Reevaluating Clozapine-Induced QT Prolongation.

IF 4.8 1区 医学 Q1 PSYCHIATRY
Timothy Tanzer, Rebecca Hanisch, Chloe Yap, Nicola Warren, Michael Barras, Steve Kisely, Katherine Isoardi, Kiana Kosari, Dan Siskind
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引用次数: 0

Abstract

Background and hypothesis: Clozapine is the most effective medicine for treatment-resistant schizophrenia, but is limited by adverse events, including potential QT prolongation which can lead to life-threatening arrhythmias. Studies linking clozapine and corrected QT (QTc) prolongation may overestimate this risk due to high rates of clozapine-associated tachycardia. We investigated whether trough clozapine plasma levels are independently associated with QT prolongation after accounting for heart rate.

Study design: We conducted a retrospective, cross-sectional analysis of inpatients treated with clozapine at a tertiary hospital between 2017 and 2023. Trough clozapine plasma levels, and 12-lead electrocardiograms were extracted from electronic medical records. QT intervals were manually measured and corrected using Bazett's, Fredericia, Hodges' formulae, and the QT nomogram. Multivariable regression and causal mediation were used to test the association between clozapine plasma level, heart rate, and QTc.

Study results: Among 313 patients, Bazett's correction classified 27.5% as having prolonged QTc, whereas only one patient (0.3%) exceeded the at-risk threshold using Fredericia, Hodges, or the QT nomogram. Clozapine plasma level correlated with Bazett's-corrected QT (QTcB) (P = .02), but not after adjustment for heart rate (P = .75). Mediation analysis showed that heart rate significantly mediated the relationship between clozapine plasma level and QTcB intervals (P < .001).

Conclusions: Apparent clozapine-induced QTc prolongation is largely an artifact of tachycardia and over-correction by Bazett's formula. The Fredericia and Hodges formulae, and the QT nomogram provide a more reliable assessment of torsadogenic risk and prevent unnecessary discontinuation or dose reductions of clozapine.

氯氮平所致QT间期延长的再评估。
背景与假设:氯氮平是治疗难治性精神分裂症最有效的药物,但其不良事件有限,包括潜在的QT间期延长,可导致危及生命的心律失常。氯氮平与校正QT间期(QTc)延长相关的研究可能高估了这种风险,因为氯氮平相关的心动过速发生率很高。我们研究了考虑心率后氯氮平过谷血浆水平是否与QT延长独立相关。研究设计:我们对2017年至2023年在一家三级医院接受氯氮平治疗的住院患者进行了回顾性、横断面分析。从电子病历中提取氯氮平槽血药浓度和12导联心电图。使用Bazett, Fredericia, Hodges公式和QT nomogram人工测量和校正QT间期。采用多变量回归和因果中介检验氯氮平血浆水平、心率和QTc之间的关系。研究结果:在313例患者中,Bazett校正将27.5%的患者分类为QTc延长,而使用Fredericia, Hodges或QT nomogram,只有1例患者(0.3%)超过了危险阈值。氯氮平血浆水平与Bazett校正QT (QTcB)相关(P = 0.02),但调整心率后与之无关(P = 0.75)。中介分析显示,心率显著介导氯氮平血浆水平与QTcB间期的关系(P < 0.001)。结论:氯氮平引起的QTc明显延长在很大程度上是由心动过速和贝泽特公式矫治过度引起的。Fredericia和Hodges公式以及QT形态图提供了更可靠的反甾体源性风险评估,并防止不必要的氯氮平停药或剂量减少。
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来源期刊
Schizophrenia Bulletin
Schizophrenia Bulletin 医学-精神病学
CiteScore
11.40
自引率
6.10%
发文量
163
审稿时长
4-8 weeks
期刊介绍: Schizophrenia Bulletin seeks to review recent developments and empirically based hypotheses regarding the etiology and treatment of schizophrenia. We view the field as broad and deep, and will publish new knowledge ranging from the molecular basis to social and cultural factors. We will give new emphasis to translational reports which simultaneously highlight basic neurobiological mechanisms and clinical manifestations. Some of the Bulletin content is invited as special features or manuscripts organized as a theme by special guest editors. Most pages of the Bulletin are devoted to unsolicited manuscripts of high quality that report original data or where we can provide a special venue for a major study or workshop report. Supplement issues are sometimes provided for manuscripts reporting from a recent conference.
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