体外膜氧合:小儿安非他明心脏毒性的抢救疗法

IF 0.5 Q4 PEDIATRICS
T. Olives, Christopher N. Sweat, Lauren Dorsey-Spitz, Farbod Bahadori-Esfahani, A. Arens, Jon B. Cole, Arif Somani
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引用次数: 0

摘要

目的 我们的目的是描述需要体外膜氧合(ECMO)生命支持的小儿安非他酮摄入的临床特征和过程。研究对象包括向美国中西部上部三个州的地区毒物控制(PC)系统报告的 18 岁以下患者的回顾性队列。所有暴露于安非他明的 18 岁以下患者均被纳入研究范围,并被编码为接受了 ECMO 治疗毒性。临床表现和包括 ECMO 在内的治疗情况以描述性统计数字的形式呈现。结果 在研究期间,共报告了 4951 例安非他明暴露,其中 1145 例(23.1%)为儿童。九名患者被编码为接受了 ECMO;四名患者(44.4%)的年龄小于 18 岁(中位数为 16 岁,范围为 14-17 岁)。所有患者均接受了静脉动脉 ECMO 治疗。从进食到就诊的中位时间为 2.25 小时(范围:1-3.5)。首次收缩压和脉搏的中位数分别为 100 毫米汞柱(范围:70-124)和 119.5(范围:70-175)。从进食到 ECMO 的中位时间为 17.63 小时(范围:7.25-33.75);使用血管加压药的中位次数为 2.5 次(范围:2-3)。所有患者都经历了多次癫痫发作、室性心律失常和低血压。四人中有三人心脏骤停。除一名患者外,其余患者均需转入具备 ECMO 功能的医疗机构接受最终治疗。三名患者存活下来,神经功能完全恢复;一名患者死亡。结论 在本研究中,需要进行 ECMO 的小儿安非他明病例很少见。启动 ECMO 的时间和 EMCO 的持续时间表明,血液动力学不稳定的不同起始时间可能会延迟 ECMO 的启动。PCs 和医学毒理学家有责任向处方者和儿科医生宣传安非他酮的潜在致死性,并考虑尽早转入 ECMO 中心。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Extracorporeal Membrane Oxygenation: Rescue Therapy in Pediatric Bupropion Cardiotoxicity
Objective Our objective was to describe clinical characteristics and course of pediatric bupropion ingestions requiring extracorporeal membrane oxygenation (ECMO) life support. Desgin The study included a retrospective cohort of patients ≤18 years of age reported to a regional poison control (PC) system covering three states in the upper Midwest United States. All bupropion exposures ≤18 years of age, coded as receiving ECMO to treat toxicity, were included. Clinical presentation and management including ECMO are presented as descriptive statistics. Results During the study period, 4,951 bupropion exposures were reported; 1,145 (23.1%) were children. Nine patients were coded as undergoing ECMO; four (44.4%) were ≤18 years of age (median 16, range 14–17). All were treated with venoarterial ECMO. The median time from ingestion to presentation was 2.25 hours (range: 1–3.5). Median first systolic blood pressure and pulse were 100 mm Hg (range: 70–124) and 119.5 (range: 70–175). The median time from ingestion to ECMO was 17.63 hours (range: 7.25–33.75); median number of vasopressors was 2.5 (range: 2–3). All experienced multiple seizures, ventricular dysrhythmias, and hypotension. Three of four sustained cardiac arrest. All but one required transfer to an ECMO-capable facility for definitive care. Three patients survived with full neurologic recovery; one died. Conclusion Pediatric bupropion cases requiring ECMO were rare in this study. Time to initiation and duration of EMCO suggest that the variable onset of hemodynamic instability may delay ECMO initiation. It is incumbent on PCs and medical toxicologists to educate prescribers and pediatricians about bupropion's potential lethality and to consider early transfer to an ECMO center.
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