Airway tryptase levels inform the lack of clinical efficacy of the tryptase inhibitor MTPS9579A in asthma

IF 12.6 1区 医学 Q1 ALLERGY Allergy Pub Date : 2024-09-09 DOI:10.1111/all.16309
Horace Rhee, Lindsay M. Henderson, Rebecca N. Bauer, Kit Wong, Tracy L. Staton, David F. Choy, Prajna Banerjee, Victor Poon, Kenta Yoshida, Chen Chen, Keyi Long, Gizette Sperinde, Steven T. Laing, Nicholas S. Jones, Sara B. Glickstein, Parul Dayal, Alice Fong, Ajit Dash, Grazyna Pulka, Brian Leaker, Dave Singh, Peter Bradding
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Abstract

Background

Tryptase, a mast cell protease, has been identified as a potential therapeutic target in managing patients with refractory asthma. We assessed the efficacy, safety, pharmacokinetics, and pharmacodynamics of MTPS9579A, an anti-tryptase antibody, in a phase 2a randomized trial for patients with uncontrolled asthma and a phase 1c trial to understand activity within the lower respiratory tract.

Methods

Phase 2a patients (n = 134) received 1800 mg MTPS9579A or placebo intravenously every 4 weeks for 48 weeks. The primary endpoint was time to the first composite exacerbation event. Phase 1c patients (n = 27) received one intravenous dose of 300 or 1800 mg MTPS9579A or placebo. Both trials measured MTPS9579A concentrations and effects on tryptase in serum and nasal lining fluid; phase 1c also analyzed bronchial lining fluid.

Results

MTPS9579A did not meet the primary endpoint (hazard ratio = 0.90; 95% CI: 0.55–1.47; p = 0.6835); exacerbation rates in the placebo group were low. Serum and nasal MTPS9579A pharmacokinetics and tryptase levels were consistent with data from healthy volunteers. However, in phase 1c patients, compared to nasal levels, MTPS9579A bronchial concentrations were 6.8-fold lower, and bronchial active and total tryptase levels were higher (119-fold and 30-fold, respectively). Pharmacokinetic/pharmacodynamic modeling predicted intravenous doses of 3800 mg every 4 weeks would be necessary to achieve 95% active tryptase inhibition from baseline.

Conclusions

The MTPS9579A dose tested in the phase 2a study was insufficient to inhibit tryptase in bronchial lining fluid, likely contributing to the observed lack of efficacy.

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气道胰蛋白酶水平说明胰蛋白酶抑制剂 MTPS9579A 对哮喘缺乏临床疗效。
背景:胰蛋白酶是一种肥大细胞蛋白酶,已被确定为治疗难治性哮喘患者的潜在靶点。我们评估了抗胰蛋白酶抗体 MTPS9579A 的疗效、安全性、药代动力学和药效动力学,2a 期随机试验针对未受控制的哮喘患者,1c 期试验旨在了解其在下呼吸道内的活性:2a期患者(n = 134)每4周静脉注射1800毫克MTPS9579A或安慰剂,共48周。主要终点是出现首次综合加重事件的时间。1c 期患者(27 人)静脉注射一次 300 或 1800 毫克 MTPS9579A 或安慰剂。两项试验均测定了血清和鼻腔黏膜液中的MTPS9579A浓度及其对胰蛋白酶的影响;1c期还分析了支气管黏膜液:MTPS9579A未达到主要终点(危险比=0.90;95% CI:0.55-1.47;P=0.6835);安慰剂组的病情恶化率较低。血清和鼻腔 MTPS9579A 药代动力学和胰蛋白酶水平与健康志愿者的数据一致。然而,在1c期患者中,与鼻腔水平相比,MTPS9579A支气管浓度低6.8倍,支气管活性和总胰蛋白酶水平更高(分别为119倍和30倍)。药代动力学/药效学模型预测,每4周静脉注射3800毫克的剂量才能使活性胰蛋白酶抑制率达到基线的95%:结论:2a期研究中测试的MTPS9579A剂量不足以抑制支气管内壁液中的胰蛋白酶,这可能是导致缺乏疗效的原因。
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来源期刊
Allergy
Allergy 医学-过敏
CiteScore
26.10
自引率
9.70%
发文量
393
审稿时长
2 months
期刊介绍: Allergy is an international and multidisciplinary journal that aims to advance, impact, and communicate all aspects of the discipline of Allergy/Immunology. It publishes original articles, reviews, position papers, guidelines, editorials, news and commentaries, letters to the editors, and correspondences. The journal accepts articles based on their scientific merit and quality. Allergy seeks to maintain contact between basic and clinical Allergy/Immunology and encourages contributions from contributors and readers from all countries. In addition to its publication, Allergy also provides abstracting and indexing information. Some of the databases that include Allergy abstracts are Abstracts on Hygiene & Communicable Disease, Academic Search Alumni Edition, AgBiotech News & Information, AGRICOLA Database, Biological Abstracts, PubMed Dietary Supplement Subset, and Global Health, among others.
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