脂蛋白(a)与腹主动脉瘤风险增加有关

Pranav Sharma, Renae Judy, Shuai Yuan, Corry Gellatly, Katie L Saxby, Matthew J. Bown, Michael Levin, Scott M. Damrauer
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引用次数: 0

摘要

导言:脂蛋白(a)(Lp(a))是一种含有载脂蛋白 B(ApoB)的循环颗粒,据观察与动脉粥样硬化性心血管疾病有关,是新兴疗法的目标。最近的研究强调了循环脂蛋白在腹主动脉瘤(AAA)中的作用。我们试图从人类观察和遗传学证据两方面评估脂蛋白(a)在腹主动脉瘤中的作用:我们在英国生物库(UKB)中对 795 名患有 AAA 的人和 374,772 名未患有 AAA 的人进行了逻辑回归,在控制传统 AAA 风险因素和载脂蛋白 B 水平的情况下,检测了循环中载脂蛋白(a)水平与临床诊断的腹主动脉瘤之间的关联。多变量孟德尔随机化(MVMR)用于检验 Lp(a) 和 AAA 之间的假定因果关系,并对载脂蛋白进行控制。脂蛋白(a)和载脂蛋白B的遗传工具是根据对脂蛋白(a)和载脂蛋白B的全基因组关联研究(GWAS)创建的,这两项研究分别包括 335,796 和 418,505 名英国糖尿病患者。利用对 39,221 名 AAA 患者和 1,086,107 名非 AAA 患者进行的全基因组关联研究的数据,测试了这些工具与 AAA 的关联性。结果显示观察发现,脂蛋白(a)水平升高与 AAA 风险增加有关(每 10 毫摩尔/升脂蛋白(a)的 OR 值为 1.04;95%CI 为 1.02-1.05;P<0.01)。与 Lp(a) 水平为 <150nmol/L 的个体相比,临床 Lp(a) 水平升高(>150nmol/L)同样与 AAA 风险增加有关(OR 1.47;95% CI 1.15-1.88;P <0.01)。MVMR证实了脂蛋白(a)增加与AAA风险增加之间存在明显的、独立于载脂蛋白B的关联(脂蛋白(a)每增加一个标准差,OR为1.13;95%CI为1.02-1.24;P<0.02):观察性分析和基因分析均支持脂蛋白(a)增加与 AAA 风险之间存在关联,而这种关联与载脂蛋白 B 无关。这些研究结果表明,脂蛋白(a)可能是 AAA 的治疗靶点,并推动将 AAA 作为脂蛋白(a)拮抗剂临床试验的结果之一。
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Lipoprotein (a) is associated with increased risk of Abdominal Aortic Aneurysm
Introduction: Lipoprotein(a) (Lp(a)) is a circulating apolipoprotein B (ApoB) containing particle that has been observationally linked to atherosclerotic cardiovascular disease and is the target of emerging therapeutics. Recent work has highlighted the role of circulating lipoproteins in abdominal aortic aneurysm (AAA). We sought to triangulate human observational and genetic evidence to evaluate the role of Lp(a) in AAA. Methods: We tested the association between circulating levels of Lp(a) and clinically diagnosed abdominal aortic aneurysms while controlling for traditional AAA risk factors and levels of ApoB using logistic regression among 795 individuals with and 374,772 individuals without AAA in the UK Biobank (UKB). Multivariable Mendelian randomization (MVMR) was used to test for putatively causal associations between Lp(a) and AAA controlling for ApoB. Genetic instruments for Lp(a) and ApoB were created from genome-wide association studies (GWAS) of Lp(a) and ApoB comprising 335,796 and 418,505 UKB participants, respectively. The instruments were tested for association with AAA using data from a GWAS of 39,221 individuals with and 1,086,107 without AAA. Results: Elevated Lp(a) levels were observationally associated with an increased risk of AAA (OR 1.04 per 10 nmol/L Lp(a); 95%CI 1.02-1.05; P<0.01). Clinically elevated Lp(a) levels (>150nmol/L) were likewise associated with an increased risk of AAA (OR 1.47; 95% CI 1.15-1.88; P < 0.01) when compared to individuals with Lp(a) levels <150nmol/L. MVMR confirmed a significant, ApoB-independent association between increased Lp(a) and increased risk of AAA (OR 1.13 per SD increase in Lp(a); 95%CI 1.02-1.24; P<0.02). Conclusion: Both observational and genetic analyses support an association between increased Lp(a) and AAA risk that is independent of ApoB. These findings suggest that Lp(a) may be a therapeutic target for AAA and drive the inclusion of AAA as an outcome in clinical trials of Lp(a) antagonists.
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