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人脂肪细胞对高密度脂蛋白胆固醇酯的选择性摄取。

Selective uptake of HDL cholesterol ester by human fat cells.

作者信息

Despres J P, Fong B S, Jimenez J, Julien P, Angel A

机构信息

Institute of Medical Science, University of Toronto, Ontario, Canada.

出版信息

Am J Physiol. 1988 May;254(5 Pt 1):E667-75. doi: 10.1152/ajpendo.1988.254.5.E667.

Abstract

In humans, high-density lipoprotein (HDL)-cholesterol ester turnover exceeds that of HDL apoproteins by severalfold or more, suggesting an independent catabolic fate of these constituents. The present study investigated the cellular uptake and dissociation of HDL labeled in its apoproteins with 125I and in its cholesterol ester with [3H]cholesteryl palmityl ether, a nonhydrolyzable cholesterol ester analogue. Approximately 50% of cell-associated 125I-HDL2 and 125I-HDL3 was released from prelabeled adipose cells by incubating the latter in the presence or absence of unlabeled lipoproteins for 2 h. The uptake of HDL-cholesterol ester by human fat cells as reflected by [3H]cholesteryl palmityl ether was 5-18 times greater than that predicted from the uptake of 125I-HDL2 and 125I-HDL3 and was irreversible. Analysis of dissociated 125I-HDL3 demonstrated changes to both higher and lower density fractions compared with the starting material. There was a high correlation between the cellular uptake of HDL3-cholesterol ester and HDL3-apoprotein uptakes (r = 0.90, P less than 0.01), suggesting that HDL-cholesterol ester uptake requires a specific apoprotein interaction or binding step. The selective uptake and retention of HDL-cholesterol ester by isolated adipocytes implies that human fat tissue may play a role in regulating the lipid composition of plasma HDL.

摘要

在人类中,高密度脂蛋白(HDL)胆固醇酯的周转率比HDL载脂蛋白的周转率高出数倍甚至更多,这表明这些成分具有独立的分解代谢命运。本研究调查了用125I标记载脂蛋白以及用[3H]胆固醇棕榈醚(一种不可水解的胆固醇酯类似物)标记胆固醇酯的HDL的细胞摄取和解离情况。通过将预先标记的脂肪细胞在有无未标记脂蛋白的情况下孵育2小时,约50%与细胞结合的125I - HDL2和125I - HDL3从脂肪细胞中释放出来。[3H]胆固醇棕榈醚所反映的人脂肪细胞对HDL胆固醇酯的摄取比根据125I - HDL2和125I - HDL3的摄取所预测的高5 - 18倍,且这种摄取是不可逆的。对解离的125I - HDL3的分析表明,与起始物质相比,其密度分数既有升高也有降低。HDL3胆固醇酯的细胞摄取与HDL3载脂蛋白摄取之间存在高度相关性(r = 0.90,P < 0.01),这表明HDL胆固醇酯的摄取需要特定的载脂蛋白相互作用或结合步骤。分离的脂肪细胞对HDL胆固醇酯的选择性摄取和保留意味着人体脂肪组织可能在调节血浆HDL的脂质组成中发挥作用。

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