Department of Respiratory Medicine, Royal Brompton and Harefield Hospitals, School of Immunology and Microbial Sciences, King's College London, London, UK.
Department of Medicine, National Jewish Health, Denver, CO, USA.
Lancet Respir Med. 2023 May;11(5):425-438. doi: 10.1016/S2213-2600(22)00492-1. Epub 2023 Jan 23.
Tezepelumab is a human monoclonal antibody that blocks thymic stromal lymphopoietin. The drug has been tested previously in the phase 3 NAVIGATOR (NCT03347279) and SOURCE (NCT03406078) studies, and was subsequently approved as a treatment for severe asthma. This extension study recruited from NAVIGATOR and SOURCE and aimed to evaluate the long-term safety and efficacy of tezepelumab in individuals with severe, uncontrolled asthma.
DESTINATION was a phase 3, multicentre, randomised, double-blind, placebo-controlled, long-term extension study. The study was done across 182 sites (including hospitals, clinics, medical centres, clinical trial centres, and private practices) in 18 countries. Participants (aged 12-80 years) were required to have good treatment compliance in the parent study. Randomisation was stratified by the parent study and all participants were re-randomised. Those who were previously randomised to receive tezepelumab in either parent study continued treatment of subcutaneous tezepelumab (210 mg every 4 weeks); those who were previously randomised to receive placebo in either parent study were re-randomised 1:1 to receive either subcutaneous tezepelumab (210 mg every 4 weeks) or placebo (every 4 weeks) using a randomisation list prepared by a computerised system. Total treatment duration (including the parent studies) was 104 weeks for all groups. Participants, investigators, and site staff were masked to treatment assignment. The primary endpoints were exposure-adjusted incidence of adverse events and serious adverse events and the secondary endpoint was the annualised asthma exacerbation rate; these were assessed from week 0 of the parent studies to week 104 of DESTINATION in all participants who were randomised and who received at least one dose of tezepelumab or placebo in either of the parent studies. The trial is registered with ClinicalTrials.gov, NCT03706079, and is closed to new participants.
Participants were recruited between Jan 7, 2019, and Oct 15, 2020. For individuals who initially received tezepelumab (n=528) in NAVIGATOR, incidence of adverse events over 104 weeks was 49·62 (95% CI 45·16 to 54·39) per 100 patient-years, compared with 62·66 (56·93 to 68·81) for those receiving placebo (n=531; difference -13·04, 95% CI -17·83 to -8·18). For serious adverse events, incidence was 7·85 (6·14 to 9·89) per 100 patient-years for individuals who initially received tezepelumab and 12·45 (9·97 to 15·35) for those who received placebo (difference -4·59, -7·69 to -1·65). In SOURCE, incidence of adverse events was 47·15 (36·06 to 60·56) per 100 patient-years for those who initially received tezepelumab (n=74) and 69·97 (54·54 to 88·40) for those who received placebo (n=76; difference -22·82, -34·77 to -10·01). For serious adverse events, incidence was 13·14 (7·65 to 21·04) per 100 patient-years for those who initially received tezepelumab and 17·99 (10·66 to 28·44) for those who received placebo (difference -4·85, -14·88 to 4·53). Tezepelumab reduced the annualised asthma exacerbation rate over 104 weeks compared with placebo. In participants initially from NAVIGATOR, the annualised asthma exacerbation rate ratio over 104 weeks was 0·42 (95% CI 0·35 to 0·51); in those initially from SOURCE, the ratio over 104 weeks was 0·61 (0·38 to 0·96).
Tezepelumab treatment was well tolerated for up to 2 years and resulted in sustained, clinically meaningful reductions in asthma exacerbations in individuals with severe, uncontrolled asthma. These findings are consistent with previous randomised, placebo-controlled studies and show the long-term safety and sustained efficacy of tezepelumab in individuals with severe, uncontrolled asthma.
AstraZeneca and Amgen.
特泽佩鲁单抗是一种人源单克隆抗体,可阻断胸腺基质淋巴细胞生成素。该药此前已在 3 期 NAVIGATOR(NCT03347279)和 SOURCE(NCT03406078)研究中进行了测试,随后被批准用于治疗严重哮喘。这项扩展研究招募了 NAVIGATOR 和 SOURCE 的参与者,旨在评估特泽佩鲁单抗在严重、未控制的哮喘患者中的长期安全性和疗效。
DESTINATION 是一项 3 期、多中心、随机、双盲、安慰剂对照、长期扩展研究。该研究在 18 个国家的 182 个地点(包括医院、诊所、医疗中心、临床试验中心和私人诊所)进行。参与者(年龄 12-80 岁)在母体研究中需要有良好的治疗依从性。根据母体研究进行分层随机化,所有参与者均重新随机分组。那些在母体研究中之前接受特泽佩鲁单抗治疗的参与者继续接受皮下特泽佩鲁单抗(210mg 每 4 周)治疗;那些在母体研究中之前接受安慰剂治疗的参与者,按照预先准备好的随机分配列表,以 1:1 的比例重新随机分配至皮下特泽佩鲁单抗(210mg 每 4 周)或安慰剂(每 4 周)治疗,该列表由计算机系统生成。所有组别的总治疗持续时间(包括母体研究)为 104 周。参与者、研究者和现场工作人员对治疗分配情况均不知情。主要终点是调整后的不良事件和严重不良事件发生率,次要终点是哮喘恶化的年化发生率;这些终点从母体研究的第 0 周评估到 DESTINATION 的第 104 周,所有随机分组且在母体研究中至少接受过一次特泽佩鲁单抗或安慰剂治疗的参与者均被纳入评估。该试验在 ClinicalTrials.gov 注册,NCT03706079,现已关闭新参与者入组。
参与者于 2019 年 1 月 7 日至 2020 年 10 月 15 日期间入组。对于最初在 NAVIGATOR 中接受特泽佩鲁单抗(n=528)的参与者,104 周内不良事件的发生率为 49.62(95%CI 45.16-54.39)/100 患者年,而接受安慰剂(n=531)的参与者为 62.66(56.93-68.81)/100 患者年(差异-13.04,95%CI-17.83-8.18)。严重不良事件的发生率,最初接受特泽佩鲁单抗的参与者为 7.85(6.14-9.89)/100 患者年,而接受安慰剂的参与者为 12.45(9.97-15.35)/100 患者年(差异-4.59,-7.69-1.65)。在 SOURCE 中,最初接受特泽佩鲁单抗的参与者 104 周内不良事件的发生率为 47.15(36.06-60.56)/100 患者年,而接受安慰剂的参与者为 69.97(54.54-88.40)/100 患者年(差异-22.82,-34.77-10.01)。严重不良事件的发生率,最初接受特泽佩鲁单抗的参与者为 13.14(7.65-21.04)/100 患者年,而接受安慰剂的参与者为 17.99(10.66-28.44)/100 患者年(差异-4.85,-14.88-4.53)。与安慰剂相比,特泽佩鲁单抗可降低 104 周内哮喘恶化的年化发生率。在最初来自 NAVIGATOR 的参与者中,104 周内哮喘恶化的年化发生率比值为 0.42(95%CI 0.35-0.51);在最初来自 SOURCE 的参与者中,104 周内哮喘恶化的年化发生率比值为 0.61(0.38-0.96)。
特泽佩鲁单抗治疗长达 2 年时耐受性良好,可降低严重、未控制的哮喘患者的哮喘恶化发生率,并具有临床意义。这些发现与之前的随机、安慰剂对照研究一致,表明特泽佩鲁单抗在严重、未控制的哮喘患者中的长期安全性和持续疗效。
阿斯利康和安进。
