Toxicity and Adverse Effects in Clozapine-Related Presentations to a Medical Toxicology Service in Western Sydney.

IF 2.5 4区 医学 Q3 TOXICOLOGY
Journal of Medical Toxicology Pub Date : 2023-10-01 Epub Date: 2023-08-25 DOI:10.1007/s13181-023-00963-1
Pramod Chandru, Naren Gunja
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引用次数: 0

Abstract

Background: Clozapine is an anti-psychotic agent, reserved for treatment-resistant schizophrenia, with demonstrated efficacy in an otherwise therapeutically challenging patient population. We aimed to review the full spectrum casemix of clozapine presentations to our tertiary toxicology service.

Methods: In this retrospective study, we reviewed consecutive clozapine related toxicity presentations to a tertiary medical toxicology inpatient and consultation service-including deliberate self-poisoning (DSP), adverse drug reaction (ADR), recreational use, and therapeutic misadventure over a 10-year period from 2011 to 2021. Data were extracted for demographics, ingested dose, exposure characteristics, and patient outcome.

Results: We identified 83 patients with clozapine-related presentations over the 10-year period. Twenty-two patients were excluded. Of the remaining 61 patients, 28 patients presented with DSP, 20 patients with accidental overdose, and 13 patients with an ADR; no patients presented with recreational use. It was noted that ADRs were largely idiosyncratic reactions and not always related to dose adjustments. In the context of therapeutic misadventure and DSP, we noted that a lower mean dose achieved a higher poison severity score (PSS) in clozapine-naive patients when compared to those patients on regular clozapine.

Conclusions: The presentation of clozapine-related toxicity differs depending on the modality of ingestion, whether DSP, accidental, or as a result of ADR. Patients naive to clozapine therapy tend to experience higher PSS with lower doses ingested either in a deliberate self-poisoning or accidental ingestion context. This is likely due to tolerance to the sedative properties of clozapine. No patients manifested clinical toxicity greater than 8 hours after ingestion, with an observation period of 6 hours accurately identifying toxicity in most patients.

氯氮平的毒性和不良反应向西悉尼的一家医学毒理学服务机构提交。
背景:氯氮平是一种抗精神病药物,专门用于治疗难治性精神分裂症,在其他具有治疗挑战性的患者群体中已证明有效。我们的目的是审查向我们的三级毒理学服务机构提交的氯氮平的全谱病例组合。方法:在这项回顾性研究中,我们回顾了2011年至2021年10年间,连续向三级医疗毒理学住院患者和咨询服务机构提交的氯氮平相关毒性报告,包括故意自我中毒(DSP)、药物不良反应(ADR)、娱乐性使用和治疗性意外事故。提取人口统计数据、摄入剂量、暴露特征和患者结果。结果:我们确定了83名在10年内出现氯氮平相关症状的患者。22名患者被排除在外。在剩下的61名患者中,28名患者出现DSP,20名患者出现意外服药过量,13名患者出现ADR;没有患者出现娱乐性使用。值得注意的是,不良反应在很大程度上是特殊反应,并不总是与剂量调整有关。在治疗性意外事故和DSP的背景下,我们注意到,与服用常规氯氮平的患者相比,服用较低平均剂量的氯氮平初始患者的中毒严重程度评分(PSS)较高。结论:氯氮平相关毒性的表现因摄入方式而异,无论是DSP、意外还是ADR。在故意自我中毒或意外摄入的情况下,氯氮平治疗初期的患者往往会经历较高的PSS,而摄入的剂量较低。这可能是由于对氯氮平的镇静特性的耐受性。没有患者在摄入后8小时以上出现临床毒性,6小时的观察期准确地确定了大多数患者的毒性。
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来源期刊
CiteScore
5.40
自引率
10.30%
发文量
46
期刊介绍: Journal of Medical Toxicology (JMT) is a peer-reviewed medical journal dedicated to advances in clinical toxicology, focusing on the diagnosis, management, and prevention of poisoning and other adverse health effects resulting from medications, chemicals, occupational and environmental substances, and biological hazards. As the official journal of the American College of Medical Toxicology (ACMT), JMT is managed by an editorial board of clinicians as well as scientists and thus publishes research that is relevant to medical toxicologists, emergency physicians, critical care specialists, pediatricians, pre-hospital providers, occupational physicians, substance abuse experts, veterinary toxicologists, and policy makers.       JMT articles generate considerable interest in the lay media, with 2016 JMT articles cited by various social media sites, the Boston Globe, and the Washington Post among others.     For questions or comments about the journal, please contact jmtinfo@acmt.net.    For questions or comments about the journal, please contact jmtinfo@acmt.net.
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