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大鼠肝脏极低密度脂蛋白的生物合成。载脂蛋白B的细胞内分布。

Biogenesis of very-low-density lipoproteins in rat liver. Intracellular distribution of apolipoprotein B.

作者信息

Wong L, Pino R M

出版信息

Eur J Biochem. 1987 Apr 15;164(2):357-67. doi: 10.1111/j.1432-1033.1987.tb11066.x.

Abstract

The hepatic subcellular distribution of apolipoprotein B (apo B) was studied quantitatively by using an enzyme immunoassay developed for apo B and by immunoadsorption-precipitation of [3H]leucine-labelled apo B. Over 50% (of 0.59 microgram/mg protein) of the apo B was located in the microsomal fraction. Further subfractionation of the microsomes revealed that 47% of the microsomal apo B was in the Golgi apparatus, while another 43% was associated with the rough endoplasmic reticulum. The smooth endoplasmic reticulum accounted for only 4% of the total. When rat livers were labelled with [3H]leucine for 10 min, the rough endoplasmic reticulum accounted for 80% of the total immunoadsorbed precipitable apo B radioactivity while the smooth accounted for 20%, with no contribution from the Golgi. However, only 8.7% of the total radioactive immunoadsorbed precipitable apo B was lipoprotein-associated, the remainder being membrane-bound. Lipoprotein-associated apo B radioactivity in the smooth endoplasmic reticulum accounted for 40%, with the rough contribution attributed at 50% and the Golgi at 9%. We concluded that (a) there are two major pools of apo B in rat liver microsomes; (b) although the apo B mass may be negligible in the smooth endoplasmic reticulum, the latter does play a role in lipoprotein biogenesis. The possible function of apo B associated with membranes of the microsomes is also discussed.

摘要

利用为载脂蛋白B(apo B)开发的酶免疫测定法以及[3H]亮氨酸标记的apo B的免疫吸附沉淀法,对apo B在肝脏亚细胞中的分布进行了定量研究。超过50%(每毫克蛋白质含0.59微克)的apo B位于微粒体部分。对微粒体进一步分级分离显示,47%的微粒体apo B存在于高尔基体中,另有43%与粗面内质网相关。滑面内质网仅占总量的4%。用[3H]亮氨酸标记大鼠肝脏10分钟时,粗面内质网占免疫吸附沉淀的apo B放射性总量的80%,滑面内质网占20%,高尔基体无贡献。然而,免疫吸附沉淀的放射性apo B总量中只有8.7%与脂蛋白相关,其余为膜结合形式。滑面内质网中与脂蛋白相关的apo B放射性占4%,粗面内质网占50%,高尔基体占9%。我们得出结论:(a)大鼠肝脏微粒体中有两个主要的apo B池;(b)尽管滑面内质网中的apo B质量可能微不足道,但后者在脂蛋白生物合成中确实发挥作用。还讨论了与微粒体膜相关的apo B的可能功能。

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