Dieplinger H, Kronenberg F
Institute of Medical Biology and Human Genetics, University of Innsbruck, Austria.
Wien Klin Wochenschr. 1999 Jan 15;111(1):5-20.
The human plasma lipoprotein Lp(a) has gained considerable clinical interest as a genetically determined risk factor for atherosclerotic vascular diseases. Numerous (including prospective) studies have described a correlation between elevated Lp(a) plasma levels and coronary heart disease, stroke and peripheral atherosclerosis. Lp(a) consists of a large LDL-like particle to which the specific glycoprotein apo(a) is covalently linked. The apo(a) gene is located on chromosome 6 and belongs to a gene family including the highly homologous plasminogen. Lp(a) plasma concentrations are controlled to a large extent by the extremely polymorphic apo(a) gene. More than 30 alleles at this locus determine a size polymorphism. The size of the apo(a) isoform is inversely correlated with Lp(a) plasma concentrations, which are non-normally distributed in most populations. To a minor extent, apo(a) gene-independent effects also influence Lp(a) concentrations. These include diet, hormonal status and diseases like renal disease and familial hypercholesterolemia. The standardisation of Lp(a) quantification is still an unresolved problem due to the enormous particle heterogeneity of Lp(a) and homologies of other members of the gene family. Stability problems of Lp(a) as well as statistical pitfalls in studies with small group sizes have created conflicting results. The apo(a)/Lp(a) secretion from hepatocytes is regulated at various levels including postranslationally by apo(a) isoform-dependent prolonged retention in the endoplasmic reticulum. This mechanism can partly explain the inverse correlation between apo(a) size and plasma concentrations. According to numerous investigations, Lp(a) is assembled extracellularly from separately secreted apo(a) and LDL. The sites and mechanisms of Lp(a) removal from plasma are only poorly understood. The human kidney seems to represent a major catabolic organ for Lp(a) uptake. The underlying mechanism is rather unclear; several candidate receptors from the LDL-receptor gene family do not or poorly bind Lp(a) in vitro. Lp(a) plasma levels are elevated over controls in patients with renal diseases like nephrotic syndrome and end-stage renal disease. Following renal transplantation, Lp(a) concentrations decrease to values observed in controls matched for apo(a) type. Controversial data on Lp(a) in diabetes mellitus mainly result from insufficient sample sizes in numerous studies. Large studies and those including apo(a) phenotype analysis have come to the conclusion that Lp(a) levels are not or only moderately elevated in insulin-dependent patients. In non-insulin-dependent diabetics Lp(a) is not elevated. Several rare disorders, such as LCAT and LPL deficiency, as well as liver diseases and abetalipoproteinemia are associated with low plasma levels or lack of Lp(a).
人类血浆脂蛋白Lp(a)作为动脉粥样硬化性血管疾病的一种遗传决定风险因素,已引起了相当大的临床关注。众多(包括前瞻性)研究描述了Lp(a)血浆水平升高与冠心病、中风及外周动脉粥样硬化之间的相关性。Lp(a)由一个大的低密度脂蛋白(LDL)样颗粒和与之共价连接的特异性糖蛋白载脂蛋白(a)[apo(a)]组成。apo(a)基因位于6号染色体上,属于一个包括高度同源的纤溶酶原的基因家族。Lp(a)血浆浓度在很大程度上受极具多态性的apo(a)基因控制。该基因座上有30多个等位基因决定了大小多态性。apo(a)异构体的大小与Lp(a)血浆浓度呈负相关,在大多数人群中Lp(a)血浆浓度呈非正态分布。在较小程度上,apo(a)基因非依赖效应也会影响Lp(a)浓度。这些因素包括饮食、激素状态以及肾病和家族性高胆固醇血症等疾病。由于Lp(a)巨大的颗粒异质性以及该基因家族其他成员的同源性,Lp(a)定量的标准化仍是一个未解决的问题。Lp(a)的稳定性问题以及小样本量研究中的统计缺陷导致了相互矛盾的结果。肝细胞分泌apo(a)/Lp(a)在多个水平受到调控,包括翻译后通过apo(a)异构体依赖的在内质网中延长滞留来调控。这一机制可以部分解释apo(a)大小与血浆浓度之间的负相关。根据众多研究,Lp(a)是由分别分泌的apo(a)和LDL在细胞外组装而成。Lp(a)从血浆中清除的部位和机制目前了解甚少。人类肾脏似乎是Lp(a)摄取的主要分解代谢器官。其潜在机制尚不清楚;LDL受体基因家族的几种候选受体在体外不与Lp(a)结合或与Lp(a)结合能力很差。肾病综合征和终末期肾病等肾病患者的Lp(a)血浆水平高于对照组。肾移植后,Lp(a)浓度降至与apo(a)类型匹配的对照组所观察到的值。关于糖尿病患者Lp(a)的有争议数据主要源于众多研究中样本量不足。大型研究以及那些包括apo(a)表型分析的研究得出结论,胰岛素依赖型患者的Lp(a)水平未升高或仅中度升高。非胰岛素依赖型糖尿病患者的Lp(a)未升高。几种罕见疾病,如卵磷脂胆固醇酰基转移酶(LCAT)和脂蛋白脂肪酶(LPL)缺乏症,以及肝脏疾病和无β脂蛋白血症与低血浆水平或Lp(a)缺乏有关。
