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解毒剂的骨内给药——一项系统评价

Intraosseous administration of antidotes - a systematic review.

作者信息

Elliott Audrée, Dubé Pierre-André, Cossette-Côté Amélie, Patakfalvi Laura, Villeneuve Eric, Morris Martin, Gosselin Sophie

机构信息

a Department of Environmental Health and Toxicology , Institut National de Santé Publique du Québec , Québec , QC , Canada.

b Faculty of Pharmacy , Université Laval , QC , Canada.

出版信息

Clin Toxicol (Phila). 2017 Dec;55(10):1025-1054. doi: 10.1080/15563650.2017.1337122. Epub 2017 Jun 23.

Abstract

CONTEXT

Intraosseous (IO) access is an established route of administration in resuscitation situations. Patients with serious poisoning presenting to the emergency department may require urgent antidote therapy. However, intravenous (IV) access is not always readily available.

OBJECTIVE

This study reviews the current evidence for IO administration of antidotes that could be used in poisoning. The primary outcome was mortality as a surrogate of efficacy. Secondary outcomes included hemodynamic variables, electrocardiographic variables, neurological status, pharmacokinetics outcomes, and adverse effects as defined by each article.

METHODS

A medical librarian created a systematic search strategy for Medline, subsequently translated to Embase, BIOSIS, PubMed, Web of Science, Cochrane, Database of Abstracts of Reviews of Effects (DARE), and the CENTRAL clinical trial register, all of which we searched from inception to 30 June 2016. Interventions included IO administration of selected antidotes. Articles included volunteer studies, poisoning, or other resuscitation contexts such as cardiac arrest, burns, dehydration, seizure, hemorrhagic shock, or undifferentiated shock. We considered all human studies and animal experiments to the exception of in vitro studies. Two reviewers independently selected studies, and a third adjudicated in case of disagreement. Three reviewers extracted all relevant data. Three reviewers evaluated the risk of bias and quality of the articles using specific scales according to each type of study design.

RESULTS

A total of 47 publications (46 articles and one abstract) met our inclusion criteria and described IO administration of 13 different antidotes. These included one case series and 21 case reports describing 26 patients, and 25 animal experiments. Of those, seven human case reports and four animal experiments specifically reported the use of antidotes in poisoning. Human case reports suggested favorable outcomes with IO use of atropine, diazepam, hydroxocobalamin, insulin, lipid emulsion, methylene blue, phentolamine, prothrombin complex concentrate, and sodium bicarbonate. Clinical outcomes varied according to the antidote used. The only reported adverse event was ventricular tachycardia following IO naloxone. Regarding the animal experiments, IO administration of lipid emulsion and of hydroxocobalamin showed improved survival in bupivacaine-poisoned rats and in cyanide-intoxicated swine, respectively. Animal data also suggested an equivalent bio-availability between IO and IV administration for atropine, calcium chloride, dextrose 50%, diazepam, methylene blue, pralidoxime, and sodium bicarbonate. Adverse effect reporting of fat emboli after IO administration of sodium bicarbonate, for example, was conflicting due to the significant heterogeneity in the timing of lung examination across studies.

CONCLUSION

The evidence supporting the use of IO route for the administration of antidotes in a context of poisoning is scarce. The majority of the evidence consists of case reports and animal experiments. Common antidotes such as acetylcysteine, fomepizole, and digoxin-specific antibody fragments have not been studied or reported with the use of the IO route. Despite the low-quality evidence available, IO access is a potential option for antidotal treatments in toxicological resuscitation when IV access is unavailable.

摘要

背景

骨内(IO)通路是复苏情况下既定的给药途径。因严重中毒到急诊科就诊的患者可能需要紧急解毒治疗。然而,静脉(IV)通路并非总是容易建立。

目的

本研究回顾了目前关于IO途径给予可用于中毒治疗的解毒剂的证据。主要结局是作为疗效替代指标的死亡率。次要结局包括血流动力学变量、心电图变量、神经状态、药代动力学结局以及各文章所定义的不良反应。

方法

医学图书馆员为Medline制定了系统检索策略,随后将其翻译为Embase、BIOSIS、PubMed、Web of Science、Cochrane、效果综述摘要数据库(DARE)和CENTRAL临床试验注册库,我们对所有这些数据库从创建至2016年6月30日进行了检索。干预措施包括IO途径给予选定的解毒剂。文章包括志愿者研究、中毒或其他复苏情况,如心脏骤停、烧伤、脱水、癫痫发作、失血性休克或未分化休克。我们纳入了所有人体研究和动物实验,但体外研究除外。两名评审员独立选择研究,如有分歧则由第三名评审员裁决。三名评审员提取所有相关数据。三名评审员根据每种研究设计的特定量表评估文章的偏倚风险和质量。

结果

共有47篇出版物(46篇文章和1篇摘要)符合我们的纳入标准,描述了13种不同解毒剂的IO给药。其中包括1个病例系列和21篇病例报告,描述了26例患者,以及25项动物实验。其中,7篇人体病例报告和4项动物实验专门报告了解毒剂在中毒中的使用。人体病例报告表明,IO途径使用阿托品、地西泮、羟钴胺、胰岛素、脂质乳剂、亚甲蓝、酚妥拉明、凝血酶原复合物浓缩物和碳酸氢钠有良好结局。临床结局因所用解毒剂而异。唯一报告的不良事件是IO途径给予纳洛酮后出现室性心动过速。关于动物实验,脂质乳剂和羟钴胺的IO给药分别在布比卡因中毒大鼠和氰化物中毒猪中显示出存活率提高。动物数据还表明,阿托品、氯化钙、50%葡萄糖、地西泮、亚甲蓝、解磷定和碳酸氢钠的IO给药和IV给药之间生物利用度相当。例如,关于IO途径给予碳酸氢钠后脂肪栓塞的不良反应报告存在矛盾,因为各研究中肺部检查时间存在显著异质性。

结论

支持在中毒情况下使用IO途径给予解毒剂的证据很少。大多数证据包括病例报告和动物实验。常见的解毒剂如乙酰半胱氨酸、甲吡唑和地高辛特异性抗体片段尚未通过IO途径进行研究或报告。尽管现有证据质量较低,但当无法建立IV通路时,IO通路是中毒复苏中解毒治疗的一个潜在选择。

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