Department of Clinical Haematology, Guy's and St Thomas' NHS Foundation Trust, London, UK.
University of Tennessee Health Science Center at Memphis, Memphis, TN, USA.
Lancet Haematol. 2021 May;8(5):e323-e333. doi: 10.1016/S2352-3026(21)00059-4. Epub 2021 Apr 7.
For decades, patients with sickle cell disease have had only a limited number of therapies available. In 2019, voxelotor (1500 mg), an oral once-daily sickle haemoglobin polymerisation inhibitor, was approved in the USA for the treatment of sickle cell disease in patients aged 12 years and older on the basis of HOPE trial data. To further describe the applicability of voxelotor as a treatment for this chronic illness, we report the long-term efficacy and safety of this drug at 72 weeks of treatment; the conclusion of the placebo-controlled HOPE trial.
HOPE is an international, randomised, double-blind, placebo-controlled, phase 3 trial done at 60 clinical sites in Canada, Egypt, France, Italy, Jamaica, Kenya, Lebanon, Netherlands, Oman, Turkey, the USA, and the UK. Patients (aged 12-65 years) with confirmed sickle cell disease, a haemoglobin concentration of 5·5-10·5 g/dL at enrolment, and who had between one and ten vaso-occlusive crisis events in the previous 12 months were enrolled. Patients receiving regularly scheduled transfusion therapy, who had received a transfusion in the previous 60 days, or who had been admitted to hospital for a vaso-occlusive crisis in the previous 14 days were excluded. Patients were randomly assigned (1:1:1) to receive either once-daily oral voxelotor 1500 mg, voxelotor 900 mg, or placebo for 72 weeks. Randomisation was done centrally by use of an interactive web response system, stratified by baseline hydroxyurea use (yes vs no), age group (adolescents [12 to <18 years] vs adults [18 to 65 years]), and geographic region (North America vs Europe vs other). The primary endpoint (already reported) was the proportion of patients who achieved a haemoglobin response at week 24. In this final analysis, we report prespecified long-term efficacy assessments by intention to treat, including changes in haemoglobin concentrations from baseline to week 72, changes in the concentration of haemolysis markers (absolute and percentage reticulocytes, indirect bilirubin concentrations, and lactate dehydrogenase concentrations) from baseline to week 72, the annualised incidence of vaso-occlusive crises, and patient functioning, as assessed with the Clinical Global Impression of Change (CGI-C) scale. Safety was assessed in patients who received at least one dose of treatment (modified intention-to-treat population). This trial is registered with ClinicalTrials.gov, NCT03036813.
Between Dec 5, 2016, and May 3, 2018, 449 patients were screened, of whom 274 were randomly assigned to the voxelotor 1500 mg group (n=90), the voxelotor 900 mg group (n=92), or the placebo group (n=92). At week 72, the adjusted mean change in haemoglobin concentration from baseline was 1·0 g/dL (95% CI 0·7 to -1·3) in the voxelotor 1500 mg group, 0·5 g/dL (0·3 to -0·8) in the voxelotor 900 mg group, and 0·0 g/dL (-0·3 to 0·3) in the placebo group, with a significant difference observed between the voxelotor 1500 mg group and the placebo group (p<0·0001), and between the voxelotor 900 mg group and the placebo group (p=0·014). Significant improvements in markers of haemolysis, as assessed by the difference in adjusted mean percentage change from baseline at week 72 versus placebo, were observed in the voxelotor 1500 mg group in indirect bilirubin concentrations (-26·6% [95% CI -40·2 to -12·9]) and percentage of reticulocytes (-18·6% [-33·9 to -3·3]). The proportion of patients in the voxelotor 1500 mg group who were rated as "moderately improved" or "very much improved" at week 72 with the CGI-C was significantly greater than in the placebo group (39 [74%] of 53 vs 24 [47%] of 51; p=0·0057). Serious adverse events unrelated to sickle cell disease were reported in 25 (28%) of 88 patients in the voxelotor 1500 mg group, 20 (22%) of 92 patients in the voxelotor 900 mg group, and 23 (25%) of 91 patients in the placebo group. Grade 3 or 4 adverse events were infrequent (ie, occurred in <10% of patients); anaemia occurred in five or more patients (two [2%] patients in the voxelotor 1500 mg group, seven [8%] patients in the voxelotor 900 mg group, and three [3%] patients in the placebo group). Of all 274 patients, six (2%) deaths occurred during the study (two deaths in each treatment group), all of which were judged as unrelated to treatment.
Voxelotor 1500 mg resulted in rapid and durable improvements in haemoglobin concentrations maintained over 72 weeks and has potential to address the substantial morbidity associated with haemolytic anaemia in sickle cell disease.
Global Blood Therapeutics.
几十年来,患有镰状细胞病的患者只有有限数量的治疗方法可用。2019 年,口服每日一次的镰状血红蛋白聚合抑制剂沃罗特(1500mg)在美国获得批准,用于治疗 12 岁及以上的镰状细胞病患者,其疗效基于 HOPE 试验数据。为了进一步描述沃罗特作为这种慢性疾病的治疗方法的适用性,我们报告了这种药物治疗 72 周的长期疗效和安全性;这是安慰剂对照 HOPE 试验的结论。
HOPE 是一项国际性、随机、双盲、安慰剂对照的 3 期临床试验,在加拿大、埃及、法国、意大利、牙买加、肯尼亚、黎巴嫩、荷兰、阿曼、土耳其、美国和英国的 60 个临床地点进行。入选患者(年龄 12-65 岁)确诊为镰状细胞病,入组时血红蛋白浓度为 5.5-10.5g/dL,并且在过去 12 个月内有 1-10 次血管阻塞性危象事件。正在接受定期输血治疗、在过去 60 天内接受过输血或在过去 14 天内因血管阻塞性危象住院的患者被排除在外。患者随机(1:1:1)接受每日一次口服沃罗特 1500mg、沃罗特 900mg 或安慰剂治疗 72 周。随机化通过使用交互式网络响应系统进行,按基线使用羟基脲(是与否)、年龄组(青少年[12 至<18 岁]与成年人[18 至 65 岁])和地理区域(北美与欧洲与其他地区)分层。主要终点(已报道)是在第 24 周达到血红蛋白反应的患者比例。在这项最终分析中,我们报告了按意向治疗进行的预先指定的长期疗效评估,包括从基线到第 72 周血红蛋白浓度的变化、从基线到第 72 周血红蛋白分解标志物(绝对和百分比网织红细胞、间接胆红素浓度和乳酸脱氢酶浓度)浓度的变化、血管阻塞性危象的年发生率以及患者功能,由临床总体印象变化(CGI-C)量表评估。至少接受一剂治疗的患者(改良意向治疗人群)进行了安全性评估。该试验在 ClinicalTrials.gov 注册,NCT03036813。
2016 年 12 月 5 日至 2018 年 5 月 3 日期间,共有 449 名患者接受了筛查,其中 274 名患者被随机分配至沃罗特 1500mg 组(n=90)、沃罗特 900mg 组(n=92)或安慰剂组(n=92)。第 72 周时,与基线相比,血红蛋白浓度的调整平均变化分别为沃罗特 1500mg 组 1.0g/dL(95%CI 0.7 至-1.3)、沃罗特 900mg 组 0.5g/dL(0.3 至-0.8)和安慰剂组 0.0g/dL(-0.3 至 0.3),沃罗特 1500mg 组与安慰剂组之间存在显著差异(p<0.0001),沃罗特 900mg 组与安慰剂组之间也存在显著差异(p=0.014)。从基线到第 72 周的调整平均百分比变化差异评估,沃罗特 1500mg 组的间接胆红素浓度(-26.6%[95%CI-40.2 至-12.9])和网织红细胞百分比(-18.6%[-33.9 至-3.3])的血红蛋白分解标志物显著改善。第 72 周时,CGI-C 评估为“中度改善”或“非常改善”的患者比例,沃罗特 1500mg 组显著高于安慰剂组(39[74%]的 53 例与 24[47%]的 51 例;p=0.0057)。沃罗特 1500mg 组 88 名患者(28%)和安慰剂组 91 名患者(25%)报告了与镰状细胞病无关的严重不良事件。沃罗特 1500mg 组有 5 名或更多患者发生 3 级或 4 级不良事件(发生率<10%);贫血发生在 5 名或更多患者中(沃罗特 1500mg 组 2 名[2%]患者,沃罗特 900mg 组 7 名[8%]患者,安慰剂组 3 名[3%]患者)。在所有 274 名患者中,有 6 名(2%)患者死亡(每个治疗组各 2 例),均被认为与治疗无关。
沃罗特 1500mg 可迅速且持久地改善血红蛋白浓度,并在 72 周内保持稳定,有可能解决镰状细胞病相关溶血性贫血的严重发病率。
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