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在血糖过高的糖尿病患者中,血浆载脂蛋白AI、AII、B、CI和E会发生糖基化。

Plasma apolipoproteins AI, AII, B, CI, and E are glucosylated in hyperglycemic diabetic subjects.

作者信息

Curtiss L K, Witztum J L

出版信息

Diabetes. 1985 May;34(5):452-61. doi: 10.2337/diab.34.5.452.

DOI:10.2337/diab.34.5.452
PMID:3921419
Abstract

Nonenzymatic posttranslational glucosylation of the free amine of lysine residues can occur in hyperglycemic diabetic subjects. Using monoclonal antibodies that specifically bind the reduced conjugate of glucose covalently bound to the epsilon amine of lysine, glucitollysine, plasma lipoprotein glucosylation was demonstrated by radioimmunoassays in all subjects tested. Lipoproteins isolated from the plasma of diabetic subjects in poor metabolic control contained up to 33-fold increases in glucitollysine residues/mg of isolated lipoprotein protein, and on an absolute basis contained between 36 and 383 nmol of glucitollysine in their total lipoprotein fraction compared with normals, who had a mean of 2.9 +/- 0.06 nmol. The majority of the glucosylated protein in the d less than 1.125 g/ml fraction was present in the triglyceride-rich lipoproteins of hyperglycemic subjects, whereas the majority of the glucosylated protein in the d less than 1.125 g/ml fraction of euglycemic subjects was present in the high-density lipoproteins (HDL). A number of immunochemical approaches were used to demonstrate that, in diabetic plasma, apo AI, apo AII, apo B, apo CI, apo E, and albumin were glucosylated. Detailed studies of the apoproteins of a d less than or equal to 1.019 g/ml lipoprotein fraction and of an HDL fraction isolated from a hyperglycemic diabetic subject indicated that glucitollysine-specific antibodies can be used to preparatively isolate proteins containing glucosylated amino acid residues so that the extent of glucosylation in specific proteins can be measured. The results indicate that some of the lysine residues of the apoproteins can be modified in hyperglycemic diabetic subjects by the covalent attachment of glucose. The possible significance of these observations is discussed.

摘要

在血糖过高的糖尿病患者体内,赖氨酸残基的游离胺可发生非酶促翻译后糖基化。使用能特异性结合与赖氨酸ε-胺共价结合的葡萄糖还原共轭物(葡糖赖氨酸)的单克隆抗体,通过放射免疫分析在所有受试对象中证实了血浆脂蛋白糖基化。从代谢控制不佳的糖尿病患者血浆中分离出的脂蛋白,每毫克分离出的脂蛋白蛋白中葡糖赖氨酸残基含量增加了33倍,与正常受试者相比,其总脂蛋白部分中葡糖赖氨酸的绝对含量在36至383纳摩尔之间,而正常受试者的平均值为2.9±0.06纳摩尔。在密度小于1.125 g/ml的组分中,大多数糖基化蛋白存在于血糖过高受试者富含甘油三酯的脂蛋白中,而在血糖正常受试者密度小于1.125 g/ml的组分中,大多数糖基化蛋白存在于高密度脂蛋白(HDL)中。采用了多种免疫化学方法来证明,在糖尿病血浆中,载脂蛋白AI、载脂蛋白AII、载脂蛋白B、载脂蛋白CI、载脂蛋白E和白蛋白都发生了糖基化。对从血糖过高的糖尿病患者中分离出的密度小于或等于1.019 g/ml的脂蛋白组分和HDL组分的载脂蛋白进行的详细研究表明,葡糖赖氨酸特异性抗体可用于制备性分离含有糖基化氨基酸残基的蛋白质,从而能够测量特定蛋白质中的糖基化程度。结果表明,在血糖过高的糖尿病患者体内,载脂蛋白的一些赖氨酸残基可通过葡萄糖的共价连接而被修饰。文中讨论了这些观察结果可能具有的意义。

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