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肝细胞单层对棕榈酸盐的摄取。白蛋白结合的影响。

Palmitate uptake by hepatocyte monolayers. Effect of albumin binding.

作者信息

Fleischer A B, Shurmantine W O, Luxon B A, Forker E L

出版信息

J Clin Invest. 1986 Mar;77(3):964-70. doi: 10.1172/JCI112397.

Abstract

The uptake of 14C-palmitate by rat liver cell monolayers is depressed by binding of the fatty acid to albumin. When the uptake flux is divided by the concentration of free palmitate in the bathing medium, however, the resulting clearance is approximately 14 times greater in the presence of albumin than in its absence. These findings are not accounted for by the different diffusion rates of free and bound palmitate across an unstirred fluid layer, nor attributable to nonequilibrium binding. Instead we argue that the most plausible explanation is accelerated dissociation of albumin-palmitate complexes mediated by the cell surface--an interpretation that also explains the uptake kinetics of other albumin-bound organic anions by perfused rat liver.

摘要

脂肪酸与白蛋白结合会抑制大鼠肝细胞单层对14C-棕榈酸的摄取。然而,当摄取通量除以浴液中游离棕榈酸的浓度时,在有白蛋白存在的情况下,所得清除率比无白蛋白时大约高14倍。这些发现不能用游离和结合的棕榈酸在未搅拌液层中的不同扩散速率来解释,也不能归因于非平衡结合。相反,我们认为最合理的解释是细胞表面介导的白蛋白-棕榈酸复合物的加速解离——这一解释也说明了灌注大鼠肝脏对其他与白蛋白结合的有机阴离子的摄取动力学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eaa9/423493/813822c48901/jcinvest00106-0322-a.jpg

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