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完整肝细胞中甘油三酯和磷脂与极低密度脂蛋白糖基化和非糖基化载脂蛋白的缔合及组装

Association and assembly of triglyceride and phospholipid with glycosylated and unglycosylated apoproteins of very low density lipoprotein in the intact liver cell.

作者信息

Siuta-Mangano P, Janero D R, Lane M D

出版信息

J Biol Chem. 1982 Oct 10;257(19):11463-7.

PMID:7118891
Abstract

Using estrogen-induced chick liver cells which synthesize and secrete large amounts of very low density lipoprotein (VLDL), we have previously shown (Siuta-Mangano, P., Howard, S., Lennarz, W. J., and Lane, M. D. (1982) J. Biol. Chem. 257, 4292-4300) that the major protein constituent of VLDL, the 350,000 molecular weight apoprotein (apoprotein B), is synthesized as a single polypeptide to which core oligosaccharides are added co-translationally. This system has now been employed to study the assembly of the apoproteins of VLDL with their glycerolipid (triglyceride and phospholipid) components and the secretion of the VLDL glycerolipids. In the presence of cycloheximide such that VLDL apoprotein synthesis is inhibited 98%, the secretion of lipids labeled from a [3H]palmitate pulse by hepatocyte monolayers was halted only after completed apoprotein chains had cleared the cell. Under conditions whereby tunicamycin inhibited [3H]glucosamine incorporation into apoprotein B by 98% and [3H]leucine incorporation into the VLDL apoproteins minimally, the unglycosylated form of apoprotein B assembled with the usual complement of triglyceride and phospholipid as did glycosylated apoprotein B to form a VLDL which was readily secreted by the hepatocyte. Taken together, these findings demonstrate that whereas apoprotein synthesis is necessary for the secretion of the major lipid components of VLDL, glycosylation of apoprotein B is not required for either the assembly of VLDL glycerolipids or for the secretion of the VLDL particle.

摘要

利用雌激素诱导的鸡肝细胞,其能合成并分泌大量极低密度脂蛋白(VLDL),我们先前已经表明(休塔 - 曼加诺,P.,霍华德,S.,伦纳兹,W. J.,和莱恩,M. D.(1982年)《生物化学杂志》257,4292 - 4300),VLDL的主要蛋白质成分,分子量为350,000的载脂蛋白(载脂蛋白B),是以单一多肽形式合成的,核心寡糖在翻译过程中与之共翻译添加。现在这个系统已被用于研究VLDL载脂蛋白与它们的甘油脂质(甘油三酯和磷脂)成分的组装以及VLDL甘油脂质的分泌。在存在环己酰亚胺使得VLDL载脂蛋白合成被抑制98%的情况下,肝细胞单层细胞用[3H]棕榈酸脉冲标记的脂质的分泌仅在完整的载脂蛋白链清除细胞后才停止。在衣霉素抑制[3H]葡糖胺掺入载脂蛋白B达98%且[3H]亮氨酸掺入VLDL载脂蛋白最少的条件下,未糖基化形式的载脂蛋白B与甘油三酯和磷脂的正常成分组装,糖基化的载脂蛋白B也是如此,形成一种VLDL,其很容易被肝细胞分泌。综上所述,这些发现表明,虽然载脂蛋白合成对于VLDL主要脂质成分的分泌是必要的,但载脂蛋白B的糖基化对于VLDL甘油脂质的组装或VLDL颗粒的分泌都不是必需的。

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