冠状动脉疾病与脂蛋白(a)浓度升高有关,与循环载脂蛋白(a)亚型的大小无关。

M Farrer, F L Game, C J Albers, H A Neil, P H Winocour, M F Laker, P C Adams, K G Alberti
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引用次数: 48

摘要

在508名社区无症状白人成员和318名血管造影确定的冠状动脉疾病(CAD)白人患者中测定脂蛋白(a) [Lp(a)]浓度和载脂蛋白(a) [apo(a)]异构体(通过十二烷基硫酸钠-聚丙烯酰胺凝胶电泳[SDS-PAGE]和Western blotting鉴定)。还测量了冠心病的常规危险因素。冠心病患者的Lp(a)浓度几乎是无症状对照组(几何平均值,84 mg/L[几何SD, 21至334 mg/L])的两倍(几何平均值,152 mg/L[几何SD, 10至1398 mg/L])。无症状女性的Lp(a)浓度高于无症状男性。CAD患者年龄较大,吸烟和有一级亲属患有早期CAD(< 55岁)的可能性更大,男性比例更高。CAD患者的Lp(a)浓度较高,与表达的异构体条带数量无关。当载脂蛋白(a)异型根据其分子大小被分配到10类中的1类时(SDS-PAGE中的Rf与载脂蛋白ob), CAD患者没有表达过多的低分子质量(高浓度)异型,但确实表达了更高比例的双带表型和更少的“零”表型。双带表型中两个同工异构体条带之间的关系在两个种群中是相同的。异构体迁移率被定义为一个连续变量,等于单个异构体带(单带表型)的迁移率或双带表型中两个异构体的平均值。两个变量,异构体迁移率和表达的异构体带的数量,被用来总结可以识别的大范围异构体模式(至少45)。异构体迁移率、表达的异构体条带数和CAD的存在是Lp(a)浓度的三个最重要的独立预测因子(按降序排列)。在逐步回归模型中,只有性别和低密度脂蛋白胆固醇是Lp(a)浓度的独立预测因子,该模型包括广泛的人口统计学因素以及脂质和血糖危险因素。我们得出结论,Lp(a)浓度与CAD无关,与表达的亚型模式无关。载脂蛋白(a)基因位点对循环脂蛋白(a)浓度有很强的控制作用,更好地了解载脂蛋白(a)基因表达的控制对于理解脂蛋白(a)与CAD之间的关系至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Coronary artery disease is associated with increased lipoprotein(a) concentrations independent of the size of circulating apolipoprotein(a) isoforms.

Lipoprotein(a) [Lp(a)] concentration and apolipoprotein(a) [apo(a)] isoforms (identified by sodium dodecyl sulfate-polyacrylamide gel electrophoresis [SDS-PAGE] and Western blotting) were determined in a group of 508 asymptomatic Caucasian members of the community and in 318 Caucasian patients with angiographically defined coronary artery disease (CAD). Conventional risk factors for CAD were also measured. Lp(a) concentration was almost twice as high in subjects with CAD (geometric mean, 152 mg/L [geometric SD, 10 to 1398 mg/L]) as in asymptomatic control subjects (geometric mean, 84 mg/L [geometric SD, 21 to 334 mg/L]). Asymptomatic women had higher concentrations of Lp(a) than asymptomatic men. Patients with CAD were older and were more likely to have smoked and to have a first-degree relative with premature CAD (< 55 years of age), and a higher proportion were male. Patients with CAD had higher concentrations of Lp(a) independently of the number of isoform bands expressed. When apo(a) isoforms were allocated to 1 of 10 classes on the basis of their molecular size (Rf versus apoB in SDS-PAGE), patients with CAD did not express an excess of low-molecular-mass (higher concentration) isoforms but did express a higher proportion of double-band phenotypes with fewer "null" phenotypes. The relationship between the two isoform bands in a double-band phenotype was the same in both populations. Isoform mobility was defined as a continuous variable equal to the mobility of a single isoform band (single-band phenotypes) or the mean of the two isoforms in a double-band phenotype. Two variables, isoform mobility and the number of isoform bands expressed, were used to summarize the large range of isoform patterns (at least 45) that could be identified. Isoform mobility, the number of isoform bands expressed, and the presence of CAD were the three most important independent predictors of Lp(a) concentration (descending order). Only sex and LDL cholesterol were additional independent predictors of Lp(a) concentration in step-wise regression models including a wide range of demographic factors and lipid and glycemic risk factors. We conclude that Lp(a) concentration is associated with CAD independently of the isoform pattern expressed. The apo(a) gene locus exerts a strong control over circulating Lp(a) concentration, and a better understanding of the control of expression of the apo(a) gene will be essential to understand the relationship between Lp(a) and CAD.

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