Lipoprotein(a) hyperlipidemia as cardiovascular risk factor: pathophysiological aspects.

Q1 Medicine Clinical Research in Cardiology Supplements Pub Date : 2015-04-01 DOI:10.1007/s11789-015-0074-0

Gerd Schmitz, Evelyn Orsó

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引用次数: 39

Abstract

Lipoprotein (a) [Lp(a)] is a modified LDL particle with an additional apolipoprotein [apo(a)] protein covalently attached by a thioester bond. Multiple isoforms of apo(a) exist that are genetically determined by differences in the number of Kringle-IV type-2 repeats encoded by the LPA gene. Elevated plasma Lp(a) is an independent risk factor for cardiovascular disease.The phenotypic diversity of familial Lp(a) hyperlipidemia [Lp(a)-HLP] and familial hypercholesterolemia [FH], as defined risks with genetic background, and their frequent co-incidence with additional cardiovascular risk factors require a critical revision of the current diagnostic and therapeutic recommendations established for isolated familial Lp(a)-HLP or FH in combination with elevated Lp(a) levels.Lp(a) assays still suffer from poor standardization, comparability and particle variation. Further evaluation of the current biomarkers and establishment of novel comorbidity biomarkers are necessary for extended risk assessment of cardiovascular disease in FH or Lp(a)-HLP and to better understand the pathophysiology and to improve patient stratification of the Lp(a) syndrome complex.Lp(a) promotes vascular remodeling, increased lesion progression and intima media thickening through induction of M1-macrophages, antiangiogenic effects (e.g. vasa vasorum) with secretion of the antiangiogenic chemokine CXCL10 (IP10) and CXCR3 mediated activation of Th1- and NK-cells.In addition inhibition of serine proteases causing disturbances of thrombosis/ hemostasis/ fibrinolysis, TGFb-activation and acute phase response (e.g. CRP, anti-PL antibodies) are major features of Lp(a) pathology. Anti-PL antibodies (EO6 epitope) also bind to oxidized Lp(a).Lipoprotein apheresis is used to reduce circulating lipoproteins in patients with severe FH and/or Lp(a)-HLP, particularly with multiple cardiovascular risks who are intolerant or insufficiently responsive to lipid-lowering drugs.

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脂蛋白(a)高脂血症作为心血管危险因素:病理生理方面。

脂蛋白(a) [Lp(a)]是一种经过修饰的低密度脂蛋白颗粒，外加一种由硫酯键共价连接的载脂蛋白[apo(a)]蛋白。载脂蛋白(a)存在多种同工型，这是由LPA基因编码的Kringle-IV型2重复序列的数量差异遗传决定的。血浆Lp(a)升高是心血管疾病的独立危险因素。家族性Lp(a)-高脂血症[Lp(a)-HLP]和家族性高胆固醇血症[FH]的表型多样性，作为具有遗传背景的定义风险，以及它们经常与其他心血管危险因素共同发生，需要对目前针对孤立性家族性Lp(a)-HLP或FH合并Lp(a)水平升高的诊断和治疗建议进行关键修订。对于FH或Lp(a)-HLP的心血管疾病风险评估，以及更好地了解其病理生理和改善患者对Lp(a)综合征的分层，进一步评估当前的生物标志物和建立新的共病生物标志物是必要的。Lp(a)通过诱导m1巨噬细胞促进血管重塑，加速病变进展和内膜中膜增厚。通过分泌抗血管生成趋化因子CXCL10 (IP10)和CXCR3介导的Th1-和nk细胞的激活，具有抗血管生成作用(如血管生成)。此外，丝氨酸蛋白酶的抑制引起血栓形成/止血/纤溶障碍、tgfb活化和急性期反应(如CRP、抗pl抗体)是Lp(a)病理的主要特征。抗pl抗体(EO6表位)也结合氧化Lp(a)。脂蛋白分离术用于降低严重FH和/或Lp(a)-HLP患者的循环脂蛋白，特别是具有多种心血管风险且对降脂药物不耐受或反应不足的患者。

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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