克罗恩病中硫唑嘌呤相关不良事件的临床预测因素
Clinical predictors of thiopurine-related adverse events in Crohn's disease.
作者信息
Moran Gordon W, Dubeau Marie-France, Kaplan Gilaad G, Yang Hong, Eksteen Bertus, Ghosh Subrata, Panaccione Remo
机构信息
Gordon W Moran, Marie-France Dubeau, Gilaad G Kaplan, Hong Yang, Bertus Eksteen, Subrata Ghosh, Remo Panaccione, Inflammatory Bowel Disease Clinic, Division of Gastroenterology, Department of Medicine, Cumming School of Medicine, University of Calgary, Alberta T2N 1N4, Canada.
出版信息
World J Gastroenterol. 2015 Jul 7;21(25):7795-804. doi: 10.3748/wjg.v21.i25.7795.
AIM
To determine the incidence and predictors of thiopurine-related adverse events.
METHODS
Subjects with Crohn's disease who were followed in the Alberta Inflammatory Bowel Disease Consortium patient database registry were identified. Retrospective chart review was conducted between August 5th, 2010 and June 1st, 2012. We collected data on: age at diagnosis; sex; disease location and behaviour at time of prescribing thiopurine; perianal fistulising disease at or prior to thiopurine prescription; smoking status at time of thiopurine prescription, use of corticosteroid within 6 mo of diagnosis; dosage, age at onset, and cessation of 5-aminosalicyclic acid (5-ASA); anti-tumour necrosis factor medication exposure and intestinal resection before thiopurine prescription. The primary outcome of interest was the first adverse event that led to discontinuation of the first thiopurine medication used. Logistic regression models were used to associate clinical characteristics with outcomes after adjusting for potential confounders. Risk estimates were presented as odds ratios (OR) with 95% CI. Effect modification by age and sex were explored.
RESULTS
Our cohort had a median follow-up duration of 5.8 years [interquartile range (IQR 25th-75th) 2.7-9.1]. Thiopurine therapy was discontinued in 31.3% of patients because of: hypersensitivity reactions (7.1%), acute pancreatitis (6.2%), gastrointestinal intolerance (5.4%), leucopenia (3.7%), hepatotoxicity (3.4%), infection (1.1%) and other reasons (4.3%). A higher incidence of thiopurine withdrawal was observed in patients over the age of 40 (39.4%, P = 0.007). A sex-by-age interaction (P = 0.04) was observed. Females older than 40 years of age had an increased risk of thiopurine discontinuation due to an adverse event (age above 40 vs age below 40, adjusted OR = 2.8; 95%CI: 1.4-5.6). In contrast, age did not influence thiopurine withdrawal in males (age above 40 vs below 40, adjusted OR = 0.9; 95%CI: 0.4-2.1). Other clinical variables (disease location and phenotype, perianal disease, smoking history, history of intestinal resection and prior 5-ASA or corticosteroid use) were not associated with an increased risk an adverse event leading to therapy cessation.
CONCLUSION
Thiopurine withdrawal due to adverse events is commoner in women over the age of 40 at prescription. These findings need to be replicated in other cohorts.
目的
确定硫唑嘌呤相关不良事件的发生率及预测因素。
方法
在艾伯塔炎症性肠病联盟患者数据库登记处随访的克罗恩病患者中进行筛选。于2010年8月5日至2012年6月1日进行回顾性病历审查。我们收集了以下数据:诊断时的年龄;性别;开具硫唑嘌呤时的疾病部位及病情;硫唑嘌呤处方时或之前的肛周瘘管病;硫唑嘌呤处方时的吸烟状况;诊断后6个月内使用皮质类固醇的情况;5-氨基水杨酸(5-ASA)的剂量、开始使用年龄及停用时间;硫唑嘌呤处方前使用抗肿瘤坏死因子药物的情况及肠道切除术情况。主要关注的结果是导致首次使用的硫唑嘌呤药物停用的首个不良事件。在对潜在混杂因素进行调整后,使用逻辑回归模型将临床特征与结果相关联。风险估计以比值比(OR)及95%置信区间(CI)表示。探讨年龄和性别对效应的修饰作用。
结果
我们的队列中位随访时间为5.8年[四分位间距(IQR 第(25)百分位数 - 第(75)百分位数)2.7 - 9.1]。31.3%的患者因以下原因停用硫唑嘌呤治疗:过敏反应(7.1%)、急性胰腺炎(6.2%)、胃肠道不耐受(5.4%)、白细胞减少(3.7%)、肝毒性(3.4%)、感染(1.1%)及其他原因(4.3%)。40岁以上患者硫唑嘌呤停药发生率更高(39.4%;P = 0.007)。观察到年龄与性别的交互作用(P = 0.04)。40岁以上女性因不良事件导致硫唑嘌呤停药的风险增加(40岁以上与40岁以下相比,调整后的OR = 2.8;95%CI:1.4 - 5.6)。相比之下,年龄对男性硫唑嘌呤停药无影响(40岁以上与40岁以下相比,调整后的OR = 0.9;95%CI:0.4 - 2.1)。其他临床变量(疾病部位及表型、肛周疾病、吸烟史、肠道切除史及既往使用5-ASA或皮质类固醇的情况)与导致治疗停止的不良事件风险增加无关。
结论
处方时年龄超过40岁的女性因不良事件停用硫唑嘌呤更为常见。这些发现需要在其他队列中进行重复验证。
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