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载脂蛋白III在成年烟草天蛾体内脂蛋白相互转化中的作用。

The role of apolipophorin III in in vivo lipoprotein interconversions in adult Manduca sexta.

作者信息

Wells M A, Ryan R O, Kawooya J K, Law J H

出版信息

J Biol Chem. 1987 Mar 25;262(9):4172-6.

PMID:3558406
Abstract

Sustained flight in the moth, Manduca sexta, necessitates lipid mobilization and transport to flight muscle, a process mediated by the adipokinetic hormone. An adult specific high density lipophorin (lipoprotein, HDLp-A, Mr = 7.68 X 10(5)) accepts diacylglycerol from the fat body, increasing in size and decreasing in density, to give a low density lipophorin (lipoprotein, LDLp, Mr = 1.56 X 10(6)). During this process, several molecules of the small apolipoprotein, apolipophorin III (apoLp-III), are added to the two molecules originally present in HDLp-A. A study of the time course of adipokinetic hormone-induced loading of diacylglycerol onto HDLp-A, using the analytical ultracentrifuge and gel filtration, suggests that a lipoprotein of density intermediate between HDLp-A and LDLp was formed transiently. Analysis of lipoproteins separated by density gradient ultracentrifugation in the course of the loading process indicates that apoLp-III is added more rapidly than diacylglycerol and that it changes its conformation on the surface as more diacylglycerol is added. Taken together with the known properties of apoLp-III, a prolate ellipsoid with an axial ratio of 3, we suggest that initially apoLp-III adds to the expanded hydrophobic surface of the lipoprotein with its short axis parallel to the surface and that apoLp-III subsequently unfolds to cover a greater area of hydrophobic surface. Exchange experiments with labeled apoLp-III showed that the two apoLp-III molecules in HDLp-A do not exchange with free apoLp-III, even when the lipoprotein passed through a loading and unloading cycle, suggesting a structural role for apoLp-III in HDLp-A.

摘要

烟草天蛾的持续飞行需要脂质动员并运输到飞行肌,这一过程由促脂动激素介导。一种成年特异性高密度脂蛋白(脂蛋白,HDLp-A,Mr = 7.68 X 10(5))从脂肪体接受二酰甘油,体积增大且密度降低,从而形成低密度脂蛋白(脂蛋白,LDLp,Mr = 1.56 X 10(6))。在此过程中,几个小分子载脂蛋白III(apoLp-III)分子被添加到原本存在于HDLp-A中的两个分子上。利用分析超速离心机和凝胶过滤对促脂动激素诱导二酰甘油加载到HDLp-A上的时间进程进行研究,结果表明在HDLp-A和LDLp之间形成了一种密度介于两者之间的脂蛋白,且该脂蛋白是短暂存在的。对加载过程中通过密度梯度超速离心分离的脂蛋白进行分析表明,apoLp-III的添加速度比二酰甘油快,并且随着更多二酰甘油的添加,其在表面会改变构象。结合已知的apoLp-III的特性(一种轴比为3的长椭球体),我们认为最初apoLp-III以其短轴平行于表面的方式添加到脂蛋白扩展的疏水表面,随后apoLp-III展开以覆盖更大面积的疏水表面。用标记的apoLp-III进行的交换实验表明,HDLp-A中的两个apoLp-III分子不会与游离的apoLp-III交换,即使脂蛋白经历了加载和卸载循环,这表明apoLp-III在HDLp-A中具有结构作用。

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