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不同分子种类的磷脂酰胆碱对大鼠脂蛋白重组体中胆固醇转运的影响。

Influence of different molecular species of phosphatidylcholine on cholesterol transport from lipoprotein recombinants in the rat.

作者信息

Leduc R, Patton G M, Atkinson D, Robins S J

出版信息

J Biol Chem. 1987 Jun 5;262(16):7680-5.

PMID:3584136
Abstract

Studies were performed to determine to what extent phosphatidylcholines (PCs) of different composition influence the turnover of lipoprotein cholesterol. Lipoprotein recombinants with the composition and structure of spherical high density lipoproteins (HDL-R) were prepared with apoproteins, 14C-labeled unesterified cholesterol (UC), a [3H]cholesteryl ester (CE), and one of four single molecular species of PC. PCs were selected to include relatively hydrophilic species (16:1-16:1 and 16:0-18:2 PCs) and relatively hydrophobic species (18:0-18:2 and 20:1-20:1 PCs). PCs were also selected to include molecules with novel acyl group pairs (16:1-16:1 and 20:1-20:1 PCs) that would permit the whole molecule to be traced during its clearance from the serum. Rats were injected with HDL-R as an intravenous bolus, and serum, liver, and bile samples were obtained for up to 2 h. The clearance from the serum of each PC was monoexponential with the two most hydrophilic species much more rapidly cleared than either of the two less hydrophilic species. Clearance of specific PCs was not accompanied by PC remodeling (i.e. transacylations), and in the main could not be attributed to the action of lecithin-cholesterol acyltransferase (LCAT). In incubations designed to simulate in vivo conditions, no more than 15% of the disappearance of 16:1-16:1 PC, one of the most rapidly cleared PCs, was due to the action of LCAT. With 20:1-20:1 PC, one of the least rapidly cleared PCs, no LCAT activity could be detected. The clearance of radiolabeled UC was multiexponential and closely corresponded to the rate of disappearance of each PC. The clearance of radiolabeled CE was linear and, in contrast to UC, was the same with the administration of different PCs. Uptake of radiolabeled UC by the liver and excretion of radiolabeled UC into bile took place in parallel and corresponded to the rapidity of turnover of UC (and PCs) in the serum. With administration of 16:1-16:1 PC, complete equilibration of serum, liver, and bile UC was achieved by about 90 min, whereas with 20:1-20:1 PC, serum UC had not equilibrated by the end of the study. These findings demonstrate that, in the live animal, the kinetic pattern of transport of different lipids from an HDL recombinant is highly disparate, the rate of PC clearance is more rapid with molecular species of greater hydrophilic strength, and the rates of PC and UC clearance are closely coordinated and largely independent of the clearance of CE.

摘要

开展了多项研究以确定不同组成的磷脂酰胆碱(PCs)在多大程度上影响脂蛋白胆固醇的周转。用载脂蛋白、14C标记的未酯化胆固醇(UC)、[3H]胆固醇酯(CE)以及四种PC单分子种类之一制备了具有球形高密度脂蛋白(HDL-R)组成和结构的脂蛋白重组体。选择的PCs包括相对亲水的种类(16:1-16:1和16:0-18:2 PCs)和相对疏水的种类(18:0-18:2和20:1-20:1 PCs)。还选择了具有新型酰基对的分子(16:1-16:1和20:1-20:1 PCs),以便在其从血清中清除的过程中追踪整个分子。将HDL-R作为静脉推注注入大鼠体内,并在长达2小时内获取血清、肝脏和胆汁样本。每种PC从血清中的清除呈单指数形式,两种最亲水的种类比两种亲水性较差的种类清除得快得多。特定PC的清除未伴随PC重塑(即转酰基作用),并且在主要方面不能归因于卵磷脂胆固醇酰基转移酶(LCAT)的作用。在旨在模拟体内条件的孵育中,16:1-16:1 PC(清除最快的PCs之一)消失的不超过15%是由于LCAT的作用。对于20:1-20:1 PC(清除最慢的PCs之一),未检测到LCAT活性。放射性标记的UC的清除是多指数的,并且与每种PC的消失速率密切对应。放射性标记的CE的清除是线性的,与UC相反,在给予不同PC时是相同的。肝脏对放射性标记的UC的摄取和放射性标记的UC向胆汁中的排泄同时发生,并且与血清中UC(和PCs)的周转速度相对应。给予16:1-16:1 PC时,血清、肝脏和胆汁UC在约90分钟时达到完全平衡,而给予20:1-20:1 PC时,在研究结束时血清UC尚未达到平衡。这些发现表明,在活体动物中,来自HDL重组体的不同脂质的转运动力学模式差异很大,具有更大亲水强度的分子种类的PC清除速率更快,并且PC和UC的清除速率密切协调且在很大程度上独立于CE的清除。

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