Zerlasiran-A Small-Interfering RNA Targeting Lipoprotein(a): A Phase 2 Randomized Clinical Trial.

Q1 Medicine
Steven E Nissen, Qiuqing Wang, Stephen J Nicholls, Ann Marie Navar, Kausik K Ray, Gregory G Schwartz, Michael Szarek, Erik S G Stroes, Roland Troquay, Jannick A N Dorresteijn, Henry Fok, David A Rider, Steven Romano, Kathy Wolski, Curtis Rambaran
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引用次数: 0

Abstract

Importance: Elevated lipoprotein(a) increases the risk of atherosclerotic cardiovascular disease (ASCVD) and aortic stenosis.

Objective: To evaluate the effects of zerlasiran, a small-interfering RNA targeting hepatic synthesis of apolipoprotein(a), on lipoprotein(a) serum concentration.

Design, setting, and participants: A multicenter trial in patients with stable ASCVD with serum lipoprotein(a) concentrations greater than or equal to 125 nmol/L at 26 sites in Europe and South Africa between January 3, 2023, and April 27, 2023, with last follow-up on July 1, 2024.

Interventions: Participants randomized to receive a subcutaneous dose of placebo every 16 weeks for 3 doses (n = 23) or every 24 weeks for 2 doses (n = 24) or zerlasiran 450 mg every 24 weeks for 2 doses (n = 45), 300 mg every 16 weeks for 3 doses (n = 42), or 300 mg every 24 weeks for 2 doses (n = 44).

Main outcome and measures: The primary outcome was the time-averaged percent change in lipoprotein(a) concentration from baseline to 36 weeks, with follow-up to 60 weeks.

Results: Among 178 patients, mean (SD) age was 63.7 (9.4) years, 46 (25.8%) were female, with a median (IQR) baseline lipoprotein(a) concentration of 213 (177-282) nmol/L; 172 patients completed the trial. Compared with the pooled placebo group, the least-squares mean time-averaged percent change in lipoprotein(a) concentration from baseline to week 36 was -85.6% (95% CI, -90.9% to -80.3%), -82.8% (95% CI, -88.2% to -77.4%), and -81.3% (95% CI, -86.7% to -76.0%) for the 450 mg every 24 weeks, 300 mg every 16 weeks, and 300 mg every 24 weeks groups, respectively. Median (IQR) percent change in lipoprotein(a) concentration at week 36 was -94.5% (-97.3% to -84.2%) for the 450 mg every 24 weeks group, -96.4% (-97.7% to -92.3%) for the 300 mg every 16 weeks group, and -90.0% (-93.7% to -81.3%) for the 300 mg every 24 weeks group. The most common treatment-related adverse effects were injection site reactions, with mild pain occurring in 2.3% to 7.1% of participants in the first day following drug administration. There were 20 serious adverse events in 17 patients, none considered related to the study drug.

Conclusions: Zerlasiran was well-tolerated and reduced time-averaged lipoprotein(a) concentration by more than 80% during 36 weeks of treatment in patients with ASCVD.

Trial registration: ClinicalTrials.gov Identifier: NCT05537571.

Zerlasiran-A 小干扰 RNA 靶向脂蛋白(a):2期随机临床试验。
重要性:脂蛋白(a)升高会增加动脉粥样硬化性心血管疾病(ASCVD)和主动脉狭窄的风险:评估以肝脏合成脂蛋白(a)为靶点的小干扰RNA泽拉西坦对脂蛋白(a)血清浓度的影响:多中心试验:2023年1月3日至2023年4月27日期间,在欧洲和南非的26个地点对血清脂蛋白(a)浓度大于或等于125 nmol/L的稳定型ASCVD患者进行试验,最后一次随访时间为2024年7月1日:参与者随机接受皮下注射安慰剂,每 16 周一次,共 3 次(n = 23),或每 24 周一次,共 2 次(n = 24),或 zerlasiran 450 毫克,每 24 周一次,共 2 次(n = 45),300 毫克,每 16 周一次,共 3 次(n = 42),或 300 毫克,每 24 周一次,共 2 次(n = 44):主要结果是脂蛋白(a)浓度从基线到 36 周的时间平均百分比变化,随访至 60 周:在178名患者中,平均(标清)年龄为63.7(9.4)岁,女性46人(25.8%),脂蛋白(a)基线浓度中位数(IQR)为213(177-282)nmol/L;172名患者完成了试验。与汇总的安慰剂组相比,从基线到第36周,每24周450毫克组、每16周300毫克组和每24周300毫克组脂蛋白(a)浓度的最小二乘平均时间平均百分比变化率分别为-85.6%(95% CI,-90.9%至-80.3%)、-82.8%(95% CI,-88.2%至-77.4%)和-81.3%(95% CI,-86.7%至-76.0%)。每24周服用450毫克组、每16周服用300毫克组和每24周服用300毫克组在第36周时脂蛋白(a)浓度变化的中位数(IQR)百分比分别为-94.5%(-97.3%至-84.2%)、-96.4%(-97.7%至-92.3%)和-90.0%(-93.7%至-81.3%)。最常见的治疗相关不良反应是注射部位反应,2.3%至7.1%的参与者在用药后第一天出现轻微疼痛。17名患者共发生了20起严重不良反应,但均与研究药物无关:结论:Zerlasiran的耐受性良好,在对ASCVD患者进行36周的治疗期间,其时间平均脂蛋白(a)浓度降低了80%以上:试验注册:ClinicalTrials.gov Identifier:试验注册:ClinicalTrials.gov Identifier:NCT05537571。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
45.40
自引率
0.00%
发文量
0
期刊介绍: JAMA, published continuously since 1883, is an international peer-reviewed general medical journal. JAMA is a member of the JAMA Network, a consortium of peer-reviewed, general medical and specialty publications.
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