Couillard Simon, Jackson David J, Pavord Ian D, Wechsler Michael E
Faculté de Médecine et des Sciences de la Santé, Université de Sherbrooke, Sherbrooke, QC, Canada.
Guy's Severe Asthma Centre, Guy's and St Thomas' Hospitals, London, England; School of Immunology and Microbial Sciences, King's College, London, England.
Chest. 2025 Feb;167(2):330-342. doi: 10.1016/j.chest.2024.08.045. Epub 2024 Sep 6.
In this installment of the How I Do It series on severe asthma, we tackle the clinical conundrum of choosing the right biologic for the right patient with severe asthma. With six biologics now approved for use in this area comprising four different targeting strategies (anti-Ig E: omalizumab; anti-IL-5 and anti-IL-5-receptor: mepolizumab, reslizumab, and benralizumab; anti-IL-4-receptor: dupilumab; anti-thymic stromal lymphopoietin: tezepelumab), this question is increasingly complex. Recognizing that no head-to-head trial has compared biologics, we based our review on the expected effects of inhibiting different aspects of type 2 airway inflammation, supported whenever possible by clinical trial and real-world data. We use four variations of a case of severe uncontrolled asthma to develop concepts and considerations introduced in the previous installment ("Workup of Severe Asthma") and discuss pregnancy-related, biomarker-related, comorbidity-related, and corticosteroid dependency-related considerations when choosing a biologic. The related questions of deciding when, why, and how to switch from one biologic to another also are discussed. Overall, we consider that the choice of biologics should be based on the available clinical trial data for the desired efficacy outcomes, the biomarker profile of the patient, safety profiles (eg, when pregnancy is considered), and opportunities to target two comorbidities with one biologic. Using systemic and airway biomarkers (blood eosinophils and exhaled nitric oxide [Feno]) and other phenotypic characteristics, we suggest a framework to facilitate therapeutic decision-making. Post hoc studies and new comparative studies are needed urgently to test this framework and to determine whether it allows us to make other clinically useful predictions.
在这一期关于重度哮喘的“我的诊疗方法”系列中,我们将解决为重度哮喘患者选择合适生物制剂这一临床难题。目前有六种生物制剂已获批用于该领域,涵盖四种不同的靶向策略(抗IgE:奥马珠单抗;抗IL-5和抗IL-5受体:美泊利单抗、瑞利珠单抗和贝那利珠单抗;抗IL-4受体:度普利尤单抗;抗胸腺基质淋巴细胞生成素:tezepelumab),这个问题变得越来越复杂。认识到尚无生物制剂的头对头试验,我们的综述基于抑制2型气道炎症不同方面的预期效果,并尽可能得到临床试验和真实世界数据的支持。我们通过一个重度未控制哮喘病例的四种变体,来阐述上一期(“重度哮喘的检查”)中介绍的概念和注意事项,并讨论选择生物制剂时与妊娠、生物标志物、合并症以及皮质类固醇依赖相关的注意事项。还将讨论决定何时、为何以及如何从一种生物制剂转换为另一种生物制剂的相关问题。总体而言,我们认为生物制剂的选择应基于所需疗效结果的现有临床试验数据、患者的生物标志物特征、安全性特征(例如考虑妊娠时)以及用一种生物制剂针对两种合并症的机会。利用全身和气道生物标志物(血液嗜酸性粒细胞和呼出一氧化氮 [Feno])以及其他表型特征,我们提出一个框架以促进治疗决策。迫切需要进行事后研究和新的比较研究来检验这个框架,并确定它是否能让我们做出其他对临床有用的预测。