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生物药物在炎症性肠病、炎症性关节炎或银屑病成人患者中的主动治疗药物监测:临床实践指南。

Proactive therapeutic drug monitoring of biologic drugs in adult patients with inflammatory bowel disease, inflammatory arthritis, or psoriasis: a clinical practice guideline.

机构信息

MAGIC Evidence Ecosystem Foundation, Oslo, Norway

Hcor Research Institute, Hcor Hospital, Sao Paulo, Brazil.

出版信息

BMJ. 2024 Oct 28;387:e079830. doi: 10.1136/bmj-2024-079830.

Abstract

CLINICAL QUESTION

In adult patients with inflammatory bowel disease, inflammatory arthritis (rheumatoid arthritis, spondyloarthritis, psoriatic arthritis), or psoriasis taking biologic drugs, does proactive therapeutic drug monitoring (TDM) improve outcomes as compared with standard care?

CONTEXT AND CURRENT PRACTICE

Standard care for immune mediated inflammatory diseases includes prescribing biologic drugs at pre-determined doses. Dosing may be adjusted reactively, for example with increased disease activity. In proactive TDM, serum drug levels and anti-drug antibodies are measured irrespective of disease activity, and the drug dosing is adjusted to achieve target serum drug levels, usually within pre-specified therapeutic ranges. The role of proactive TDM in clinical practice remains unclear, with conflicting guideline recommendations and emerging evidence from randomised controlled trials.

THE EVIDENCE

Linked systematic review and pairwise meta-analysis which identified 10 trials including 2383 participants. Inflammatory bowel disease, inflammatory arthritis, and psoriasis were grouped together as best current research evidence on proactive TDM did not suggest heterogeneity of effects on outcomes of interest. Proactive TDM of intravenous infliximab during maintenance treatment may increase the proportion of patients who experience sustained disease control or sustained remission without considerable additional harm. For adalimumab, it remains unclear if proactive TDM during maintenance treatment has an effect on sustained disease control or sustained remission. At induction (start) of treatment, proactive TDM of intravenous infliximab may have little or no effect on achieving remission. No eligible trial evidence was available for proactive TDM of adalimumab at induction (start) of treatment. No eligible trial evidence was available for proactive TDM of other biologic drugs in maintenance or at induction (start) of treatment.

RECOMMENDATIONS

The guideline panel issued the following recommendations for patients with inflammatory bowel disease, inflammatory arthritis, or psoriasis:1. A weak recommendation in favour of proactive TDM for intravenous infliximab during maintenance treatment2. A weak recommendation against proactive TDM for adalimumab and other biologic drugs during maintenance treatment3. A weak recommendation against proactive TDM for intravenous infliximab, adalimumab, and other biologic drugs during induction (start) of treatment.

UNDERSTANDING THE RECOMMENDATIONS

When considering proactive TDM, clinicians and patients should engage in shared decision making to ensure patients make choices that reflect their values and preferences. The availability of laboratory assays to implement proactive TDM should also be considered. Further research is warranted and may alter recommendations in the future.

HOW THIS GUIDELINE WAS CREATED

An international panel including patient partners, clinicians, and methodologists produced these recommendations based on a linked systematic review and pairwise meta-analysis which identified 10 trials including 2383 participants. The panel followed standards for trustworthy guidelines and used the GRADE approach, explicitly considering the balance of benefits and harms and burdens of treatment from an individual patient perspective.

摘要

临床问题

在接受生物药物治疗的炎症性肠病、炎症性关节炎(类风湿关节炎、脊柱关节炎、银屑病关节炎)或银屑病的成年患者中,与标准护理相比,主动治疗药物监测(TDM)是否能改善结局?

背景和当前实践

免疫介导的炎症性疾病的标准护理包括以预定剂量开处生物药物。可以根据疾病活动度进行反应性剂量调整,例如疾病活动度增加时。在主动 TDM 中,无论疾病活动度如何,都会测量血清药物水平和抗药物抗体,并调整药物剂量以达到目标血清药物水平,通常在预先规定的治疗范围内。主动 TDM 在临床实践中的作用仍不清楚,指南建议存在冲突,随机对照试验也出现了新的证据。

证据

链接的系统评价和成对的荟萃分析确定了 10 项试验,包括 2383 名参与者。炎症性肠病、炎症性关节炎和银屑病被归为一组,因为关于主动 TDM 的最佳现有研究证据并未表明对所关注结局的影响存在异质性。在维持治疗期间对静脉注射英夫利昔单抗进行主动 TDM 可能会增加经历持续疾病控制或持续缓解的患者比例,而不会造成相当大的额外伤害。对于阿达木单抗,目前尚不清楚维持治疗期间的主动 TDM 是否对持续疾病控制或持续缓解有影响。在诱导(起始)治疗时,对静脉注射英夫利昔单抗进行主动 TDM 可能对实现缓解几乎没有影响。没有符合条件的试验证据可用于诱导(起始)治疗时对阿达木单抗进行主动 TDM。没有符合条件的试验证据可用于维持或诱导(起始)治疗时对其他生物药物进行主动 TDM。

建议

该指南小组为炎症性肠病、炎症性关节炎或银屑病患者发布了以下建议:

  1. 对于在维持治疗期间对静脉注射英夫利昔单抗进行主动 TDM ,建议倾向于使用。

  2. 不建议在维持治疗期间对阿达木单抗和其他生物药物进行主动 TDM。

  3. 不建议在诱导(起始)治疗时对静脉注射英夫利昔单抗、阿达木单抗和其他生物药物进行主动 TDM。

理解建议

在考虑主动 TDM 时,临床医生和患者应进行共同决策,以确保患者做出反映其价值观和偏好的选择。还应考虑实施主动 TDM 的实验室检测的可用性。未来可能需要进一步研究,并可能改变建议。

指南如何制定

一个由患者伙伴、临床医生和方法学家组成的国际小组根据链接的系统评价和成对荟萃分析制定了这些建议,该分析确定了 10 项试验,包括 2383 名参与者。该小组遵循值得信赖的指南标准,并使用 GRADE 方法,从个体患者的角度明确考虑了治疗的获益与危害和负担之间的平衡。

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