大鼠肝细胞单层对胆固醇酯标记的乳糜微粒残余颗粒的结合、内化和降解

Binding, interiorization and degradation of cholesteryl ester-labelled chylomicron-remmant particles by rat hepatocyte monolayers.

作者信息

Florén C H, Nilsson A

出版信息

Biochem J. 1977 Dec 15;168(3):483-94. doi: 10.1042/bj1680483.

DOI:10.1042/bj1680483

PMID:204289

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1183796/

Abstract

The cholesteryl ester of isolated chylomicron-remnant particles was efficiently degraded by hepatocyte monolayers. The degradation was sensitive to metabolic inhibitors. 2. With increasing amounts of remnant cholesteryl ester the rate of uptake approached saturation and conformed to a linear double-reciprocal plot. The V(max.) was determined as 80ng of cholesteryl ester/h per mg of protein and the apparent K(m) as 1.4mug of cholesteryl ester per mg of protein. The time course for the uptake and hydrolysis suggested that binding of particles to the cell surface preceded the degradation. 3. Cholesteryl esters of native chylomicrons were degraded to a much smaller extent and their presence had only a small inhibitory effect on the degradation of chylomicron remnants. Intestinal very-low-density lipoproteins were degraded somewhat faster than chylomicrons, and caused more inhibition of remnant degradation. Rat high-density lipoproteins inhibited the hydrolysis of remnant cholesteryl ester by up to 50%, but had less influence on the amount of cholesteryl ester that was bound to the cells. Serum decreased both the uptake and hydrolysis, whereas d=1.21 infranatant had no effect. 4. The cholesteryl ester hydrolysis after the uptake by the cells was inhibited by chloroquine and by colchicine. Only 28-36% of the unhydrolysed cholesteryl ester could be released from these cells by trypsin treatment, indicating that the major portion was truly intracellular. The particles that could be released from the cell surface by trypsin and those remaining in the medium had the same triacylglycerol/cholesteryl ester ratio as the added remnant particles. Significant amounts of denser particles were thus not formed during contact with the cell surface. 5. The presence of heparin, as well as preincubation of the cells with heparin, increased the uptake of chylomicron remnants. This effect was most marked in the presence of serum. A much smaller proportion of the other serum lipoproteins was taken up, and this proportion was not increased by heparin.

摘要

分离出的乳糜微粒残粒的胆固醇酯能被肝细胞单层有效降解。这种降解对代谢抑制剂敏感。2. 随着残粒胆固醇酯量的增加，摄取速率接近饱和，并符合线性双倒数图。最大反应速度（V(max.)）测定为每毫克蛋白质每小时80纳克胆固醇酯，表观米氏常数（K(m)）为每毫克蛋白质1.4微克胆固醇酯。摄取和水解的时间进程表明，颗粒与细胞表面的结合先于降解。3. 天然乳糜微粒的胆固醇酯降解程度小得多，其存在对乳糜微粒残粒的降解仅有微小的抑制作用。肠道极低密度脂蛋白的降解比乳糜微粒稍快，且对残粒降解的抑制作用更大。大鼠高密度脂蛋白对残粒胆固醇酯水解的抑制作用高达50%，但对与细胞结合的胆固醇酯量影响较小。血清降低了摄取和水解，而密度为1.21的下层清液则无影响。4. 细胞摄取后胆固醇酯的水解受到氯喹和秋水仙碱的抑制。经胰蛋白酶处理后，只有28% - 36%未水解的胆固醇酯能从这些细胞中释放出来，这表明大部分胆固醇酯确实在细胞内。能被胰蛋白酶从细胞表面释放的颗粒以及留在培养基中的颗粒，其甘油三酯/胆固醇酯比值与添加的残粒颗粒相同。因此，在与细胞表面接触期间未形成大量密度更高的颗粒。5. 肝素的存在以及细胞与肝素的预孵育增加了乳糜微粒残粒的摄取。在有血清存在时这种作用最为明显。其他血清脂蛋白的摄取比例要小得多，且该比例不会因肝素而增加。