Tezepelumab for early-onset severe allergic asthma with persistent airflow limitation and small airway dysfunction: a treatable traits approach.

IF 2.8 Q2 Pharmacology, Toxicology and Pharmaceutics
Drugs in Context Pub Date : 2025-09-25 eCollection Date: 2025-01-01 DOI:10.7573/dic.2025-7-2
Francesco Menzella, Claudio Sorino, Carlo Lombardi, Annamaria Bosi, Silvia Tonin, Lorenzo Corsi, Andrea Ballarin, Marcello Cottini
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引用次数: 0

Abstract

We report the case of an 18-year-old woman with early-onset severe allergic asthma and no other type 2 biomarkers except the presence of IgE, complicated by persistent airflow limitation, air trapping and forced oscillation technique-defined small airway dysfunction, who achieved significant clinical improvement with first-line tezepelumab (TZP) therapy. Initial treatments, including high-dose extrafine-inhaler triple therapy with a beclomethasone-formoterol-glycopyrronium combination, failed to improve asthma control and lung function. Given the discordance between allergic phenotype and treatable traits, such as persistent airflow limitation and small airway dysfunction, TZP, a thymic stromal lymphopoietin inhibitor with broad anti-inflammatory effects, was initiated instead of omalizumab. After 6 months of treatment, the patient showed marked clinical and functional improvement: Asthma Control Test score increased from 12 to 22, forced expiratory volume in 1 second rose from 67% to 95%, residual volume normalized, and forced oscillation technique parameters improved substantially. This case illustrates how the identification of specific treatable traits can guide personalized biologic therapy, even when conventional phenotype-driven algorithms suggest otherwise. In patients with early-onset allergic asthma and atypical functional profiles, TZP may offer a superior therapeutic option by targeting upstream airway inflammation and reversing small airway dysfunction. Our findings support a precision medicine approach in severe asthma, emphasizing multidimensional assessment and biomarker-guided biologic selection.

Tezepelumab用于早发性严重过敏性哮喘伴持续性气流限制和小气道功能障碍:一种可治疗的特征方法。
我们报告了一例18岁的女性早发性严重过敏性哮喘,除了IgE存在外没有其他2型生物标志物,并伴有持续气流限制,空气捕获和强制振荡技术定义的小气道功能障碍,她通过一线tezepelumab (TZP)治疗获得了显着的临床改善。最初的治疗,包括高剂量吸入器和倍氯米松-福莫特罗-甘溴铵联合治疗,未能改善哮喘控制和肺功能。鉴于过敏表型与可治疗特征(如持续气流受限和小气道功能障碍)之间的不一致,采用具有广泛抗炎作用的胸腺基质淋巴生成素抑制剂TZP代替奥玛单抗。治疗6个月后,患者临床和功能均有明显改善:哮喘控制测试评分由12分提高到22分,1秒用力呼气量由67%提高到95%,残气量归一化,用力振荡技术参数有明显改善。这个案例说明了如何识别特定的可治疗特征可以指导个性化的生物治疗,即使当传统的表型驱动算法提示相反。对于早发性过敏性哮喘和非典型功能的患者,TZP可能通过靶向上游气道炎症和逆转小气道功能障碍提供优越的治疗选择。我们的研究结果支持重症哮喘的精准医学方法,强调多维评估和生物标志物引导的生物选择。
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
Drugs in Context
Drugs in Context Medicine-Medicine (all)
CiteScore
5.90
自引率
0.00%
发文量
63
审稿时长
9 weeks
期刊介绍: Covers all phases of original research: laboratory, animal and human/clinical studies, health economics and outcomes research, and postmarketing studies. Original research that shows positive or negative results are welcomed. Invited review articles may cover single-drug reviews, drug class reviews, latest advances in drug therapy, therapeutic-area reviews, place-in-therapy reviews, new pathways and classes of drugs. In addition, systematic reviews and meta-analyses are welcomed and may be published as original research if performed per accepted guidelines. Editorials of key topics and issues in drugs and therapeutics are welcomed. The Editor-in-Chief will also consider manuscripts of interest in areas such as technologies that support diagnosis, assessment and treatment. EQUATOR Network reporting guidelines should be followed for each article type. GPP3 Guidelines should be followed for any industry-sponsored manuscripts. Other Editorial sections may include Editorial, Case Report, Conference Report, Letter-to-the-Editor, Educational Section.
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