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血浆低密度和高密度脂蛋白中游离及酯化胆固醇与载脂蛋白的代谢

Metabolism of free and esterified cholesterol and apolipoproteins of plasma low and high density lipoproteins.

作者信息

Portman O W, Alexander M, O'Malley J P

出版信息

Biochim Biophys Acta. 1980 Sep 8;619(3):545-58. doi: 10.1016/0005-2760(80)90106-x.

Abstract

We studied the patterns of equilibration of free and esterified cholesterol between lipoprotein fractions of plasma separated by heparin-Mn2+ and of their disappearance from plasma and appearance in liver and bile. Free or esterified [4-14C]cholesterol in low density lipoproteins (LDL) and [7(n)-3H]cholesterol in high density lipoproteins (HDL2 or HDL3) were incubated together with plasma or injected simultaneously into squirrel monkeys. The isotope was alternated for successive experiments. Free cholesterol was equilibrated completely between lipoprotein classes within 30-45 min, but esterified cholesterol was not completely equilibrated within 2 h. Within 10 min after the injection of lipoproteins that had labeled free cholesterol, the bile contained labeled free cholesterol and within 20 min labeled bile acids. Both biliary cholesterol and bile acids initially were enriched 5-10-fold with the isotope that was originally contained in plasma HDL. Hepatic cholesterol was less enriched than bile cholesterol with the isotope of HDL. There was much less incorporation of radioactivity into biliary cholesterol and bile acids after the injection of [7(n)-3H]cholesteryl esters in HDL2 or HDL3 and [4-14C]cholesterol esters in LDL than after labeled free cholesterol, and there was little preference for cholesterol from one lipoprotein class. Although cholesteryl esters were equilibrated slowly between lipoprotein classes, their overall rate of removal from plasma was identical to that for the apolipoproteins of 125I-labeled LDL and 125I-labeled HDL during the first 2 h after injection. Labeled free cholesterol initially disappeared from the plasma compartment several times more rapidly than the esterified form or the lipoprotein apolipoprotein. Thus, cholesteryl esters probably interact with cells as part of intact lipoproteins, since they are not exchanged with cellular cholesterol like plasma free cholesterol.

摘要

我们研究了通过肝素 - Mn²⁺ 分离的血浆脂蛋白组分中游离胆固醇和酯化胆固醇的平衡模式,以及它们从血浆中消失并出现在肝脏和胆汁中的情况。将低密度脂蛋白(LDL)中的游离或酯化[4 - ¹⁴C]胆固醇与高密度脂蛋白(HDL₂ 或 HDL₃)中的[7(n)-³H]胆固醇与血浆一起孵育,或同时注射到松鼠猴体内。在连续实验中交替使用同位素。游离胆固醇在30 - 45分钟内在脂蛋白类别之间完全平衡,但酯化胆固醇在2小时内未完全平衡。在注射标记有游离胆固醇的脂蛋白后10分钟内,胆汁中含有标记的游离胆固醇,20分钟内含有标记的胆汁酸。最初,胆汁中的胆固醇和胆汁酸都富含血浆HDL中最初含有的同位素5 - 10倍。肝脏胆固醇的同位素富集程度低于胆汁胆固醇。与注射标记的游离胆固醇后相比,注射HDL₂ 或 HDL₃ 中的[7(n)-³H]胆固醇酯和LDL中的[4 - ¹⁴C]胆固醇酯后,进入胆汁胆固醇和胆汁酸的放射性掺入要少得多,并且对来自一种脂蛋白类别的胆固醇几乎没有偏好。尽管胆固醇酯在脂蛋白类别之间平衡缓慢,但在注射后的前2小时内,它们从血浆中的总体清除率与¹²⁵I标记的LDL和¹²⁵I标记的HDL的载脂蛋白相同。标记的游离胆固醇最初从血浆区室消失的速度比酯化形式或脂蛋白载脂蛋白快几倍。因此,胆固醇酯可能作为完整脂蛋白的一部分与细胞相互作用,因为它们不像血浆游离胆固醇那样与细胞胆固醇进行交换。

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