对重症监护病房中接受右美托咪定持续输注的儿童所出现不良事件的评估。
Evaluation of adverse events noted in children receiving continuous infusions of dexmedetomidine in the intensive care unit.
作者信息
Honey Brooke L, Harrison Donald L, Gormley Andrew K, Johnson Peter N
机构信息
Department of Pharmacy, Clinical and Administrative Sciences, Tulsa at University of Oklahoma College of Pharmacy, Tulsa, Oklahoma.
出版信息
J Pediatr Pharmacol Ther. 2010 Jan;15(1):30-7.
OBJECTIVES
Dexmedetomidine is an α(2)-adrenergic receptor agonist with sedative and analgesic effects in mechanically ventilated adults and children. Safety and efficacy data are limited in children. The purpose of this study is to retrospectively identify the incidence and types of adverse events noted in children receiving continuous infusions of dexmedetomidine and evaluate potential risk factors for adverse events.
METHODS
Between July 1, 2006, and July 31, 2007, data were collected on all children (< 18 years) who received continuous infusions of dexmedetomidine. Data collection included demographics, dexmedetomidine regimen, and type/number of adverse events. The primary endpoint was the total number of adverse events noted, including: transient hypertension, hypotension, neurological manifestations, apnea, and bradycardia. Secondary endpoints included categorization of each type of adverse event and an assessment of risk factors. A logistic regression model was used to assess the relationship of adverse events with independent variables including length of ICU stay, cumulative dose, peak infusion rate, duration of therapy, PRISM III score, and bolus dose.
RESULTS
Thirty-six patients received dexmedetomidine representing 41 infusions. The median age was 16 months (range, 0.1-204 months) and median PRISM III score was 2 (range, 0-18). Eighteen (43.9%) patients received a bolus dose of dexmedetomidine. The median cumulative dose (mcg/kg) and peak dose (mcg/kg/hr) were 8.5 (range, 2.2-193.7) and 0.5 (range, 0.2-0.7), respectively. Dexmedetomidine was continued for a median of 20 (range, 3-263) hours. Six (14.6%) patients were slowly tapered off the continuous infusions. Twenty-one adverse events were noted in 17 patients, including 4 neurologic manifestations. Fourteen patients required interventions for adverse events. ICU length of stay was the only independent risk factor (p=0.036) for development of adverse events.
CONCLUSIONS
Several potential adverse events were noted with dexmedetomidine continuous infusions including possible neurological manifestations. Further studies are needed looking at adverse events associated with dexmedetomidine use in the pediatric population.
目的
右美托咪定是一种α(2)-肾上腺素能受体激动剂,对接受机械通气的成人和儿童具有镇静和镇痛作用。儿童中的安全性和有效性数据有限。本研究的目的是回顾性确定接受持续输注右美托咪定的儿童中不良事件的发生率和类型,并评估不良事件的潜在风险因素。
方法
在2006年7月1日至2007年7月31日期间,收集了所有接受持续输注右美托咪定的儿童(<18岁)的数据。数据收集包括人口统计学、右美托咪定治疗方案以及不良事件的类型/数量。主要终点是记录的不良事件总数,包括:短暂性高血压、低血压、神经学表现、呼吸暂停和心动过缓。次要终点包括对每种不良事件类型进行分类以及评估风险因素。使用逻辑回归模型评估不良事件与独立变量之间的关系,这些独立变量包括重症监护病房(ICU)住院时间、累积剂量、峰值输注速率、治疗持续时间、小儿死亡风险评分(PRISM III)和推注剂量。
结果
36例患者接受了右美托咪定治疗,共进行了41次输注。中位年龄为16个月(范围为0.1-204个月),中位PRISM III评分为2分(范围为0-18分)。18例(43.9%)患者接受了右美托咪定推注剂量。中位累积剂量(微克/千克)和峰值剂量(微克/千克/小时)分别为8.5(范围为2.2-193.7)和0.5(范围为0.2-0.7)。右美托咪定持续输注的中位时间为20小时(范围为3-263小时)。6例(14.6%)患者逐渐减少持续输注剂量。17例患者出现了21次不良事件,包括4例神经学表现。14例患者因不良事件需要进行干预。ICU住院时间是发生不良事件的唯一独立风险因素(p=0.036)。
结论
右美托咪定持续输注时出现了几种潜在的不良事件,包括可能的神经学表现。需要进一步研究小儿人群中与使用右美托咪定相关的不良事件。
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