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与动脉粥样硬化疾病相关但与Ⅲ型高脂蛋白血症无关的载脂蛋白E新突变体。

New mutants of apolipoprotein E associated with atherosclerotic diseases but not to type III hyperlipoproteinemia.

作者信息

Yamamura T, Yamamoto A, Sumiyoshi T, Hiramori K, Nishioeda Y, Nambu S

出版信息

J Clin Invest. 1984 Oct;74(4):1229-37. doi: 10.1172/JCI111532.

Abstract

We analyzed the heterogeneity of apo E in very low density lipoprotein from 58 hyperlipidemic subjects with or without atherosclerosis, 69 patients with ischemic heart disease, and 100 apparently healthy individuals. Apo E gene frequencies in the group of healthy individuals were comparable with those in German and American populations. The distribution of six common apo E phenotypes in the groups of hyperlipidemia and ischemic heart disease was similar to that in the healthy group. In addition to the three major isoforms of apolipoprotein E (apo E-4, E-3, and E-2) and the new one (apo E-5) which was recently found in this laboratory, we have discovered an additional series of components, which showed themselves as at least three bands on an isoelectric focusing gel in the region of E-VII through E-V, in four patients with hyperlipidemia and atherosclerosis. The new series of apo E components, named apo E-Suita, was identical with the ordinary apo E in its interaction with heparin-Sepharose gel and with anti-apo E antibody. The most basic component of apo E-Suita (E-VII) was the unsialylated form and other components (E-VI and E-V), the sialylated forms. Family studies revealed that apo E-Suita was determined by inheritance of a new apo E allele located at the same locus as the hitherto known apo E components. Apo E-5 and apo E-Suita isoproteins had isoelectric points more basic than apo E-3, the parent type, by two and four units of charge, respectively. While the apo E-Suita isoprotein had the same molecular weight as ordinary major apo E isoproteins, the molecular weight of the apo E-5 isoprotein was approximately 1,500-2,000 lower than the other apo E isoproteins by sodium dodecyl sulfate-polyacrylamide gel electrophoresis. The incidence of abnormal apo E components, including apo E-5 and apo E-Suita, was high among patients with hyperlipidemia and ischemic heart disease (7:127), while we could not find such components among 100 healthy individuals. Moreover, five of seven patients with the abnormal apo E had overt atherosclerotic disease. The findings suggest that these kinds of apolipoprotein mutation are closely related to the development of atherosclerosis.

摘要

我们分析了58名有或无动脉粥样硬化的高脂血症患者、69名缺血性心脏病患者以及100名貌似健康个体的极低密度脂蛋白中载脂蛋白E(apo E)的异质性。健康个体组中的apo E基因频率与德国和美国人群中的相似。高脂血症组和缺血性心脏病组中六种常见apo E表型的分布与健康组相似。除了载脂蛋白E的三种主要异构体(apo E-4、E-3和E-2)以及本实验室最近发现的新异构体(apo E-5)外,我们在4名患有高脂血症和动脉粥样硬化的患者中还发现了另一系列成分,在等电聚焦凝胶上,它们在E-VII至E-V区域显示为至少三条带。新的apo E成分系列,命名为apo E-Suita,在与肝素-琼脂糖凝胶和抗apo E抗体的相互作用方面与普通apo E相同。apo E-Suita的最碱性成分(E-VII)是去唾液酸化形式,其他成分(E-VI和E-V)是唾液酸化形式。家系研究表明,apo E-Suita由一个新的apo E等位基因遗传决定,该等位基因与迄今已知的apo E成分位于同一基因座。apo E-5和apo E-Suita同工蛋白的等电点分别比亲本类型apo E-3的等电点多两个和四个电荷单位。虽然apo E-Suita同工蛋白的分子量与普通主要apo E同工蛋白相同,但通过十二烷基硫酸钠-聚丙烯酰胺凝胶电泳,apo E-5同工蛋白的分子量比其他apo E同工蛋白低约1500 - 2000。包括apo E-5和apo E-Suita在内的异常apo E成分在高脂血症和缺血性心脏病患者中的发生率较高(7:127),而在100名健康个体中未发现此类成分。此外,7名apo E异常的患者中有5名患有明显的动脉粥样硬化疾病。这些发现表明,这类载脂蛋白突变与动脉粥样硬化的发展密切相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a76/425289/c59d5191f691/jcinvest00136-0111-a.jpg

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