根据国际滴定指南评估氯氮平的主要不良反应。

The mental health clinician Pub Date : 2024-06-03 eCollection Date: 2024-06-01 DOI:10.9740/mhc.2024.06.204
Matthew Nuebel, Jonathan G Leung, Christopher Hughes, Ian McGrane
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引用次数: 0

摘要

简介氯氮平是唯一获准用于治疗耐药性精神分裂症的抗精神病药物,但如果没有适当的监测,可能会导致致命后果。国际成人氯氮平滴定指南》将患者分为正常代谢者和缓慢代谢者。分类提供了氯氮平滴定时间表,并建议定期监测 c 反应蛋白(CRP)和氯氮平浓度,以降低药物不良反应(ADR)的风险。该指南对氯氮平药物不良反应的影响尚未进行评估:一项回顾性病历审查评估了一个中心从 2013 年 1 月 1 日至 2022 年 6 月 1 日期间氯氮平无效成人住院患者的氯氮平滴定、实验室监测、ADR 和停药情况。将每位患者的每周氯氮平累积用量与其指南推荐用量进行比较,得出符合百分比。线性逻辑回归评估了滴定速度与出现不良反应之间的关系,描述性统计分析了实验室监测结果:共纳入 43 名患者,其中大部分是患有精神分裂症的白人男性。最近一周住院的氯氮平剂量百分比与出现不良反应的概率呈反比关系。与肥胖患者相比,非肥胖患者发生 ADR 的几率较低(几率比 = 0.17;95% CI,0.03-0.99)。CRP和氯氮平浓度监测效果不佳:讨论:根据我们主要针对白人男性进行的小型回顾性研究,更积极的氯氮平滴定并不会增加ADR。未来的研究需要更多样化的样本,并应关注特定的 ADR,因为快速滴定可能会增加 ADR 的发生率。肥胖患者发生 ADR 的风险较高,这与指南建议这些患者减慢滴定速度有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Evaluation of major adverse events of clozapine based on accordance to an international titration guideline.

Introduction: Clozapine is the only antipsychotic approved for treatment-resistant schizophrenia, but without appropriate monitoring, it can be associated with potentially fatal outcomes. An International Adult Clozapine Titration Guideline categorizes patients into normal or slow metabolizers. Categorization provides clozapine titration schedules and recommends regular c-reactive protein (CRP) and clozapine concentration monitoring to reduce the risk of adverse drug reactions (ADRs). The impact of the guideline on clozapine ADRs has not been evaluated.

Methods: A retrospective chart review assessed clozapine titrations, laboratory monitoring, ADRs, and discontinuations for clozapine-naive adult inpatients at a single center from January 1, 2013, to June 1, 2022. Each patient's cumulative weekly clozapine dosage was compared with their guideline recommended dosage to create a percent accordance. Linear logistic regression evaluated the relationship between titration speed and the presence of an ADR, while descriptive statistics analyzed laboratory monitoring.

Results: Forty-three patients were included, with the majority being White males with schizophrenia. An inverse relationship existed between the last inpatient week clozapine dose percent accordance and the probability of an ADR. Nonobese patients were less likely than obese patients to experience an ADR (odds ratio = 0.17; 95% CI, 0.03-0.99). CRP and clozapine concentration monitoring was suboptimal.

Discussion: Based on our small retrospective review of primarily White males, more aggressive clozapine titrations did not increase ADRs. Future studies with more diverse samples are needed and should focus on specific ADRs, which may have increased occurrence with rapid titrations. Obese patients were at higher risk of ADRs, correlating with the guideline-recommended slower titrations for these patients.

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