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The binding of cholesterol and bile salts to recombinant rat liver fatty acid-binding protein.

机译:胆固醇和胆汁盐与重组大鼠肝脏脂肪酸结合蛋白的结合。

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摘要

The physiological role of liver fatty acid-binding protein (L-FABP) has yet to be clarified. An important feature of this member of the family of intracellular lipid-binding proteins is the wide range of compounds that have been identified as potential physiological ligands. By using recombinant L-FABP, the binding of cholesterol, bile salts and their derivatives has been investigated under conditions that allow a direct comparison of the binding affinities of these ligands for fatty acids. The results demonstrate an inability of L-FABP to bind cholesterol, although the anionic derivative, cholesteryl sulphate, will bind under similar assay conditions. Of the bile salts examined, lithocholate and taurolithocholate sulphate showed the greatest binding to L-FABP. It is proposed that an important function of L-FABP is to bind certain physiological amphipathic anions, thus preventing the "free' concentrations of these compounds from exceeding their critical micelle concentration, which could result in cell damage.
机译:肝脏脂肪酸结合蛋白(L-FABP)的生理作用尚未阐明。该细胞内脂质结合蛋白家族成员的重要特征是已被鉴定为潜在生理配体的多种化合物。通过使用重组L-FABP,已经在允许直接比较这些配体对脂肪酸的结合亲和力的条件下研究了胆固醇,胆汁盐及其衍生物的结合。结果表明,L-FABP无法结合胆固醇,尽管阴离子衍生物胆固醇胆固醇硫酸盐将在相似的测定条件下结合。在所检查的胆盐中,石胆酸盐和牛磺石胆酸盐硫酸盐显示出与L-FABP的最大结合。提出L-FABP的重要功能是结合某些生理两亲性阴离子,从而防止这些化合物的“游离”浓度超过其临界胶束浓度,这可能导致细胞损伤。

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