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载脂蛋白B在大鼠体内在结构和代谢上具有异质性。

Apolipoprotein B is structurally and metabolically heterogeneous in the rat.

作者信息

Elovson J, Huang Y O, Baker N, Kannan R

出版信息

Proc Natl Acad Sci U S A. 1981 Jan;78(1):157-61. doi: 10.1073/pnas.78.1.157.

Abstract

Electrophoresis of rat apolipoprotein B (apoB) on 5% polyacrylamide gels in the presence of NaDodSO4 separates three major components: PI, which comigrates with human low density lipoprotein (LDL) apoB; PII, a slightly faster-moving satellite band; and PIII, which migrates somewhat more slowly than myosin heavy chain. The proportion of PIII decreases with increasing density of the parent rat lipoprotein, from 90% an 70%, respectively, in chylomicrons and very low density lipoproteins (VLDL), to 7% in the major LDL2 (density 1.038-1.063 g/ml) fraction. A major component that comigrates with rat PIII is a marker for human chylomicron apoB, being absent from human VLDL, intermediate density lipoprotein (IDL), and LDL. Preliminary immunological and peptide mapping data show that rat apoB PI and PIII are closely related structurally, with the latter possibly being a large fragment of the former. Both peptides are synthesized in rat liver and found in Golgi secretory vesicles. Kinetic tracer experiments show that rat PI and PIII are present on separate VLDL particles, both of which are extensively removed from the circulation at the remnant stage, and that the declining PIII-to-PI/II ratios in IDL and LDL may be attributed to the more rapid turnover of PIII-containing lipoproteins at all levels, particularly within the LDL density range.

摘要

在十二烷基硫酸钠(NaDodSO4)存在的情况下,将大鼠载脂蛋白B(apoB)在5%聚丙烯酰胺凝胶上进行电泳,可分离出三个主要成分:PI,它与人类低密度脂蛋白(LDL)的apoB迁移率相同;PII,一条迁移稍快的卫星带;以及PIII,其迁移速度比肌球蛋白重链稍慢。PIII的比例随着大鼠母体脂蛋白密度的增加而降低,在乳糜微粒和极低密度脂蛋白(VLDL)中分别为90%和70%,在主要的LDL2(密度1.038 - 1.063 g/ml)组分中降至7%。与大鼠PIII迁移率相同的一个主要成分是人类乳糜微粒apoB的标志物,在人类VLDL、中间密度脂蛋白(IDL)和LDL中不存在。初步的免疫学和肽图谱数据表明,大鼠apoB PI和PIII在结构上密切相关,后者可能是前者的一个大片段。这两种肽都在大鼠肝脏中合成,并存在于高尔基体分泌小泡中。动力学示踪实验表明,大鼠PI和PIII存在于不同的VLDL颗粒上,这两种颗粒在残余阶段都从循环中大量清除,并且IDL和LDL中PIII与PI/II比值的下降可能归因于含PIII的脂蛋白在各个水平上,特别是在LDL密度范围内的更快周转。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bd64/319010/99ead0066d76/pnas00652-0181-a.jpg

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