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抑制与脂肪酸结合蛋白的结合会减少脂肪酸的细胞内转运。

Inhibition of binding to fatty acid binding protein reduces the intracellular transport of fatty acids.

作者信息

Luxon B A

机构信息

Division of Gastroenterology and Hepatology, St. Louis University Health Sciences Center, Missouri 63110-0250, USA.

出版信息

Am J Physiol. 1996 Jul;271(1 Pt 1):G113-20. doi: 10.1152/ajpgi.1996.271.1.G113.

DOI:10.1152/ajpgi.1996.271.1.G113
PMID:8760114
Abstract

Male livers, containing lesser amounts of fatty acid binding protein (FABP), utilize fatty acids more slowly than female livers. Conventional wisdom dictates that FABP stimulates fatty acid use by increasing cytoplasmic transport rates. Previously, we showed that the cytoplasmic diffusion of a fatty acid analogue [12-N-methyl-7-nitrobenzo-2-oxa-1,3-diazol-amino stearate (NBD-stearate)] is faster in female hepatocytes, paralleling the larger amounts of FABP. Sex differences in other cytoplasmic factors could also lead to faster diffusion, independent of FABP levels. The aim of this study was to determine the effect of inhibition of fatty acid binding to FABP on the directly measured intracellular transport rate of NBD-stearate. The binding of NBD-stearate to FABP was reduced by incubating hepatocytes isolated from male and female rats with alpha-bromo-palmitate (0-1,500 microM), a modified long-chain fatty acid that binds to FABP. The inhibition by alpha-bromo-palmitate on NBD-stearate binding to FABP was measured with the use of centrifugation to separate cytosol from cytoplasmic membranes. Laser photobleaching (fluorescence recovery after photobleaching) was used to measure the cytoplasmic diffusion of NBD-stearate in hepatocytes. Alpha-Bromo-palmitate incubation reduced NBD-stearate binding to FABP in a dose-dependent manner. The measured diffusion rate was also reduced in proportion to the degree of binding inhibition. We conclude that cytoplasmic transport of NBD-stearate is modulated by binding to soluble proteins like FABP. FABP enhances diffusive transport by reducing binding to immobile cytosolic membranes.

摘要

雄性肝脏中脂肪酸结合蛋白(FABP)含量较少,其利用脂肪酸的速度比雌性肝脏慢。传统观点认为,FABP通过提高细胞质转运速率来刺激脂肪酸的利用。此前,我们发现脂肪酸类似物[12-N-甲基-7-硝基苯并-2-恶唑-1,3-二氮杂环庚烷-氨基硬脂酸酯(NBD-硬脂酸酯)]在雌性肝细胞中的细胞质扩散速度更快,这与FABP含量较高相一致。其他细胞质因子的性别差异也可能导致扩散速度加快,而与FABP水平无关。本研究的目的是确定抑制脂肪酸与FABP结合对直接测量的NBD-硬脂酸酯细胞内转运速率的影响。通过用α-溴棕榈酸酯(0-1500 microM)孵育从雄性和雌性大鼠分离的肝细胞,α-溴棕榈酸酯是一种与FABP结合的修饰长链脂肪酸,从而降低NBD-硬脂酸酯与FABP的结合。使用离心法将细胞质膜与细胞质分离,测量α-溴棕榈酸酯对NBD-硬脂酸酯与FABP结合的抑制作用。使用激光漂白法(光漂白后荧光恢复)测量NBD-硬脂酸酯在肝细胞中的细胞质扩散。α-溴棕榈酸酯孵育以剂量依赖方式降低NBD-硬脂酸酯与FABP的结合。测得的扩散速率也与结合抑制程度成比例降低。我们得出结论,NBD-硬脂酸酯的细胞质转运通过与FABP等可溶性蛋白结合来调节。FABP通过减少与固定细胞质膜的结合来增强扩散转运。

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