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培养的小鼠巨噬细胞泡沫细胞中胆固醇酯循环的形态学特征

Morphological characterization of the cholesteryl ester cycle in cultured mouse macrophage foam cells.

作者信息

McGookey D J, Anderson R G

出版信息

J Cell Biol. 1983 Oct;97(4):1156-68. doi: 10.1083/jcb.97.4.1156.

Abstract

Mouse peritoneal macrophages can be induced to accumulate cholesteryl esters by incubating them in the presence of acetylated low density lipoprotein. The cholesteryl esters are sequestered in neutral lipid droplets that remain in the cell even when the acetylated low density lipoprotein is removed from the culture media. Previous biochemical studies have determined that the cholesterol component of cholesteryl ester droplets constantly turns over with a half time of 24 h by a cyclic process of de-esterification and re-esterification. We have used morphologic techniques to determine the spatial relationship of cholesteryl ester, free cholesterol, and lipase activity during normal turnover and when turnover is disrupted. Lipid droplets were surrounded by numerous 7.5-10.0-nm filaments; moreover, at focal sites on the margin of each droplet there were whorles of concentrically arranged membrane that penetrated the matrix. Histochemically detectable lipase activity was associated with these stacks of membrane. Using filipin as a light and electron microscopic probe for free cholesterol, we determined that a pool of free cholesterol was associated with each lipid droplet. Following incubation in the presence of the exogenous cholesterol acceptor, high density lipoprotein, the cholesteryl ester droplets disappeared and were replaced with lipid droplets of a different lipid composition. Inhibition of cholesterol esterification caused cholesteryl ester droplets to disappear and free cholesterol to accumulate in numerous myelin-like structures in the body of the cell.

摘要

通过在乙酰化低密度脂蛋白存在的情况下孵育,可诱导小鼠腹腔巨噬细胞积累胆固醇酯。即使从培养基中去除乙酰化低密度脂蛋白,胆固醇酯仍会被隔离在中性脂滴中并留在细胞内。以往的生化研究已确定,胆固醇酯滴中的胆固醇成分通过脱酯化和再酯化的循环过程持续周转,半衰期为24小时。我们已使用形态学技术来确定正常周转期间以及周转中断时胆固醇酯、游离胆固醇和脂肪酶活性的空间关系。脂滴被众多7.5 - 10.0纳米的细丝包围;此外,在每个脂滴边缘的焦点部位,有同心排列的膜的涡旋结构穿透基质。组织化学可检测到的脂肪酶活性与这些膜堆叠相关。使用 Filipin 作为游离胆固醇的光学和电子显微镜探针,我们确定每个脂滴都有一个游离胆固醇池。在存在外源性胆固醇受体高密度脂蛋白的情况下孵育后,胆固醇酯滴消失,取而代之的是具有不同脂质组成的脂滴。抑制胆固醇酯化会导致胆固醇酯滴消失,游离胆固醇在细胞体内的许多髓鞘样结构中积累。

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