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对乙酰氨基酚中毒的评估与治疗。

Evaluation and treatment of acetaminophen toxicity.

作者信息

Fisher Erik S, Curry Steven C

机构信息

Department of Medical Toxicology, Banner-University Medical Center Phoenix, Phoenix, AZ, United States; Division of Clinical Data Analytics and Decision Support, University of Arizona College of Medicine-Phoenix, Phoenix, AZ, United States; Division of Medical Toxicology and Precision Medicine, University of Arizona College of Medicine-Phoenix, Phoenix, AZ, United States.

Department of Medical Toxicology, Banner-University Medical Center Phoenix, Phoenix, AZ, United States; Division of Clinical Data Analytics and Decision Support, University of Arizona College of Medicine-Phoenix, Phoenix, AZ, United States; Division of Medical Toxicology and Precision Medicine, University of Arizona College of Medicine-Phoenix, Phoenix, AZ, United States.

出版信息

Adv Pharmacol. 2019;85:263-272. doi: 10.1016/bs.apha.2018.12.004. Epub 2019 Jan 22.

Abstract

A review of the typical clinical course, diagnosis and treatment of acetaminophen toxicity is provided. For an acute overdose, most adults must ingest about 12g or more acetaminophen (APAP) before risk of serious hepatotoxicity is of concern. A nomogram of serum APAP concentration vs hours post-ingestion can assist in determining risk of liver injury and need for treatment. However, histories concerning the time of ingestion and the amount of drug ingested are usually unreliable. Peak serum transaminase activities usually occur 48-96h after acute ingestion. It is possible for patients to present in liver failure days after ingestion with undetectable serum APAP concentrations. Patients who have chronically ingested excessive APAP doses and develop hepatotoxicity usually present with such, and renal failure is more common in this population. Current treatment centers on administration of N-acetylcysteine (NAC) to prevent hepatotoxicity, though NAC also improves outcomes in patients who present with acute liver failure. When given early after APAP ingestion, NAC's main mechanism of action is to maintain intracellular glutathione stores so to detoxify the electrophilic APAP metabolite, NAPQI. NAC is generally well-tolerated when given intravenously, with the main concern being anaphylactoid reactions. These reactions usually occur during loading doses and are easily treated with discontinuation of the NAC infusion, administration of antihistamines, and then restarting the loading dose at a slower infusion rate. There is concern that current NAC dosing is not large enough to adequately treat large APAP ingestions. Patients with acute liver failure may be candidates for orthotopic liver transplantation.

摘要

本文对乙酰氨基酚中毒的典型临床病程、诊断及治疗进行了综述。对于急性过量摄入,大多数成年人必须摄入约12克或更多的对乙酰氨基酚(APAP),才会引发严重肝毒性风险。摄入后血清APAP浓度与时间的列线图有助于确定肝损伤风险及是否需要治疗。然而,关于摄入时间和摄入药物量的病史通常不可靠。急性摄入后,血清转氨酶活性峰值通常在48 - 96小时出现。摄入后数天,患者可能出现肝功能衰竭,而此时血清APAP浓度检测不到。长期过量摄入APAP并发生肝毒性的患者通常如此,且该人群中肾衰竭更为常见。目前的治疗以给予N - 乙酰半胱氨酸(NAC)预防肝毒性为主,不过NAC也能改善急性肝功能衰竭患者的预后。在APAP摄入后早期给予时,NAC的主要作用机制是维持细胞内谷胱甘肽储备,从而使亲电子的APAP代谢产物N - 乙酰 - p - 苯醌亚胺(NAPQI)解毒。静脉给予NAC时一般耐受性良好,主要问题是类过敏反应。这些反应通常发生在负荷剂量期间,通过停止NAC输注、给予抗组胺药,然后以较慢的输注速率重新开始负荷剂量即可轻松处理。有人担心目前的NAC剂量不足以充分治疗大量APAP摄入。急性肝功能衰竭患者可能是原位肝移植的候选者。

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