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硫唑嘌呤代谢物的实际应用改变了炎症性肠病的临床管理。

Real-World Use of Azathioprine Metabolites Changes Clinical Management of Inflammatory Bowel Disease.

作者信息

Wilson Laura, Tuson Stephanie, Yang Lufang, Loomes Dustin

机构信息

Division of Gastroenterology, Vancouver Island IBD Clinic, Victoria, British Columbia, Canada.

Department of Medicine, University of British Columbia, Vancouver, British Columbia, Canada.

出版信息

J Can Assoc Gastroenterol. 2020 Mar 4;4(3):101-109. doi: 10.1093/jcag/gwaa005. eCollection 2021 Jun.

Abstract

BACKGROUND

Thiopurines such as 6-mercaptopurine and azathioprine have complex metabolism, resulting in significant inter-individual differences in clinical efficacy and risk of drug toxicity, making conventional weight-based dosing inaccurate and potentially unsafe. Therapeutic drug monitoring (TDM) of thiopurine metabolites improves clinical outcomes through dose optimization and toxicity monitoring. Despite evidence for TDM, use is limited, due in part to test availability and awareness. The objectives of this study were twofold: (1) to investigate how thiopurine TDM impacts clinical management of IBD patients and (2) to evaluate proportion of patients outside therapeutic 6TGN levels or exhibiting signs of toxicity.

METHODS

Patients who received thiopurine TDM as part of routine care underwent chart review of demographics, disease activity, medication dosing, metabolite levels, and adverse events. Changes in clinical management following TDM were measured. Additionally, we conducted a retrospective review of clinical decision making blinded and unblinded to TDM result.

RESULTS

A total of 92 IBD patients were included. Levels of 6TGN were therapeutic in 29% of patients. 6TGN levels correlated weakly with weight-based dosing ( = 0.057, = 0.02). Adverse reactions were observed in 6.5%. TDM informed clinical management in 64%. Significantly more changes to clinical management occurred in those with active disease than in remission (73% versus 48%; = 0.02) and in those on mono- versus combination therapy (48% versus 27.5%; = 0.03).

CONCLUSIONS

TDM informs clinical decision making in over two-thirds of patients. The demonstrated poor efficacy of weight-based dosing and impact of TDM on clinical management contributes to the evidence supporting the need for greater availability and uptake of thiopurine TDM.

摘要

背景

硫唑嘌呤等硫嘌呤类药物具有复杂的代谢过程,导致临床疗效和药物毒性风险存在显著个体差异,使得传统的基于体重的给药方式不准确且可能不安全。硫嘌呤代谢物的治疗药物监测(TDM)通过优化剂量和监测毒性来改善临床结局。尽管有TDM的相关证据,但由于检测的可及性和认知度等原因,其应用有限。本研究的目的有两个:(1)研究硫嘌呤TDM如何影响炎症性肠病(IBD)患者的临床管理;(2)评估6-硫鸟嘌呤核苷酸(6TGN)水平超出治疗范围或出现毒性迹象的患者比例。

方法

将接受硫嘌呤TDM作为常规治疗一部分的患者的人口统计学、疾病活动度、药物剂量、代谢物水平和不良事件等信息进行病历审查。测量TDM后临床管理的变化。此外,我们对未了解和了解TDM结果的临床决策进行了回顾性审查。

结果

共纳入92例IBD患者。29%的患者6TGN水平处于治疗范围内。6TGN水平与基于体重的给药相关性较弱(r = 0.057,P = 0.02)。观察到6.5%的患者出现不良反应。64%的患者中TDM为临床管理提供了依据。与缓解期患者相比,活动期患者临床管理的变化显著更多(73%对48%;P = 0.02),单药治疗患者与联合治疗患者相比也是如此(48%对27.5%;P = 0.03)。

结论

TDM为超过三分之二的患者的临床决策提供了依据。基于体重给药的疗效不佳以及TDM对临床管理的影响,为支持更广泛地提供和采用硫嘌呤TDM提供了证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d361/8158651/9233105b1cee/gwaa005f0001.jpg

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