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狒狒肝细胞原代培养物中脂蛋白(a)的细胞表面组装

Cell surface assembly of lipoprotein(a) in primary cultures of baboon hepatocytes.

作者信息

White A L, Lanford R E

机构信息

Department of Virology and Immunology, Southwest Foundation for Biomedical Research, San Antonio, Texas.

出版信息

J Biol Chem. 1994 Nov 18;269(46):28716-23.

PMID:7961823
Abstract

Lipoprotein(a) (Lp(a)) consists of a low density lipoprotein particle in which apolipoprotein(a) (apo(a)), is disulfide linked to apoB. Lp(a) is produced by the liver, and high plasma levels represent an independent risk factor for cardiovascular diseases. However, pathways of production and metabolism of Lp(a) are poorly understood. We used primary cultures of baboon hepatocytes to analyze the steps involved in Lp(a) biogenesis. The results demonstrated that Lp(a) assembly was extracellular, since it was inhibited when anti-apo(a) antiserum was present in the culture medium. In addition, free apo(a) produced by hepatocytes could associate extracellularly with apoB in either very low density or low density lipoproteins. Lp(a) assembly required lysine-binding pockets in apo(a) kringles, as it was inhibited by the lysine analog, 6-amino hexanoic acid. A portion of apo(a) was also bound to the cell surface via its kringle domains and could be released into the medium by 6-amino hexanoic acid or proline. In add-back experiments, apo(a), but not Lp(a), bound to the cell surface. Addition of low density lipoprotein or very low density lipoprotein to hepatocyte cultures released apo(a) from the cell surface into the lipoprotein fraction of culture medium. We conclude that assembly of Lp(a) can occur at the cell surface. This represents one potential mechanism of Lp(a) production in vivo.

摘要

脂蛋白(a) [Lp(a)] 由一个低密度脂蛋白颗粒和载脂蛋白(a) [apo(a)] 组成,其中apo(a) 通过二硫键与载脂蛋白B相连。Lp(a) 由肝脏产生,血浆中高水平的Lp(a) 是心血管疾病的独立危险因素。然而,Lp(a) 的产生和代谢途径目前还知之甚少。我们利用狒狒肝细胞的原代培养来分析Lp(a) 生物合成所涉及的步骤。结果表明,Lp(a) 的组装是在细胞外进行的,因为当培养基中存在抗apo(a) 抗血清时,组装过程受到抑制。此外,肝细胞产生的游离apo(a) 可以在细胞外与极低密度脂蛋白或低密度脂蛋白中的apoB结合。Lp(a) 的组装需要apo(a) kringle结构域中的赖氨酸结合口袋,因为它会被赖氨酸类似物6-氨基己酸抑制。一部分apo(a) 也通过其kringle结构域与细胞表面结合,并且可以被6-氨基己酸或脯氨酸释放到培养基中。在回补实验中,是apo(a) 而非Lp(a) 与细胞表面结合。向肝细胞培养物中添加低密度脂蛋白或极低密度脂蛋白会使apo(a) 从细胞表面释放到培养基的脂蛋白组分中。我们得出结论,Lp(a) 的组装可以在细胞表面发生。这代表了体内Lp(a) 产生的一种潜在机制。

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