炎症性肠病中硫嘌呤诱导的肝毒性的早期预测
Early prediction of thiopurine-induced hepatotoxicity in inflammatory bowel disease.
作者信息
Wong D R, Coenen M J H, Derijks L J J, Vermeulen S H, van Marrewijk C J, Klungel O H, Scheffer H, Franke B, Guchelaar H-J, de Jong D J, Engels L G J B, Verbeek A L M, Hooymans P M
机构信息
Sittard-Geleen, The Netherlands.
Nijmegen, The Netherlands.
出版信息
Aliment Pharmacol Ther. 2017 Feb;45(3):391-402. doi: 10.1111/apt.13879. Epub 2016 Dec 12.
BACKGROUND
Hepatotoxicity, gastrointestinal complaints and general malaise are common limiting adverse reactions of azathioprine and mercaptopurine in IBD patients, often related to high steady-state 6-methylmercaptopurine ribonucleotide (6-MMPR) metabolite concentrations.
AIM
To determine the predictive value of 6-MMPR concentrations 1 week after treatment initiation (T1) for the development of these adverse reactions, especially hepatotoxicity, during the first 20 weeks of treatment.
METHODS
The cohort study consisted of the first 270 IBD patients starting thiopurine treatment as part of the Dutch randomised-controlled trial evaluating pre-treatment thiopurine S-methyltransferase genotype testing (ClinicalTrials.gov NCT00521950). Blood samples for metabolite assessment were collected at T1. Hepatotoxicity was defined by alanine aminotransaminase elevations >2 times the upper normal limit or a ratio of alanine aminotransaminase/alkaline phosphatase ≥5.
RESULTS
Forty-seven patients (17%) presented hepatotoxicity during the first 20 weeks of thiopurine treatment. A T1 6-MMPR threshold of 3615 pmol/8 × 10 erythrocytes was defined. Analysis of patients on stable thiopurine dose (n = 174) showed that those exceeding the 6-MMPR threshold were at increased risk of hepatotoxicity: OR = 3.8 (95% CI: 1.8-8.0). Age, male gender and BMI were significant determinants. A predictive algorithm was developed based on these determinants and the 6-MMPR threshold to assess hepatotoxicity risk [AUC = 0.83 (95% CI: 0.75-0.91)]. 6-MMPR concentrations above the threshold also correlated with gastrointestinal complaints: OR = 2.4 (95% CI: 1.4-4.3), and general malaise: OR = 2.0 (95% CI: 1.1-3.7).
CONCLUSIONS
In more than 80% of patients, thiopurine-induced hepatotoxicity could be explained by elevated T1 6-MMPR concentrations and the independent risk factors age, gender and BMI, allowing personalised thiopurine treatment in IBD to prevent early failure.
背景
肝毒性、胃肠道不适和全身不适是炎症性肠病(IBD)患者使用硫唑嘌呤和巯嘌呤时常见的限制不良反应,通常与高稳态6 - 甲基巯基嘌呤核糖核苷酸(6 - MMPR)代谢物浓度有关。
目的
确定治疗开始后1周(T1)时6 - MMPR浓度对这些不良反应,尤其是治疗前20周内肝毒性发生的预测价值。
方法
队列研究包括荷兰一项评估治疗前硫嘌呤S - 甲基转移酶基因型检测的随机对照试验(ClinicalTrials.gov NCT00521950)中开始硫嘌呤治疗的前270例IBD患者。在T1时采集用于代谢物评估的血样。肝毒性定义为丙氨酸氨基转移酶升高超过正常上限的2倍或丙氨酸氨基转移酶/碱性磷酸酶比值≥5。
结果
47例患者(17%)在硫嘌呤治疗的前20周出现肝毒性。定义了T1时6 - MMPR阈值为3615 pmol/8×10红细胞。对硫嘌呤剂量稳定的患者(n = 174)分析显示,超过6 - MMPR阈值的患者肝毒性风险增加:比值比(OR)= 3.8(95%置信区间:1.8 - 8.0)。年龄、男性性别和体重指数(BMI)是显著的决定因素。基于这些决定因素和6 - MMPR阈值开发了一种预测算法,以评估肝毒性风险[AUC = 0.83(95%置信区间:0.75 - 0.91)]。6 - MMPR浓度高于阈值也与胃肠道不适相关:OR = 2.4(95%置信区间:1.4 - 4.3),以及全身不适:OR = 2.0(95%置信区间:1.1 - 3.7)。
结论
在超过80%的患者中,硫嘌呤诱导的肝毒性可由T1时升高的6 - MMPR浓度以及年龄、性别和BMI等独立风险因素解释,这使得IBD患者能够进行个性化硫嘌呤治疗以预防早期治疗失败。
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