Effectiveness and safety of injectable PCSK9 inhibitors in dyslipidaemias’ treatment and cardiovascular disease prevention: An overview of 86 systematic reviews and a network metaanalysis

Konstantinos Pamporis , Paschalis Karakasis , Spyridon Simantiris , Marios Sagris , Konstantinos I. Bougioukas , Nikolaos Fragakis , Dimitrios Tousoulis
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Abstract

Objective

Multiple systematic reviews (SR) have been performed on the effects of proprotein convertase subtilisin/kexin type 9 inhibitors (PCSK9i), often providing conflicting findings. This overview and network meta-analysis (NMA) aimed to summarize SR findings on the efficacy and safety of PCSK9i and provide an updated NMA.

Materials and methods

MEDLINE (Pubmed), Scopus, Cochrane, Epistemonikos and Google Scholar were searched from inception to September 21, 2023 for SRs of randomized controlled trials (RCTs) and from January 1, 2020 to September 21, 2023 for additional RCTs. Double-independent study selection, data extraction and quality assessment were performed. Qualitative analysis was performed for SRs and a frequentist random-effects model NMA was performed for RCTs.

Results

Totally, 86 SRs and 76 RCTs were included. Alirocumab (77/86 [90%]) and evolocumab (73/86 [85%]) were mostly analyzed. Associations from SRs (35/42 [83%]) and the updated NMA indicated PCSK9i benefit on major adverse cardiovascular events (MACEs). Reductions were also noted for cerebrovascular events (47/66 [71%]), coronary revascularization (29/33 [88%]) and myocardial infarction (41/63 [65%]). Alirocumab was associated with reductions on all-cause mortality (RR = 0.82, 95%CI [0.72,0.94]). Data on any CV event reduction were conflicting (7/16 [44%]). Inclisiran appeared effective only on MACEs (RR = 0.76, 95%CI [0.61,0.94]). No reductions in heart failure were observed (0/16). No increases were identified between PCSK9i and any (0/35) or serious adverse events (0/52). However, PCSK9i were associated with injection-site reactions (20/28 [71%]).

Conclusion

PCSK9i appeared to be effective in CV outcomes and their clinical application was generally safe.

注射用 PCSK9 抑制剂在治疗血脂异常和预防心血管疾病方面的有效性和安全性:86篇系统综述和网络荟萃分析综述
目的针对9型丙蛋白转换酶亚基酶/kexin抑制剂(PCSK9i)的作用已进行了多次系统综述(SR),但结果往往相互矛盾。本综述和网络荟萃分析(NMA)旨在总结有关 PCSK9i 的疗效和安全性的 SR 研究结果,并提供最新的 NMA。材料与方法检索了 MedLINE (Pubmed)、Scopus、Cochrane、Epistemonikos 和 Google Scholar,从开始到 2023 年 9 月 21 日检索了随机对照试验 (RCT) 的 SR,从 2020 年 1 月 1 日到 2023 年 9 月 21 日检索了其他 RCT。进行了双重独立的研究筛选、数据提取和质量评估。对SR进行了定性分析,对RCT进行了频数随机效应模型NMA分析。阿利珠单抗(77/86 [90%])和埃沃洛库单抗(73/86 [85%])是分析的主要对象。SRs(35/42 [83%])和更新的 NMA 显示 PCSK9i 对主要不良心血管事件 (MACE) 有益。脑血管事件(47/66 [71%])、冠状动脉血运重建(29/33 [88%])和心肌梗死(41/63 [65%])也有所减少。阿利珠单抗可降低全因死亡率(RR = 0.82,95%CI [0.72,0.94])。有关减少任何 CV 事件的数据相互矛盾(7/16 [44%])。英克来兰似乎只对 MACEs 有效(RR = 0.76,95%CI [0.61,0.94])。没有观察到心力衰竭的减少(0/16)。未发现 PCSK9i 与任何不良事件(0/35)或严重不良事件(0/52)之间存在关联。然而,PCSK9i 与注射部位反应有关(20/28 [71%])。
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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