对乙酰氨基酚-氨基转移酶乘积预测缓释型对乙酰氨基酚过量所致肝毒性的准确性。
Accuracy of the paracetamol-aminotransferase multiplication product to predict hepatotoxicity in modified-release paracetamol overdose.
作者信息
Wong Anselm, Sivilotti Marco L A, Graudins Andis
机构信息
a Victorian Poisons Information Centre and Austin Toxicology Service , Heidelberg , Australia.
b School of Clinical Sciences, Faculty of Medicine, Nursing and Health Sciences , Monash University , Clayton , Australia.
出版信息
Clin Toxicol (Phila). 2017 Jun;55(5):346-351. doi: 10.1080/15563650.2017.1290253. Epub 2017 Feb 15.
CONTEXT
The paracetamol-aminotransferase multiplication product (APAP × ALT) is a risk predictor of hepatotoxicity that is somewhat independent of time and type of ingestion. However, its accuracy following ingestion of modified-release formulations is not known, as the product has been derived and validated after immediate-release paracetamol overdoses.
OBJECTIVE
The aim of this retrospective cohort study was to evaluate the accuracy of the multiplication product to predict hepatotoxicity in a cohort of patients with modified-release paracetamol overdose.
METHODS
We assessed all patients with modified-release paracetamol overdose presenting to our hospital network from October 2009 to July 2016. Ingestion of a modified-release formulation was identified by patient self-report or retrieval of the original container. Hepatotoxicity was defined as peak alanine aminotransferase ≥1000 IU/L, and acute liver injury (ALI) as a doubling of baseline ALT to more than 50 IU/L.
RESULTS
Of 1989 paracetamol overdose presentations, we identified 73 modified-release paracetamol exposures treated with acetylcysteine. Five patients developed hepatotoxicity, including one who received acetylcysteine within eight hours of an acute ingestion. No patient with an initial multiplication product <10,000 mg/L × IU/L developed hepatotoxicity (sensitivity 100% [95%CI 48%, 100%], specificity 97% [90%, 100%]). Specificity fell to 54% (95%CI: 34, 59%) at a product cut-off point <1500 mg/L × IU/L. When calculated within eight hours of ingestion, mild elevations of the multiplication product fell quickly on repeat testing in patients without ALI or hepatotoxicity.
CONCLUSIONS
In modified-release paracetamol overdose treated with acetylcysteine, the paracetamol-aminotransferase multiplication product demonstrated similar accuracy and temporal profile to previous reports involving mostly immediate-release formulations. Above a cut-point of 10,000 mg/L × IU/L, it was very strongly associated with the development of acute liver injury and hepatotoxicity, especially when calculated more than eight hours post-ingestion. When below 1500 mg/L × IU/L the likelihood of developing hepatotoxicity was very low. Persistently high serial multiplication product calculations were associated with the greatest risk of hepatotoxicity.
背景
对乙酰氨基酚 - 转氨酶乘积(APAP×ALT)是肝毒性的一个风险预测指标,在一定程度上独立于摄入时间和类型。然而,其在服用缓释制剂后的准确性尚不清楚,因为该指标是在速释对乙酰氨基酚过量服用后得出并验证的。
目的
这项回顾性队列研究的目的是评估该乘积在预测服用缓释对乙酰氨基酚过量的患者队列中肝毒性的准确性。
方法
我们评估了2009年10月至2016年7月期间就诊于我院网络的所有服用缓释对乙酰氨基酚过量的患者。通过患者自述或找回原始容器来确定是否服用了缓释制剂。肝毒性定义为谷丙转氨酶峰值≥1000 IU/L,急性肝损伤(ALI)定义为基线ALT翻倍至超过50 IU/L。
结果
在1989例对乙酰氨基酚过量就诊病例中,我们确定了73例接受乙酰半胱氨酸治疗的缓释对乙酰氨基酚暴露病例。5例患者发生了肝毒性,其中1例在急性摄入后8小时内接受了乙酰半胱氨酸治疗。初始乘积<10,000 mg/L×IU/L的患者均未发生肝毒性(敏感性100% [95%CI 48%,100%],特异性97% [90%,100%])。当乘积截断点<1500 mg/L×IU/L时,特异性降至54%(95%CI:34,59%)。在摄入后8小时内计算时,在无ALI或肝毒性的患者中,乘积的轻度升高在重复检测时迅速下降。
结论
在接受乙酰半胱氨酸治疗的缓释对乙酰氨基酚过量病例中,对乙酰氨基酚 - 转氨酶乘积显示出与之前主要涉及速释制剂的报告相似的准确性和时间特征。在截断点高于10,000 mg/L×IU/L时,它与急性肝损伤和肝毒性的发生密切相关,尤其是在摄入后8小时以上计算时。当低于1500 mg/L×IU/L时,发生肝毒性的可能性非常低。持续高的系列乘积计算与肝毒性的最大风险相关。
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