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Clozapine, relapse and adverse events: 10-year electronic cohort study in Canada: commentary, Kikuchi

Published online by Cambridge University Press:  30 January 2025

Yuki Kikuchi Open the ORCID record for Yuki Kikuchi [Opens in a new window]
Yuki Kikuchi*
Affiliation:
Department of Psychiatry, Graduate School of Medicine, Tohoku University, Sendai, Japan; and Department of Psychiatry, Kodama Hospital, Ishinomaki, Japan
*
Correspondence: Yuki Kikuchi. Email: ykikuchi@sand.ocn.ne.jp
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Abstract

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Keywords

Clozapinerelapseadverse eventscohort studyCanada
Type
Commentary
Information
The British Journal of Psychiatry , Volume 226 , Issue 1 , January 2025 , pp. 53 - 54
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Copyright
Copyright © The Author(s), 2025. Published by Cambridge University Press on behalf of Royal College of Psychiatrists

Response

I read with great interest the paper by Balbuena et al that investigated the impact of clozapine on the risk of readmission to hospital owing to psychiatric symptoms or adverse effects, based on 10 years of electronic records in Canada.Reference Balbuena, Halayka, Lee, Ahmed, Hinz and Kolla1 The study found that, compared to other antipsychotics, clozapine was associated with a reduced risk of psychiatric readmission to hospital after the initial 21 months in the adult cohort, a higher risk of readmission to hospital owing to adverse effects in the adult cohort and a lower risk of psychiatric readmission to hospital in the child or youth cohort. However, I would like to highlight some methodological concerns that may affect the interpretation of these results.

First, the study did not consider the clinical diagnosis or indication for treatment of the patients in the cohort. The patient diagnoses included in the study were diverse, with 49% of the adult cohort and 72% of the child or youth cohort diagnosed with bipolar disorder. The number of patients treated with clozapine and their diagnoses were not clearly stated. In addition, the number of patients treated with other antipsychotics and their diagnoses were not reported. Furthermore, the study did not account for confounding by indication, which arises because of the more severe conditions of patients treated with clozapine. To address this, previous studies have conducted within-individual analyses,Reference Tiihonen, Taipale, Mehtala, Vattulainen, Correll and Tanskanen2Reference Taipale, Tanskanen, Mehtala, Vattulainen, Correll and Tiihonen4 focused on patients with treatment-resistant schizophreniaReference Stroup, Gerhard, Crystal, Huang and Olfson5 or adjusted as much as was feasible for covariates that could reflect the disease severity.Reference Weiser, Davis, Brown, Slade, Fang and Medoff6,Reference Vanasse, Blais, Courteau, Cohen, Roberge and Larouche7 The Canadian Network for Mood and Anxiety Treatments and International Society for Bipolar Disorders 2018 guidelines for the management of patients with bipolar disorder support the use of clozapine in treatment-resistant bipolar disorder. Therefore, although it was not inappropriate to include patients with bipolar disorder, it is necessary to compare clozapine treatments with other antipsychotic treatments, stratified by patient diagnosis and disease severity. Given that clozapine is the most well-established treatment for treatment-resistant schizophrenia, its efficacy may have been underestimated. In the study by Balbuena et al, it would be more appropriate to compare clozapine treatments with other antipsychotic treatments among patients with schizophrenia who have used clozapine or to conduct within-individual analyses.

Second, admissions to hospital owing to adverse reactions were limited to neutropenia, cardiomyopathy, myocarditis, pneumonia and constipation. However, given that these adverse effects are relatively more common with clozapine than with other antipsychotics, the number of admissions to hospital attributed to the adverse effects of clozapine may be relatively overestimated. A previous Finnish registry study, which included all somatic and cardiovascular admissions to hospital, did not find that clozapine was associated with significantly more somatic readmissions to hospital than other antipsychotics.Reference Taipale, Tanskanen, Mehtala, Vattulainen, Correll and Tiihonen4 Recent studies indicate that clozapine is associated with a higher risk of pneumoniaReference Luykx, Correll, Manu, Tanskanen, Hasan and Tiihonen8,Reference Partanen, Happola, Kampe, Ahola-Olli, Hellsten and Rask9 and ileus,Reference Partanen, Happola, Kampe, Ahola-Olli, Hellsten and Rask9 which may align with Balbuena et al's findings. Furthermore, the risk of several clozapine-related adverse effects, including pneumonia, increases with age;Reference Luykx, Correll, Manu, Tanskanen, Hasan and Tiihonen8,Reference Partanen, Happola, Kampe, Ahola-Olli, Hellsten and Rask9 thus, it may have been beneficial to stratify the adult cohort by age in this study.

Third, this study did not analyse the period of antipsychotic non-use. A total of 10 952 (19%) adults and 683 (32%) children and adolescents were excluded from the analysis because they experienced a relapse or admission to hospital owing to adverse events before antipsychotic medication was prescribed. In addition, readmissions to hospital that occurred after a prescription had been interrupted for >1 month were excluded based on the interpretation that it was not related to any drug. Given the notable impact of nonadherence on relapse, this exclusion was significant. There may be some debate about how to set the length of the interruption period. However, if there were more interrupted prescriptions for antipsychotics other than clozapine, the relapse of antipsychotics other than clozapine could have been underestimated. Moreover, the study does not describe how long-acting injections were administered. Categorising the duration of antipsychotic non-use medications might have allowed for a more comprehensive analysis.

Data availability

Data availability is not applicable to this article, as no new data were created or analysed in this study.

Funding

This research received no specific grant from any funding agency, commercial or not-for-profit sectors.

Declaration of interest

None.

References

Balbuena, L, Halayka, S, Lee, A, Ahmed, AG, Hinz, T, Kolla, N, et al. Clozapine, relapse, and adverse events: a 10-year electronic cohort study in Canada. Br J Psychiatry [Epub ahead of print] 18 Sep 2024. Available from: https://doi.org/10.1192/bjp.2024.140.Google Scholar
Tiihonen, J, Taipale, H, Mehtala, J, Vattulainen, P, Correll, CU, Tanskanen, A. Association of antipsychotic polypharmacy vs monotherapy with psychiatric rehospitalization among adults with schizophrenia. JAMA Psychiatry 2019; 76: 499507.CrossRefGoogle ScholarPubMed
Taipale, H, Mehtala, J, Tanskanen, A, Tiihonen, J. Comparative effectiveness of antipsychotic drugs for rehospitalization in schizophrenia – a nationwide study with 20-year follow-up. Schizophr Bull 2018; 44: 1381–7.CrossRefGoogle ScholarPubMed
Taipale, H, Tanskanen, A, Mehtala, J, Vattulainen, P, Correll, CU, Tiihonen, J. 20-year follow-up study of physical morbidity and mortality in relationship to antipsychotic treatment in a nationwide cohort of 62,250 patients with schizophrenia (FIN20). World Psychiatry 2020; 19: 61–8.CrossRefGoogle Scholar
Stroup, TS, Gerhard, T, Crystal, S, Huang, C, Olfson, M. Comparative effectiveness of clozapine and standard antipsychotic treatment in adults with schizophrenia. Am J Psychiatry 2016; 173: 166–73.CrossRefGoogle ScholarPubMed
Weiser, M, Davis, JM, Brown, CH, Slade, EP, Fang, LJ, Medoff, DR, et al. Differences in antipsychotic treatment discontinuation among veterans with schizophrenia in the U.S. Department of veterans affairs. Am J Psychiatry 2021; 178: 932–40.CrossRefGoogle ScholarPubMed
Vanasse, A, Blais, L, Courteau, J, Cohen, AA, Roberge, P, Larouche, A, et al. Comparative effectiveness and safety of antipsychotic drugs in schizophrenia treatment: a real-world observational study. Acta Psychiatr Scand 2016; 134: 374–84.CrossRefGoogle ScholarPubMed
Luykx, JJ, Correll, CU, Manu, P, Tanskanen, A, Hasan, A, Tiihonen, J, et al. Pneumonia risk, antipsychotic dosing, and anticholinergic burden in schizophrenia. JAMA Psychiatry 2024; 81: 967–75.CrossRefGoogle ScholarPubMed
Partanen, JJ, Happola, P, Kampe, A, Ahola-Olli, A, Hellsten, A, Rask, SM, et al. High burden of ileus and pneumonia in clozapine-treated individuals with schizophrenia: a Finnish 25-year follow-up register study. Am J Psychiatry 2024; 181: 879–92.CrossRefGoogle ScholarPubMed
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