鲁马西拉对1型原发性高草酸尿症婴幼儿的疗效和安全性:3期ILLUMINATE-B试验的30个月分析
Efficacy and safety of lumasiran for infants and young children with primary hyperoxaluria type 1: 30-month analysis of the phase 3 ILLUMINATE-B trial.
作者信息
Frishberg Yaacov, Hayes Wesley, Shasha-Lavsky Hadas, Sas David J, Michael Mini, Sellier-Leclerc Anne-Laure, Hogan Julien, Willey Richard, Gansner John M, Magen Daniella
机构信息
Division of Pediatric Nephrology, Shaare Zedek Medical Center and Faculty of Medicine, Hebrew University of Jerusalem, Jerusalem, Israel.
Department of Paediatric Nephrology, Great Ormond Street Hospital, London, United Kingdom.
出版信息
Front Pediatr. 2024 Sep 16;12:1392644. doi: 10.3389/fped.2024.1392644. eCollection 2024.
BACKGROUND
Primary hyperoxaluria type 1 (PH1) is a genetic disorder resulting in overproduction of hepatic oxalate, potentially leading to recurrent kidney stones, nephrocalcinosis, chronic kidney disease, and kidney failure. Lumasiran, the first RNA interference therapeutic approved for infants and young children, is a liver-directed treatment that reduces hepatic oxalate production. Lumasiran demonstrated sustained efficacy with an acceptable safety profile over 12 months in infants and young children (age <6 years) with PH1 in ILLUMINATE-B (clinicaltrials.gov: NCT03905694), an ongoing, Phase 3, multinational, open-label, single-arm study.
METHODS
Here, we report interim efficacy and safety findings from ILLUMINATE-B following 30 months of lumasiran treatment. Eligible patients had an estimated glomerular filtration rate (eGFR) >45 ml/min/1.73 m if ≥12 months old or normal serum creatinine if <12 months old, and a urinary oxalate to creatinine ratio (UOx:Cr) greater than the upper limit of normal. All 18 patients enrolled in ILLUMINATE-B completed the 6-month primary analysis period, entered an extension period of up to 54 months, and continue to participate in the study.
RESULTS
At Month 30, mean percent change from baseline in spot UOx:Cr was -76%, and mean percent change in plasma oxalate was -42%. eGFR remained stable through Month 30. In 14 patients (86%) with nephrocalcinosis at baseline, nephrocalcinosis grade improved at Month 24 in 12; no patient worsened. In the 4 patients without baseline nephrocalcinosis, nephrocalcinosis was absent at Month 24. Kidney stone event rates were ≤0.25 per person-year through Month 30. Mild, transient injection site reactions were the most common lumasiran-related adverse events (17% of patients).
CONCLUSION
In infants and young children with PH1, long-term lumasiran treatment resulted in sustained reductions in urinary and plasma oxalate that were sustained for 30 months, with an acceptable safety profile. Kidney function remained stable, low kidney stone event rates were observed through Month 30, and nephrocalcinosis grade improvements were observed through Month 24.
CLINICAL TRIAL REGISTRATION
https://clinicaltrials.gov, identifier NCT03905694.
背景
1型原发性高草酸尿症(PH1)是一种遗传性疾病,会导致肝脏草酸盐产生过多,可能引发复发性肾结石、肾钙质沉着症、慢性肾脏病和肾衰竭。鲁马西纳是首个获批用于婴幼儿的RNA干扰疗法,是一种针对肝脏的治疗方法,可减少肝脏草酸盐的产生。在一项正在进行的3期多国开放标签单臂研究ILLUMINATE - B(clinicaltrials.gov:NCT03905694)中,鲁马西纳在12个月内对PH1的婴幼儿(年龄<6岁)显示出持续疗效和可接受的安全性。
方法
在此,我们报告鲁马西纳治疗30个月后ILLUMINATE - B的中期疗效和安全性结果。符合条件的患者,如果年龄≥12个月,估计肾小球滤过率(eGFR)>45 ml/min/1.73 m²,如果年龄<12个月,则血清肌酐正常,且尿草酸盐与肌酐比值(UOx:Cr)高于正常上限。ILLUMINATE - B研究中入组的所有18例患者均完成了6个月的主要分析期,进入了长达54个月的延长期,并继续参与研究。
结果
在第30个月时,随机尿UOx:Cr较基线的平均百分比变化为-76%,血浆草酸盐的平均百分比变化为-42%。至第30个月时eGFR保持稳定。14例(86%)基线时有肾钙质沉着症的患者中,12例在第24个月时肾钙质沉着症分级改善;无患者病情恶化。4例无基线肾钙质沉着症的患者在第24个月时无肾钙质沉着症。至第30个月时肾结石事件发生率≤0.25人年。轻度、短暂性注射部位反应是最常见的与鲁马西纳相关的不良事件(17%的患者)。
结论
在PH1的婴幼儿中,长期使用鲁马西纳治疗可使尿和血浆草酸盐持续降低达30个月,且安全性可接受。肾功能保持稳定,至第30个月时肾结石事件发生率较低,至第24个月时观察到肾钙质沉着症分级改善。
临床试验注册
Zotero 插件