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体外富含胆固醇和载脂蛋白E的高密度脂蛋白的形成

Formation of cholesterol- and apoprotein E-enriched high density lipoproteins in vitro.

作者信息

Gordon V, Innerarity T L, Mahley R W

出版信息

J Biol Chem. 1983 May 25;258(10):6202-12.

PMID:6343371
Abstract

The delivery of cholesterol to canine serum or plasma altered the distribution of cholesterol and apoproteins in subclasses of high density lipoproteins (HDL). In these experiments, two in vitro systems were employed. The first system used cholesterol-celite particles to deliver cholesterol to canine plasma during 4-h incubations. When the cholesterol distribution in the lipoproteins was analyzed by Geon-Pevikon electrophoresis, an increase in cholesterol content was found in the slower migrating subclasses of HDL (HDL1 and HDLc). A large increase in apoprotein E (apo-E) was also observed in the lipoproteins. Densitometric analysis of lipid-stained, 4 to 30% gradient acrylamide gels of canine plasma after incubation with cholesterol-celite revealed that the concentration of the major high density lipoproteins (HDL3) decreased, and the concentration of subclasses of HDL-with apo-E (HDL1 and HDLc) increased 2- to 5-fold. In the second system, cholesterol-loaded mouse peritoneal macrophages released cholesterol to HDL in an incubation medium containing 10 to 20% canine serum. The HDL1 and HDLc, which demonstrated slower electrophoretic mobility as determined by Geon-Pevikon block electrophoresis, became enriched in cholesterol and cholesteryl esters. Gradient gel electrophoresis showed substantial increases in these subclasses of HDL-with apo-E. The cholesterol-loaded mouse peritoneal macrophages synthesized and secreted apo-E into the medium. When L-[35S]methionine was used as a precursor, 65 to 90% of the 35S-labeled protein associated with the lipoproteins in the 1.02 to 1.09 density range was immunoprecipitated with antibody directed against rat apo-E. Gradient gel electrophoresis of density fractions demonstrated the presence of HDL1 and HDLc as the major lipoproteins. In addition, when canine 125I-HDL3 (primarily apo-A-I-containing HDL) were added to canine serum and incubated with cholesterol-loaded macrophages, the appearance of HDL1 and HDLc was associated with a marked increase in the 125I label in these newly formed, cholesteryl ester-rich lipoproteins. There was a corresponding marked reduction in the 125I-HDL3 in the serum. Similar results were observed using human HDL3 and human serum.

摘要

将胆固醇输送到犬血清或血浆中会改变高密度脂蛋白(HDL)亚类中胆固醇和载脂蛋白的分布。在这些实验中,采用了两种体外系统。第一个系统使用胆固醇-硅藻土颗粒在4小时孵育期间将胆固醇输送到犬血浆中。当通过Geon-Pevikon电泳分析脂蛋白中的胆固醇分布时,发现HDL迁移较慢的亚类(HDL1和HDLc)中的胆固醇含量增加。在脂蛋白中还观察到载脂蛋白E(apo-E)大幅增加。对与胆固醇-硅藻土孵育后的犬血浆进行脂质染色的4%至30%梯度丙烯酰胺凝胶的光密度分析显示,主要高密度脂蛋白(HDL3)的浓度降低,而含有apo-E的HDL亚类(HDL1和HDLc)的浓度增加了2至5倍。在第二个系统中,载有胆固醇的小鼠腹腔巨噬细胞在含有10%至20%犬血清的孵育培养基中将胆固醇释放到HDL中。通过Geon-Pevikon区带电泳测定,电泳迁移较慢的HDL1和HDLc富含胆固醇和胆固醇酯。梯度凝胶电泳显示这些含有apo-E的HDL亚类大幅增加。载有胆固醇的小鼠腹腔巨噬细胞合成并将apo-E分泌到培养基中。当使用L-[35S]甲硫氨酸作为前体时,密度在1.02至1.09范围内与脂蛋白相关的35S标记蛋白的65%至90%被抗大鼠apo-E抗体免疫沉淀。密度级分的梯度凝胶电泳显示HDL1和HDLc是主要脂蛋白。此外,当将犬125I-HDL3(主要含apo-A-I的HDL)添加到犬血清中并与载有胆固醇的巨噬细胞孵育时,HDL1和HDLc的出现与这些新形成的富含胆固醇酯的脂蛋白中125I标记的显著增加相关。血清中的125I-HDL3相应显著减少。使用人HDL3和人血清观察到类似结果。

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