Monoclonal antibodies targeting small airways: a new perspective for biological therapies in severe asthma.

Carlo Lombardi, Marcello Cottini, Alvise Berti, Pasquale Comberiati
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引用次数: 3

Abstract

Small airway dysfunction (SAD) in asthma is characterized by the inflammation and narrowing of airways with less of 2 mm in diameter between generations 8 and 23 of the bronchial tree. It is now widely accepted that small airways are involved in the pathogenesis of asthma and are a major determinant of airflow obstruction in this disease. In recent years, specialized tests have been developed, such as Impulse Oscillometry (IOS) and Multiple Breath Nitrogen Washout (MBNW) tests, which have been deemed more accurate in detecting SAD than conventional spirometry. Clinical studies show that SAD is associated with more severe bronchial hyperresponsiveness, worse asthma control, and a higher risk of exacerbations. Recent data from a large cohort study showed that the prevalence of SAD in asthma patients increases with asthma severity. Overall, SAD seems to represent a treatable trait, which makes it appealing for asthma control optimization and exacerbation rate reduction, especially in moderate-to-severe asthma.Biologic agents are now available for the treatment of different severe asthma phenotypes and endotypes. However, the effect of these therapies on SAD remains poorly characterized. Literature showing that biologic agents can also favorably improve small airway function is accumulating. In particular, anti-IL5 agents (mepolizumab and benralizumab) seems to have a greater impact on SAD as compared to other biological agents, but direct comparisons in prospective randomized controlled trials are lacking.In this mini-review article, we address the latest evidence on the effect of biological therapies on SAD in patients with severe asthma.

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靶向小气道的单克隆抗体:重度哮喘生物治疗的新视角。
哮喘小气道功能障碍(SAD)的特征是支气管树第8代至第23代之间直径小于2mm的气道炎症和狭窄。目前,人们普遍认为小气道参与哮喘的发病机制,是该病气流阻塞的主要决定因素。近年来,已经开发了专门的测试,如脉冲振荡(IOS)和多次呼吸氮冲洗(MBNW)测试,它们被认为比传统的肺活量测定法更准确地检测SAD。临床研究表明,SAD与更严重的支气管高反应性、更差的哮喘控制和更高的恶化风险相关。最近一项大型队列研究的数据显示,哮喘患者中SAD的患病率随着哮喘严重程度的增加而增加。总的来说,SAD似乎代表了一种可治疗的特征,这使得它对哮喘控制优化和恶化率降低具有吸引力,特别是在中重度哮喘中。生物制剂现在可用于治疗不同的严重哮喘表型和内型。然而,这些疗法对SAD的影响仍然不清楚。文献显示生物制剂也能改善小气道功能。特别是,与其他生物制剂相比,抗il - 5药物(mepolizumab和benralizumab)似乎对SAD的影响更大,但缺乏前瞻性随机对照试验的直接比较。在这篇小型综述文章中,我们讨论了生物疗法对重度哮喘患者SAD影响的最新证据。
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
自引率
0.00%
发文量
6
审稿时长
20 weeks
期刊介绍: Asthma Research and Practice is the official publication of Interasma and publishes cutting edge basic, clinical and translational research in addition to hot topic reviews and debate articles relevant to asthma and related disorders (such as rhinitis, COPD overlapping syndrome, sinusitis). The journal has a specialized section which focusses on pediatric asthma research. Asthma Research and Practice aims to serve as an international platform for the dissemination of research of interest to pulmonologists, allergologists, primary care physicians and family doctors, ENTs and other health care providers interested in asthma, its mechanisms and comorbidities.
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