Assessing early therapeutic drug monitoring of adalimumab as a predictor of treatment efficacy and immunogenicity in rheumatic diseases: "early therapeutic drug monitoring of adalimumab".

IF 2.9 3区医学 Q2 RHEUMATOLOGY

Clinical Rheumatology Pub Date : 2025-01-18 DOI:10.1007/s10067-025-07307-0

Patricia Ortiz-Fernández, Carles Iniesta-Navalón, Elena Urbieta-Sanz, Juan José Gascón-Cánovas

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Abstract

Introduction: Therapeutic drug monitoring (TDM) in inflammatory rheumatic diseases (RMDs) is gaining interest. However, there are unresolved questions about the best practices for implementing TDM effectively in clinical settings.

Objective: The primary objective of this study was to evaluate whether early TDM of adalimumab predicts drug survival at 52 weeks in patients with RMDs. The secondary objective was to identify factors associated with pharmacokinetic failure and treatment discontinuation.

Methods: A retrospective cohort study included patients aged ≥ 18 years with RMDs who initiated adalimumab therapy. Early TDM was performed within the first 26 weeks, and adalimumab trough levels (ATL) and anti-drug antibodies were measured. Drug survival was assessed at 52 weeks and defined as the time from adalimumab initiation to discontinuation for any reason. Multivariate analyses were conducted to identify factors influencing outcomes.

Results: The study included 194 patients, of whom 56.7% exhibited ATL below the therapeutic range during the first 26 weeks. In the multivariate analysis, subtherapeutic concentrations were significantly associated with higher weight (OR = 1.02; p = 0.040) and ankylosing spondylitis diagnosis (OR = 3.68; p < 0.001). At 52 weeks, 43.8% of patients had discontinued adalimumab. Low ATL (< 1 µg/mL) was strongly associated with treatment discontinuation (OR = 7.31; p < 0.001), while concomitant methotrexate reduced this risk (OR = 0.46; p = 0.026).

Conclusions: Early TDM of adalimumab predicts drug persistence and underscores its clinical relevance as a proactive tool to guide personalized treatment and reduce the risk of treatment failure. These findings highlight the importance of incorporating TDM into routine practice to optimize therapeutic outcomes. Key Points • Early TDM of adalimumab in rheumatic diseases shows that low drug exposure predicts reduced drug survival at 52 weeks. • Approximately half of the patients exhibit low adalimumab exposure with the standard dose (40 mg every other week). • Body weight and methotrexate use significantly impact adalimumab levels. • Immunogenicity, found in 14.4% of patients with low ADL levels, underscores the need for early ADA detection to prevent non-response and discontinuation.

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评估阿达木单抗早期治疗药物监测作为风湿病治疗疗效和免疫原性的预测指标：“阿达木单抗早期治疗药物监测”。

治疗性药物监测（TDM）在炎症性风湿病（RMDs）中的应用越来越受到关注。然而，关于在临床环境中有效实施TDM的最佳实践仍存在未解决的问题。目的：本研究的主要目的是评估阿达木单抗的早期TDM是否能预测rmd患者52周的药物生存。次要目的是确定与药代动力学失效和停药相关的因素。方法：一项回顾性队列研究纳入了年龄≥18岁且开始阿达木单抗治疗的rmd患者。在前26周内进行早期TDM，并测量阿达木单抗谷水平（ATL）和抗药物抗体。药物生存期在52周时进行评估，并定义为从阿达木单抗开始到因任何原因停药的时间。进行多变量分析以确定影响结果的因素。结果：该研究纳入194例患者，其中56.7%的患者在前26周出现ATL低于治疗范围。在多变量分析中，亚治疗浓度与体重增加显著相关(OR = 1.02；p = 0.040)和强直性脊柱炎诊断(OR = 3.68；结论：阿达木单抗的早期TDM可预测药物持久性，并强调其作为指导个性化治疗和降低治疗失败风险的前瞻性工具的临床相关性。这些发现强调了将TDM纳入常规实践以优化治疗结果的重要性。•阿达木单抗在风湿病中的早期TDM显示，低药物暴露可预测52周时药物生存期降低。•大约一半的患者在标准剂量（每隔一周40mg）下表现出低剂量的阿达木单抗暴露。•体重和甲氨蝶呤的使用显著影响阿达木单抗水平。•14.4%的低ADL水平患者存在免疫原性，这强调了早期检测ADA以防止无反应和停药的必要性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Clinical Rheumatology 医学-风湿病学

CiteScore

6.90

自引率

2.90%

发文量

441

审稿时长

3 months

期刊介绍： Clinical Rheumatology is an international English-language journal devoted to publishing original clinical investigation and research in the general field of rheumatology with accent on clinical aspects at postgraduate level. The journal succeeds Acta Rheumatologica Belgica, originally founded in 1945 as the official journal of the Belgian Rheumatology Society. Clinical Rheumatology aims to cover all modern trends in clinical and experimental research as well as the management and evaluation of diagnostic and treatment procedures connected with the inflammatory, immunologic, metabolic, genetic and degenerative soft and hard connective tissue diseases.