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灌注大鼠肝脏对极低密度脂蛋白及其残粒中胆固醇的摄取。

Uptake of cholesterol from the very low density lipoprotein or its remnants by the perfused rat liver.

作者信息

Noël S P, Rubinstein D

出版信息

Can J Biochem. 1981 Jun;59(6):447-53. doi: 10.1139/o81-062.

Abstract

[3H]Cholesterol labelled very low density lipoproteins ([3H]chol-VLDL) were prepared to study the hepatic uptake of cholesterol associated with VLDL and its remnants in the perfused liver system. [3H]Chol-VLDL was incubated with rat postheparin plasma to produce labelled remnants in vitro. The degree of lipolysis of [3H]chol-VLDL depended on the ratio of triacylglycerols to lipase in the incubation medium. Therefore, the produced remnant of d less than 1.019 g. mL-1 had a variable lipid composition depending on the degree of lipolysis. [3H]Chol-VLDL or its remnants were added to liver perfusate and the radioactivity remaining in the perfusate was measured. The kinetic disappearance of [3H]chol-VLDL and its remnants in the perfused liver system indicated that remnant of d less than 1.019 g. mL-1 was taken up by the liver faster than the original VLDL preparation (t1/2 of 8 min vs. 51 min). Appearance of the label in bile during the perfusion was significantly faster when livers were perfused with [3H]chol-VLDL remnants as opposed to uncatabolized [3H]chol-VLDL. The results indicate that first of all, VLDL remnants produced in vitro and reisolated at density less than 1.019 g.mL-1 do not have a fixed lipid composition but a rather variable one depending on the degree of lipolysis. Secondly, the rat liver may preferentially recognize this VLDL remnant of d less than 1.019 g.mL-1 and take it up more readily than uncatabolized VLDL. Finally when equimolar amount of cholesterol from VLDL or VLDL remnants are circulated in the liver perfusion, the VLDL remnants convey a significantly greater mass of cholesterol in the bile.

摘要

制备了[3H]胆固醇标记的极低密度脂蛋白([3H]胆固醇-VLDL),以研究在灌注肝脏系统中与VLDL及其残粒相关的胆固醇的肝脏摄取情况。将[3H]胆固醇-VLDL与大鼠肝素后血浆一起孵育,以在体外产生标记的残粒。[3H]胆固醇-VLDL的脂解程度取决于孵育介质中三酰甘油与脂肪酶的比例。因此,产生的密度小于1.019 g·mL-1的残粒具有可变的脂质组成,这取决于脂解程度。将[3H]胆固醇-VLDL或其残粒添加到肝脏灌注液中,并测量灌注液中剩余的放射性。[3H]胆固醇-VLDL及其残粒在灌注肝脏系统中的动力学消失表明,密度小于1.019 g·mL-1的残粒比原始的VLDL制剂被肝脏摄取得更快(半衰期分别为8分钟和51分钟)。当肝脏用[3H]胆固醇-VLDL残粒灌注而不是未分解代谢的[3H]胆固醇-VLDL灌注时,灌注期间胆汁中标记物的出现明显更快。结果表明,首先,体外产生并重新分离出的密度小于1.019 g·mL-1的VLDL残粒没有固定的脂质组成,而是根据脂解程度具有相当可变的脂质组成。其次,大鼠肝脏可能优先识别这种密度小于1.019 g·mL-1的VLDL残粒,并比未分解代谢的VLDL更容易摄取它。最后,当等量的来自VLDL或VLDL残粒的胆固醇在肝脏灌注中循环时,VLDL残粒在胆汁中携带的胆固醇量明显更大。

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