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肝脏和肠道脂肪酸结合蛋白的功能与调节

Function and regulation of hepatic and intestinal fatty acid binding proteins.

作者信息

Bass N M

出版信息

Chem Phys Lipids. 1985 Aug 30;38(1-2):95-114. doi: 10.1016/0009-3084(85)90060-x.

Abstract

Two structurally different fatty acid binding proteins (FABP) have been isolated from rat liver and small intestinal epithelium. hFABP is a 14 184 Da protein found in abundance in both liver and small intestine, whereas gFABP (15 063 Da) is abundantly present only in small intestine. This review discusses studies which have provided insight into the physiological functions of these proteins. These include analyses of endogenous and exogenous ligand binding to FABP in vitro; examination of the modulating effect of FABP preparations on enzyme activities in vitro; exploration of relationships between alterations in cytosolic FABP content in response to hormonal, pharmacological, and dietary manipulations and changes in the rates of cellular fatty acid uptake and utilization; and studies of hFABP turnover and the mechanisms of FABP regulation. These experiments provide compelling evidence for a broad role of the FABPs in the transport, utilization and cellular economy of free fatty acids in the liver and small intestine, and also in protecting several aspects of cellular function against the modulatory effects of fatty acids, fatty acyl-CoA esters, and other ligands. Studies of FABP regulation also suggest a role in long-term rather than short-term modulation of hepatic fatty acid metabolism and indicate that hFABP and gFABP may perform different functions in the small intestine.

摘要

已从大鼠肝脏和小肠上皮中分离出两种结构不同的脂肪酸结合蛋白(FABP)。hFABP是一种分子量为14 184道尔顿的蛋白质,在肝脏和小肠中均大量存在,而gFABP(15 063道尔顿)仅在小肠中大量存在。本综述讨论了有助于深入了解这些蛋白质生理功能的研究。这些研究包括体外对内源性和外源性配体与FABP结合的分析;FABP制剂对体外酶活性调节作用的检测;探究激素、药物和饮食干预引起的细胞溶质FABP含量变化与细胞脂肪酸摄取和利用速率变化之间的关系;以及对hFABP周转和FABP调节机制的研究。这些实验提供了令人信服的证据,证明FABP在肝脏和小肠中游离脂肪酸的运输、利用和细胞代谢方面发挥着广泛作用,并且在保护细胞功能的多个方面免受脂肪酸、脂肪酰辅酶A酯和其他配体的调节作用方面也发挥着作用。对FABP调节的研究还表明其在肝脏脂肪酸代谢的长期而非短期调节中发挥作用,并表明hFABP和gFABP在小肠中可能发挥不同功能。

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