Wechsler Michael E, Ford Linda B, Maspero Jorge F, Pavord Ian D, Papi Alberto, Bourdin Arnaud, Watz Henrik, Castro Mario, Nenasheva Natalia M, Tohda Yuji, Langton David, Cardona Guido, Domingo Christian, Park Hae Sim, Chapman Kenneth R, Mao Xuezhou, Zhang Yi, Khan Asif H, Deniz Yamo, Rowe Paul J, Kapoor Upender, Khokhar Faisal A, Mannent Leda P, Ruddy Marcella, Laws Elizabeth, Amin Nikhil, Hardin Megan
Division of Pulmonary, Critical Care and Sleep Medicine, National Jewish Health, Denver, CO, USA.
Asthma and Allergy Center, Bellevue, NE, USA.
Lancet Respir Med. 2022 Jan;10(1):11-25. doi: 10.1016/S2213-2600(21)00322-2. Epub 2021 Sep 28.
Clinical trials have shown treatment benefits of dupilumab in patients with uncontrolled asthma for up to 1 year. This study aimed to evaluate the long-term safety and efficacy of dupilumab in patients with moderate-to-severe asthma, as data for extended treatment with dupilumab beyond 1 year are not available.
TRAVERSE was an open-label extension study in 362 hospitals and clinical centres across 27 countries that assessed the safety and efficacy of dupilumab 300 mg every 2 weeks up to 96 weeks in adults and adolescents (aged 12-84 years) with moderate-to-severe or oral-corticosteroid-dependent severe asthma who had completed a previous dupilumab asthma study (phase 2A EXPEDITION, phase 2B DRI [P2b], phase 3 QUEST, or VENTURE). The primary endpoint was the number and percentage of patients with any treatment-emergent adverse events. Secondary endpoints included annualised exacerbation rate (AER) over the treatment period and change from parent study baseline in pre-bronchodilator FEV, the five-item asthma control questionnaire (ACQ-5), the asthma quality of life questionnaire (AQLQ), type 2 biomarkers (blood eosinophils and serum total IgE), and anti-drug antibodies (ADAs). Statistical analyses were descriptive. We report safety in all enrolled patients, and efficacy in patients with non-oral-corticosteroid-dependent asthma and in subgroups, including patients with a type 2 inflammatory phenotype who received 148 weeks of treatment. This study is registered with ClinicalTrials.gov, NCT02134028.
Between Aug 5, 2014, and Oct 11, 2019, of 2302 patients assessed for eligibility, 2282 adults and adolescents were enrolled (median age 50 years, 62·1% female and 37·9% male). Safety during TRAVERSE was consistent with the known dupilumab safety profile. The proportion of patients reporting treatment-emergent adverse events throughout the study duration was similar to that observed in the parent studies and ranged from 76·3% to 94·7%. The most frequently reported treatment-emergent adverse events were nasopharyngitis (17·5-25·9%), injection-site erythema (2·2-23·4%), and bronchitis (9·3-19·0%). Serious asthma exacerbations (0·5-3·6%) and pneumonia (0·7-2·7%) were the most frequently reported serious adverse events. There were four treatment-emergent adverse events leading to death. Efficacy during TRAVERSE was also consistent with the results of parent studies. In patients who were non-oral-corticosteroid-dependent, AER remained low (0·277-0·327) across parent study and treatment groups, pre-bronchodilator FEV improvements were sustained to the end of treatment at week 96 (mean changes from parent study baseline ranged from 0·22 L [SD 0·44] to 0·33 L [0·44] across parent study and treatment groups), and improvements in ACQ-5 and AQLQ scores were sustained to the last timepoint assessed at week 48. Rapid improvements were observed in pre-bronchodilator FEV and sustained improvements were seen in all outcome measures for patients given dupilumab who previously received placebo in parent studies; further improvements in AER, asthma control, and health-related quality of life were observed in patients who continued receiving dupilumab. Blood eosinophils and serum total IgE decreased progressively. ADA status had no effect on safety or efficacy. In the subgroup of patients with a type 2 inflammatory phenotype followed-up for 148 weeks, AER decreased progressively, and initial lung function improvements were sustained over 148 weeks.
Data show that safety and efficacy of dupilumab in adult and adolescent patients with moderate-to-severe asthma are sustained when treatment is extended up to 148 weeks. These findings therefore support the long-term use of dupilumab in this patient population.
Sanofi and Regeneron Pharmaceuticals.
临床试验已表明度普利尤单抗对控制不佳的哮喘患者具有长达1年的治疗益处。本研究旨在评估度普利尤单抗在中度至重度哮喘患者中的长期安全性和疗效,因为尚无度普利尤单抗超过1年的延长治疗数据。
TRAVERSE是一项在27个国家的362家医院和临床中心开展的开放标签扩展研究,评估每2周一次皮下注射300mg度普利尤单抗长达96周,用于完成过度普利尤单抗哮喘研究(2A期EXPEDITION、2B期DRI [P2b]、3期QUEST或VENTURE)的中度至重度或口服糖皮质激素依赖的重度哮喘成人和青少年(12-84岁)。主要终点是发生任何治疗中出现的不良事件的患者数量及百分比。次要终点包括治疗期间的年化加重率(AER),以及支气管扩张剂使用前第一秒用力呼气容积(FEV₁)、五项哮喘控制问卷(ACQ-5)、哮喘生活质量问卷(AQLQ)、2型生物标志物(血液嗜酸性粒细胞和血清总IgE)和抗药物抗体(ADA)相对于母研究基线的变化。统计分析为描述性分析。我们报告所有入组患者的安全性,以及非口服糖皮质激素依赖哮喘患者和亚组(包括接受148周治疗的2型炎症表型患者)的疗效。本研究已在ClinicalTrials.gov注册,注册号为NCT02134028。
2014年8月5日至2019年10月11日期间,在评估的2302例患者中,共纳入2282例成人和青少年(中位年龄50岁,女性占62.1%,男性占37.9%)。TRAVERSE期间的安全性与已知的度普利尤单抗安全性特征一致。在整个研究期间报告治疗中出现不良事件的患者比例与母研究中观察到的相似,范围为76.3%至94.7%。最常报告的治疗中出现的不良事件为鼻咽炎(17.5%-25.9%)、注射部位红斑(2.2%-23.4%)和支气管炎(9.3%-19.0%)。严重哮喘加重(0.5%-3.6%)和肺炎(0.7%-2.7%)是最常报告的严重不良事件。有4例治疗中出现的不良事件导致死亡。TRAVERSE期间的疗效也与母研究结果一致。在非口服糖皮质激素依赖的患者中,母研究和治疗组的AER均维持在较低水平(0.277-0.327),支气管扩张剂使用前FEV₁的改善在第96周治疗结束时仍持续存在(母研究和治疗组相对于母研究基线的平均变化范围为0.22L [标准差0.44]至0.33L [0.44]),ACQ-5和AQLQ评分的改善持续至第48周评估的最后时间点。对于母研究中先前接受安慰剂治疗、此次给予度普利尤单抗的患者,支气管扩张剂使用前FEV₁迅速改善,所有结局指标均持续改善;继续接受度普利尤单抗治疗的患者,AER、哮喘控制和健康相关生活质量进一步改善。血液嗜酸性粒细胞和血清总IgE逐渐下降。ADA状态对安全性或疗效无影响。在随访148周的2型炎症表型亚组患者中,AER逐渐下降,初始肺功能改善在148周内持续存在。
数据显示,将度普利尤单抗治疗延长至148周时,其在成人和青少年中度至重度哮喘患者中的安全性和疗效得以维持。因此,这些发现支持在该患者群体中长效使用度普利尤单抗。
赛诺菲和再生元制药公司。
