 (1.60–2.58) for quetiapine, aripiprazole, risperidone, and olanzapine, respectively, compared with pimavanserin. Similar results were observed in sensitivity analyses.ConclusionsOver one-third of individuals with PD discontinued antipsychotic therapy, especially if the initial drug has greater dopamine-receptor blocking activity. Understanding the drivers of antipsychotic discontinuation, including ineffectiveness, potentially inappropriate use, clinician inertia, patient adherence and adverse effects, is needed to inform clinical management of psychosis in PD and appropriate antipsychotic use in this population.
Highlights
Antipsychotics are used in Parkinson disease (PD) to treat psychosis, mood, and behavioral disturbances
Pimavanserin is a selective serotonin type 2A (5-HT2A) inverse agonist, with negligible binding at almost all other receptors targeted by atypical APs, and is expected to treat psychosis symptoms in PD without worsening motor symptoms [19, 21]
Individual baseline characteristics We identified 3566 individuals meeting our inclusion criteria:153 new users of pimavanserin, 2452 of quetiapine, 169 of aripiprazole, 462 of risperidone, and 304 of olanzapine
Summary
Antipsychotics are used in Parkinson disease (PD) to treat psychosis, mood, and behavioral disturbances. Second-generation or atypical APs — clozapine, quetiapine, risperidone, olanzapine, and aripiprazole — have long been prescribed off-label for PDP [7,8,9,10], as well as for behavioral or mood disturbance in adults with neurodegenerative disease [11,12,13], use for the latter indications and in older adult populations is discouraged by clinical safety guidelines [8, 14, 15]. Safety and tolerance data for AP use in PD patients has traditionally focused on dopamine receptor antagonism leading to worsening of parkinsonism. Pimavanserin is a selective 5-HT2A inverse agonist, with negligible binding at almost all other receptors targeted by atypical APs, and is expected to treat psychosis symptoms in PD without worsening motor symptoms [19, 21]
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