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人高密度脂蛋白的色谱聚焦及脂蛋白A和A-I的分离

Chromatofocusing of human high density lipoproteins and isolation of lipoproteins A and A-I.

作者信息

Nestruck A C, Niedmann P D, Wieland H, Seidel D

出版信息

Biochim Biophys Acta. 1983 Aug 29;753(1):65-73. doi: 10.1016/0005-2760(83)90099-1.

Abstract

Using chromatofocusing, a column chromatography method with an internally generated pH gradient and focusing effects, human plasma high density lipoproteins (HDL) were fractionated into six subclasses within an interval of less than 1 pH unit (pH 5.1-4.2). All fractions floated in the ultracentrifuge at density = 1.21 g X ml-1, retained a typical HDL electron micrographic morphology and as a single band, alpha-migration on agarose electrophoresis. Compositional analysis of the subclasses revealed an inverse relationship between cholesterol ester and cholesterol on a molar basis. Distinct differences in the distribution of the apolipoproteins between the fractions were found. Two of the subclasses contained only apolipoprotein A-I and were therefore considered to be two forms of the lipid-combined form of apolipoprotein A-I, i.e., lipoprotein A-I. One subclass contained only apolipoproteins A-I + A-II and was, therefore, lipoprotein A. One subclass contained apolipoproteins A-I + A-II + D, and the two remaining contained additionally apolipoproteins C and E. Lipoprotein A-I was also demonstrated after immunoabsorption of apolipoprotein A-II-containing lipoproteins from whole serum. It is suggested that this method, which allows the fractionation of HDL into subclasses with distinct differences in apolipoprotein composition, offers new avenues for the study of the structural and metabolic heterogeneity of HDL.

摘要

采用等速聚焦层析法(一种具有内源性pH梯度和聚焦效应的柱层析方法),将人血浆高密度脂蛋白(HDL)在小于1个pH单位(pH 5.1 - 4.2)的区间内分离为六个亚类。所有组分在密度为1.21 g·ml⁻¹的超速离心机中上浮,保留典型的HDL电子显微镜形态,且在琼脂糖电泳中呈单一α迁移带。亚类的成分分析显示,胆固醇酯与胆固醇在摩尔基础上呈反比关系。各组分之间载脂蛋白的分布存在明显差异。其中两个亚类仅含载脂蛋白A-I,因此被认为是载脂蛋白A-I的两种脂质结合形式,即脂蛋白A-I。一个亚类仅含载脂蛋白A-I + A-II,因此是脂蛋白A。一个亚类含载脂蛋白A-I + A-II + D,其余两个亚类还额外含有载脂蛋白C和E。从全血清中免疫吸附含载脂蛋白A-II的脂蛋白后也证实了脂蛋白A-I的存在。有人提出,这种能将HDL分离为载脂蛋白组成有明显差异的亚类的方法,为研究HDL的结构和代谢异质性提供了新途径。

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