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大鼠乳糜微粒代谢:动力学模型表明,这些颗粒在血管内皮部位停留数分钟。

Chylomicron metabolism in rats: kinetic modeling indicates that the particles remain at endothelial sites for minutes.

机构信息

Departments of Surgical and Perioperative Sciences, Anaesthesiology and Intensive Care, Umeå University, S-901 87 Umeå, Sweden.

出版信息

J Lipid Res. 2013 Oct;54(10):2595-605. doi: 10.1194/jlr.M032979. Epub 2013 Aug 6.

Abstract

Chylomicrons labeled in vivo with (14)C-oleic acid (primarily in triglycerides, providing a tracer for lipolysis) and (3)H-retinol (primarily in ester form, providing a tracer for the core lipids) were injected into rats. Radioactivity in tissues was followed at a series of times up to 40 min and the data were analyzed by compartmental modeling. For heart-like tissues it was necessary to allow the chylomicrons to enter into a compartment where lipolysis is rapid and then transfer to a second compartment where lipolysis is slower. The particles remained in these compartments for minutes and when they returned to blood they had reduced affinity for binding in the tissue. In contrast, the data for liver could readily be fitted with a single compartment for native and lipolyzed chylomicrons in blood, and there was no need for a pathway back to blood. A composite model was built from the individual tissue models. This whole-body model could simultaneously fit all data for both fed and fasted rats and allowed estimation of fluxes and residence times in the four compartments; native and lipolyzed chylomicrons ("remnants") in blood, and particles in the tissue compartments where lipolysis is rapid and slow, respectively.

摘要

用 (14)C-油酸(主要在甘油三酯中,提供脂肪分解的示踪剂)和 (3)H-视黄醇(主要以酯的形式存在,提供核心脂质的示踪剂)对活体标记的乳糜微粒进行注射。在多达 40 分钟的一系列时间内跟踪组织中的放射性,并通过房室模型分析数据。对于类似心脏的组织,需要允许乳糜微粒进入一个脂肪分解迅速的隔室,然后转移到第二个脂肪分解较慢的隔室。这些颗粒在这些隔室中停留几分钟,当它们返回血液时,它们与组织的结合亲和力降低。相比之下,肝脏的数据可以很容易地用一个隔室拟合血液中的天然和脂肪分解的乳糜微粒,并且不需要回到血液的途径。从个体组织模型构建了一个综合模型。这个全身模型可以同时拟合进食和禁食大鼠的所有数据,并允许估计四个隔室中的通量和停留时间;血液中的天然和脂肪分解的乳糜微粒(“残片”),以及脂肪分解迅速和缓慢的组织隔室中的颗粒。

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