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游离脂肪酸对体内α-酮异己酸与白蛋白结合的调节作用。

Regulation of alpha-ketoisocaproate binding to albumin in vivo by free fatty acids.

作者信息

Nissen S L, Miles J M, Gerich J E, Haymond M W

出版信息

Am J Physiol. 1982 Jan;242(1):E67-71. doi: 10.1152/ajpendo.1982.242.1.E67.

Abstract

The importance of alpha-keto acid binding to plasma proteins was investigated both in vitro and in vivo using alpha-ketoisocaproate (KIC), the alpha-keto acid of leucine. Gel chromatography indicated that 65% of the radioactivity comigrated with serum albumin. An ultrafiltration assay was developed to estimate the percentage of free and bound KIC. These percentages, along with total plasma KIC concentrations, were used to calculate the circulating concentrations of free and bound KIC. KIC or free fatty acids (FFA) displaced [14C]KIC bound to bovine albumin or whole plasma. KIC was totally displaced from plasma proteins by 10 mM oleate, stearate, and myristate; whereas the alpha-keto acids of isoleucine and value were 50 and 85%, respectively, as effective as KIC. To determine whether increased plasma FFA concentrations alter the binding of KIC to plasma proteins in vivo, five postabsorptive humans were infused with triglyceride and heparin during the simultaneous administration of somatostatin, glucagon, and insulin. During the FFA elevation, plasma leucine decreased by 9% (P less than 0.02). Total plasma KIC remained constant, whereas free KIC increased (P less than 0.02) and bound KIC decreased (P less than 0.001). These results indicate that KIC is bound to plasma albumin in vivo and suggests that FFA, by altering circulating free KIC concentrations, may influence protein metabolism in man.

摘要

利用亮氨酸的α-酮酸α-酮异己酸(KIC),在体外和体内研究了α-酮酸与血浆蛋白结合的重要性。凝胶色谱法表明,65%的放射性与血清白蛋白一起迁移。开发了一种超滤测定法来估计游离和结合KIC的百分比。这些百分比以及血浆总KIC浓度用于计算游离和结合KIC的循环浓度。KIC或游离脂肪酸(FFA)取代了与牛白蛋白或全血浆结合的[14C]KIC。10 mM的油酸、硬脂酸和肉豆蔻酸可使KIC完全从血浆蛋白中置换出来;而异亮氨酸和缬氨酸的α-酮酸的置换效果分别为KIC的50%和85%。为了确定血浆FFA浓度升高是否会在体内改变KIC与血浆蛋白的结合,在同时给予生长抑素、胰高血糖素和胰岛素的过程中,对五名吸收后状态的人输注甘油三酯和肝素。在FFA升高期间,血浆亮氨酸下降了9%(P<0.02)。血浆总KIC保持不变,而游离KIC增加(P<0.02),结合KIC减少(P<0.001)。这些结果表明,KIC在体内与血浆白蛋白结合,并提示FFA通过改变循环中游离KIC的浓度,可能会影响人体的蛋白质代谢。

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