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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Differential effects of conjugated linoleic acid isomers on the biophysical and biochemical properties of model membranes.
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Differential effects of conjugated linoleic acid isomers on the biophysical and biochemical properties of model membranes.

机译:共轭亚油酸异构体对模型膜的生物物理和生化特性的差异作用。

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Conjugated linoleic acids (CLA) are known to exert several isomer-specific biological effects, but their mechanisms of action are unclear. In order to determine whether the physicochemical effects of CLA on membranes play a role in their isomer-specific effects, we synthesized phosphatidylcholines (PCs) with 16:0 at sn-1 position and one of four CLA isomers (trans 10 cis 12 (A), trans 9 trans 11 (B), cis 9 trans 11 (C), and cis 9 cis 11 (D)) at sn-2, and determined their biophysical properties in monolayers and bilayers. The surface areas of the PCs with the two natural CLA (A and C) were similar at all pressures, but they differed significantly in the presence of cholesterol, with PC-A condensing more than PC-C. Liposomes of PC-A similarly showed increased binding of cholesterol compared to PC-C liposomes. PC-A liposomes were less permeable to carboxyfluorescein compared to PC-C liposomes. The PC with two trans double bonds (B) showed the highest affinity to cholesterol and lowest permeability. The two natural CLA-PCs (A and C) stimulated lecithin-cholesterol acyltransferase activity by 2-fold, whereas the unnatural CLA-PCs (B and D) were inhibitory. These results suggest that the differences in the biophysical properties of CLA isomers A and C may partly contribute to the known differences in their biological effects.
机译:已知共轭亚油酸(CLA)会发挥多种异构体特异性生物学效应,但其作用机理尚不清楚。为了确定CLA对膜的理化作用是否在其异构体特异性作用中起作用,我们合成了在sn-1位置具有16:0的磷脂酰胆碱(PCs)和四种CLA异构体之一(反式10顺12(A ),sn-2上的反式9反式11(B),顺式9反式11(C)和顺式9顺式11(D)),并确定了它们在单层和双层中的生物物理特性。具有两种天然CLA(A和C)的PC的表面积在所有压力下都相似,但是在存在胆固醇的情况下,它们的表面积存在显着差异,其中PC-A的冷凝量大于PC-C。与PC-C脂质体相比,PC-A脂质体同样显示出增加的胆固醇结合。与PC-C脂质体相比,PC-A脂质体对羧基荧光素的渗透性较低。具有两个反式双键(B)的PC对胆固醇的亲和力最高,通透性最低。两种天然CLA-PC(A和C)将卵磷脂胆固醇酰基转移酶活性提高了2倍,而非天然CLA-PC(B和D)具有抑制作用。这些结果表明,CLA异构体A和C的生物物理性质的差异可能部分地导致了其生物学效应的已知差异。

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