Prediction of cardiovascular risk by Lp(a) concentrations or genetic variants within the LPA gene region.

Q1 Medicine
Florian Kronenberg
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引用次数: 27

Abstract

In the middle of the 1990s the interest in Lp(a) vanished after a few badly performed studies almost erased Lp(a) from the map of biological targets. However, since roughly 10 years the interest has begun to grow again mainly for two reasons: first, genetic studies using easily accessible and high-throughput techniques for genotyping of single-nucleotide polymorphisms (SNPs) have allowed large studies in patients with cardiovascular disease and controls to be performed. This strengthened the earlier findings on a copy number variation in the LPA gene and its association with cardiovascular outcomes. Second, new therapies are on the horizon raising strong and justified hope that in a few years drugs will become available which tremendously lower Lp(a) concentrations. This review article should provide an introduction to the genetic determination of Lp(a) concentrations and considerations whether Lp(a) concentrations or genetic variants are important for the prediction of cardiovascular risk.

通过Lp(a)浓度或LPA基因区域的遗传变异预测心血管风险。
在20世纪90年代中期,在一些表现不佳的研究几乎将Lp(a)从生物靶标地图上抹去之后,人们对Lp(a)的兴趣消失了。然而,大约10年来,人们的兴趣又开始增长,主要有两个原因:首先,利用易于获得的高通量单核苷酸多态性(snp)基因分型技术进行遗传研究,使得在心血管疾病患者和对照患者中进行大规模研究成为可能。这加强了早期关于LPA基因拷贝数变异及其与心血管结局的关联的发现。其次,新的治疗方法正在出现,这给人们带来了强烈而合理的希望,即在几年内,可以获得大大降低Lp(a)浓度的药物。这篇综述文章应该介绍Lp(a)浓度的遗传测定,并考虑Lp(a)浓度或遗传变异对预测心血管风险是否重要。
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
Clinical Research in Cardiology Supplements
Clinical Research in Cardiology Supplements Medicine-Radiology, Nuclear Medicine and Imaging
CiteScore
6.10
自引率
0.00%
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