乐泊迪西然——一种靶向脂蛋白(a)的长效小干扰RNA
Lepodisiran - A Long-Duration Small Interfering RNA Targeting Lipoprotein(a).
作者信息
Nissen Steven E, Ni Wei, Shen Xi, Wang Qiuqing, Navar Ann Marie, Nicholls Stephen J, Wolski Kathy, Michael Laura, Haupt Axel, Krege John H
机构信息
Cleveland Clinic Coordinating Center for Clinical Research, Cleveland.
Eli Lilly, Indianapolis.
出版信息
N Engl J Med. 2025 May 1;392(17):1673-1683. doi: 10.1056/NEJMoa2415818. Epub 2025 Mar 30.
BACKGROUND
Elevated lipoprotein(a) concentrations are associated with atherosclerotic cardiovascular disease. The safety and efficacy of lepodisiran, an extended-duration, small interfering RNA targeting hepatic synthesis of lipoprotein(a), are unknown.
METHODS
We randomly assigned participants in a 1:2:2:2:2 ratio to receive lepodisiran at a dose of 16 mg, 96 mg, or 400 mg at baseline and again at day 180, lepodisiran at a dose of 400 mg at baseline and placebo at day 180, or placebo at baseline and at day 180, all administered by subcutaneous injection. Data from the two groups that received lepodisiran at a dose of 400 mg at baseline were pooled for the primary analysis. The primary end point was the time-averaged percent change from baseline in the serum lipoprotein(a) concentration (lepodisiran difference from placebo [i.e., placebo-adjusted]) during the period from day 60 to day 180.
RESULTS
A total of 320 participants underwent randomization; the median baseline lipoprotein(a) concentration was 253.9 nmol per liter. The placebo-adjusted time-averaged percent change from baseline in the serum lipoprotein(a) concentration from day 60 to day 180 was -40.8 percentage points (95% confidence interval [CI], -55.8 to -20.6) in the 16-mg lepodisiran group, -75.2 percentage points (95% CI, -80.4 to -68.5) in the 96-mg group, and -93.9 percentage points (95% CI, -95.1 to -92.5) in the pooled 400-mg groups. The corresponding change from day 30 to day 360 was -41.2 percentage points (95% CI, -55.4 to -22.4), -77.2 percentage points (95% CI, -81.8 to -71.5), -88.5 percentage points (95% CI, -90.8 to -85.6), and -94.8 percentage points (95% CI, -95.9 to -93.4) in the 16-mg, 96-mg, 400-mg-placebo, and 400-mg-400-mg dose groups, respectively. Serious adverse events, none of which were deemed by investigators to be related to lepodisiran or placebo, occurred in 35 participants. Dose-dependent, generally mild injection-site reactions occurred in up to 12% (8 of 69) of the participants in the highest lepodisiran dose group.
CONCLUSIONS
Lepodisiran reduced mean serum concentrations of lipoprotein(a) from 60 to 180 days after administration. (Funded by Eli Lilly; ALPACA ClinicalTrials.gov number, NCT05565742.).
背景
脂蛋白(a)浓度升高与动脉粥样硬化性心血管疾病相关。乐泊迪司然(lepodisiran)是一种长效小干扰RNA,靶向肝脏脂蛋白(a)的合成,其安全性和有效性尚不清楚。
方法
我们将参与者按1:2:2:2:2的比例随机分组,在基线时以及第180天分别接受16毫克、96毫克或400毫克的乐泊迪司然,或在基线时接受400毫克乐泊迪司然而在第180天接受安慰剂,或在基线时和第180天均接受安慰剂,所有药物均通过皮下注射给药。对基线时接受400毫克乐泊迪司然的两组数据进行汇总以进行主要分析。主要终点是第60天至第180天期间血清脂蛋白(a)浓度相对于基线的时间平均百分比变化(乐泊迪司然与安慰剂的差异[即安慰剂校正值])。
结果
共有320名参与者进行了随机分组;基线脂蛋白(a)浓度中位数为每升253.9纳摩尔。在第60天至第180天期间,16毫克乐泊迪司然组血清脂蛋白(a)浓度相对于基线的安慰剂校正时间平均百分比变化为-40.8个百分点(95%置信区间[CI],-55.8至-20.6),96毫克组为-75.2个百分点(95%CI,-80.4至-68.5),400毫克汇总组为-93.9个百分点(95%CI,-95.1至-92.5)。在第30天至第360天期间,16毫克、96毫克、400毫克-安慰剂和400毫克-400毫克剂量组的相应变化分别为-41.2个百分点(95%CI,-55.4至-22.4)、-77.2个百分点(95%CI,-81.8至-71.5)、-88.5个百分点(95%CI,-90.8至-85.6)和-94.8个百分点(95%CI,-95.9至-93.4)。35名参与者发生了严重不良事件,调查人员认为这些事件均与乐泊迪司然或安慰剂无关。在最高乐泊迪司然剂量组中,高达12%(69名中的8名)的参与者出现了剂量依赖性、一般为轻度的注射部位反应。
结论
乐泊迪司然在给药后60至180天降低了脂蛋白(a)的平均血清浓度。(由礼来公司资助;ALPACA临床试验注册号,NCT05565742。)
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