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脂蛋白重塑在人体间质液中产生脂质贫乏的载脂蛋白 A-I 颗粒。

Lipoprotein remodeling generates lipid-poor apolipoprotein A-I particles in human interstitial fluid.

机构信息

Magdalen College, University of Oxford, Oxford, UK.

出版信息

Am J Physiol Endocrinol Metab. 2013 Feb 1;304(3):E321-8. doi: 10.1152/ajpendo.00324.2012. Epub 2012 Dec 11.

DOI:10.1152/ajpendo.00324.2012
PMID:23233540
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3566430/
Abstract

Although much is known about the remodeling of high density lipoproteins (HDLs) in blood, there is no information on that in interstitial fluid, where it might have a major impact on the transport of cholesterol from cells. We incubated plasma and afferent (prenodal) peripheral lymph from 10 healthy men at 37°C in vitro and followed the changes in HDL subclasses by nondenaturing two-dimensional crossed immunoelectrophoresis and size-exclusion chromatography. In plasma, there was always initially a net conversion of small pre-β-HDLs to cholesteryl ester (CE)-rich α-HDLs. By contrast, in lymph, there was only net production of pre-β-HDLs from α-HDLs. Endogenous cholesterol esterification rate, cholesteryl ester transfer protein (CETP) concentration, CE transfer activity, phospholipid transfer protein (PLTP) concentration, and phospholipid transfer activity in lymph averaged 5.0, 10.4, 8.2, 25.0, and 82.0% of those in plasma, respectively (all P < 0.02). Lymph PLTP concentration, but not phospholipid transfer activity, was positively correlated with that in plasma (r = +0.63, P = 0.05). Mean PLTP-specific activity was 3.5-fold greater in lymph, reflecting a greater proportion of the high-activity form of PLTP. These findings suggest that cholesterol esterification rate and PLTP specific activity are differentially regulated in the two matrices in accordance with the requirements of reverse cholesterol transport, generating lipid-poor pre-β-HDLs in the extracellular matrix for cholesterol uptake from neighboring cells and converting pre-β-HDLs to α-HDLs in plasma for the delivery of cell-derived CEs to the liver.

摘要

虽然人们对血液中高密度脂蛋白(HDL)的重塑过程了解颇多,但对于细胞外间质中的情况却知之甚少,而这一过程可能对胆固醇从细胞内向细胞外的转运产生重大影响。我们在 37°C 体外培养了 10 名健康男性的血浆和输入(前结)外周淋巴液,并通过非变性二维交叉免疫电泳和分子筛层析法,追踪 HDL 亚类的变化。在血浆中,小 pre-β-HDL 最初总是会向富含胆固醇酯(CE)的α-HDL 发生净转化。相比之下,在淋巴液中,只有α-HDL 会净生成 pre-β-HDL。内源性胆固醇酯化率、胆固醇酯转移蛋白(CETP)浓度、CE 转移活性、磷脂转移蛋白(PLTP)浓度和磷脂转移活性在淋巴液中的平均值分别为血浆中的 5.0、10.4、8.2、25.0 和 82.0%(均 P < 0.02)。淋巴液 PLTP 浓度与血浆中的浓度呈正相关(r = +0.63,P = 0.05),但磷脂转移活性无此相关性。淋巴液中 PLTP 比活是血浆的 3.5 倍,这反映了 PLTP 高活性形式所占比例较大。这些发现表明,胆固醇酯化率和 PLTP 比活在两种基质中是根据胆固醇反向转运的需要进行差异调节的,在细胞外基质中生成富含脂质的 pre-β-HDL,以从邻近细胞摄取胆固醇,并在血浆中将 pre-β-HDL 转化为α-HDL,以便将细胞来源的 CE 运送到肝脏。

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