Icosapent ethyl-induced lipoprotein remodeling and its impact on cardiovascular disease risk markers in normolipidemic individuals.

IF 6.1 1区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

JCI insight Pub Date : 2025-10-08 DOI:10.1172/jci.insight.193637

Lauri Äikäs, Petri T Kovanen, Martina B Lorey, Reijo Laaksonen, Minna Holopainen, Hanna Ruhanen, Reijo Käkelä, Matti Jauhiainen, Martin Hermansson, Katariina Öörni

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引用次数: 0

Abstract

BACKGROUNDIcosapent ethyl (IPE), an ethyl ester of eicosapentaenoic acid (EPA), reduces cardiovascular disease (CVD), but the mechanism remains elusive. We examined the effect of IPE supplementation on lipoprotein subclasses, lipidomes, and pro-atherogenic properties.METHODSUsing 3 independent metabolomic platforms, we examined the effect of high-dose IPE supplementation for 28 days on fatty acid profiles, lipoprotein subclasses, lipidomes, and pro-atherogenic properties in normolipidemic volunteers (n = 38).RESULTSIPE supplementation increased lipoprotein EPA on average 4-fold within 7 days, returning to baseline after a 7-day washout. Notably, the incorporation displayed marked interindividual variance, negatively correlating with baseline levels. We identified persistent participant-specific lipoprotein fingerprints despite uniform IPE-induced lipidome remodeling across all lipoprotein classes. This remodeling resulted in reductions in saturated, monounsaturated, and n-6 polyunsaturated fatty acids, resulting in reduced clinical risk markers, including triglyceride, remnant cholesterol, and apolipoprotein B (apoB) levels and 10-year CVD risk score. Of the pro-atherogenic properties tested, IPE significantly reduced apoB lipoprotein binding to proteoglycans, which correlated with lower apoB particle concentration, cholesterol content, and specific lipid species in LDL, including phosphatidylcholine 38:3 previously associated with CVD.CONCLUSIONThese findings highlight IPE's rapid, uniform remodeling of lipoproteins and reduced proteoglycan binding, likely contributing to previously observed CVD risk reduction. Persistent interindividual lipidome signatures underscore the potential for personalized therapeutic approaches in atherosclerotic CVD treatment.TRIAL REGISTRATIONNCT04152291.FUNDINGJenny and Antti Wihuri Foundation, Research Council of Finland, Sigrid Jusélius Foundation, Finnish Foundation for Cardiovascular Research, Emil Aaltonen Foundation, Ida Montin Foundation, Novo Nordisk Foundation, Finnish Cultural Foundation, and Jane and Aatos Erkko Foundation.

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正常血脂人群中二碳二烯诱导的脂蛋白重塑及其对心血管疾病危险标志物的影响

二十碳五烯乙基（IPE）是二十碳五烯酸（EPA）的一种乙酯，可降低心血管疾病（CVD），但其机制尚不明确。我们研究了IPE补充剂对脂蛋白亚类、脂质体和促动脉粥样硬化特性的影响。方法：使用3个独立的代谢组学平台，我们研究了高剂量IPE补充28天对正常血脂志愿者（n = 38）脂肪酸谱、脂蛋白亚类、脂质体和促动脉粥样硬化特性的影响。结果：在7天内，pe补充剂使脂蛋白EPA平均增加4倍，在7天的洗脱期后恢复到基线水平。值得注意的是，合并显示出显著的个体间差异，与基线水平负相关。尽管在所有脂蛋白类别中，ipe诱导的脂质组重塑都是一致的，但我们发现了持久的参与者特异性脂蛋白指纹。这种重塑导致饱和、单不饱和和n-6多不饱和脂肪酸减少，导致临床风险指标降低，包括甘油三酯、残余胆固醇、载脂蛋白B （apoB）水平和10年心血管疾病风险评分。在促动脉粥样硬化特性测试中，IPE显著降低了载脂蛋白ob脂蛋白与蛋白聚糖的结合，这与较低的载脂蛋白ob颗粒浓度、胆固醇含量和LDL中的特定脂质种类（包括先前与CVD相关的磷脂酰胆碱38:3）相关。结论：这些发现突出了IPE快速、均匀地重塑脂蛋白和减少蛋白聚糖结合，可能有助于先前观察到的心血管疾病风险降低。持续的个体间脂质组特征强调了在动脉粥样硬化性CVD治疗中个性化治疗方法的潜力。REGISTRATIONNCT04152291审判。资助：jenny and Antti Wihuri基金会、芬兰研究委员会、Sigrid jussamlius基金会、芬兰心血管研究基金会、Emil Aaltonen基金会、Ida Montin基金会、Novo Nordisk基金会、芬兰文化基金会、Jane and Aatos Erkko基金会。

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来源期刊

JCI insight Medicine-General Medicine

CiteScore

13.70

自引率

1.20%

发文量

543

审稿时长

6 weeks

期刊介绍： JCI Insight is a Gold Open Access journal with a 2022 Impact Factor of 8.0. It publishes high-quality studies in various biomedical specialties, such as autoimmunity, gastroenterology, immunology, metabolism, nephrology, neuroscience, oncology, pulmonology, and vascular biology. The journal focuses on clinically relevant basic and translational research that contributes to the understanding of disease biology and treatment. JCI Insight is self-published by the American Society for Clinical Investigation (ASCI), a nonprofit honor organization of physician-scientists founded in 1908, and it helps fulfill the ASCI's mission to advance medical science through the publication of clinically relevant research reports.