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哺乳动物谷氨酰胺转运的近期分子研究进展。

Recent molecular advances in mammalian glutamine transport.

作者信息

Bode B P

机构信息

Department of Biology, Saint Louis University, St. Louis, MO 63103-2010, USA.

出版信息

J Nutr. 2001 Sep;131(9 Suppl):2475S-85S; discussion 2486S-7S. doi: 10.1093/jn/131.9.2475S.

Abstract

Much has been learned about plasma membrane glutamine transporter activities in health and disease over the past 30 years, including their potential regulatory role in metabolism. Since the 1960s, discrimination among individual glutamine transporters was based on functional characteristics such as substrate specificity, ion dependence, and kinetic and regulatory properties. Within the past two years, several genes encoding for proteins with these defined activities (termed "systems") have been isolated from human and rodent cDNA libraries and found to be distributed among four distinct gene families. The Na(+)-dependent glutamine transporter genes isolated thus far are System N (SN1), System A (ATA1, ATA2), System ASC/B(0) (ASCT2 or ATB(0)), System B(0,+) (ATB(0,+)) and System y(+)L (y(+)LAT1, y(+)LAT2). Na(+)-independent glutamine transporter genes encoding for System L (LAT1, LAT2) and System b(0,+) (b(0,+)AT) have also been recently isolated, and similar to y(+)L, have been shown to function as disulfide-linked heterodimers with the 4F2 heavy chain (CD98) or rBAT (related to b(0,+) amino acid transporter). In this review, the molecular features, catalytic mechanisms and tissue distributions of each are addressed. Although most of these transporters mediate the transmembrane movement of several other amino acids, their potential roles in regulating interorgan glutamine flux are discussed. Most importantly, these newly isolated transporter genes provide the long awaited tools necessary to study their molecular regulation during the catabolic states in which glutamine is considered to be "conditionally essential."

摘要

在过去30年里,我们对健康和疾病状态下质膜谷氨酰胺转运体的活性有了很多了解,包括它们在代谢中的潜在调节作用。自20世纪60年代以来,对单个谷氨酰胺转运体的区分是基于功能特性,如底物特异性、离子依赖性以及动力学和调节特性。在过去两年中,几个编码具有这些特定活性(称为“系统”)蛋白质的基因已从人和啮齿动物的cDNA文库中分离出来,并发现它们分布在四个不同的基因家族中。迄今为止分离出的钠依赖性谷氨酰胺转运体基因有系统N(SN1)、系统A(ATA1、ATA2)、系统ASC/B(0)(ASCT2或ATB(0))、系统B(0,+)(ATB(0,+))和系统y(+)L(y(+)LAT1、y(+)LAT2)。编码系统L(LAT1、LAT2)和系统b(0,+)(b(0,+)AT)的钠非依赖性谷氨酰胺转运体基因最近也已分离出来,并且与y(+)L类似,已被证明与4F2重链(CD98)或rBAT(与b(0,+)氨基酸转运体相关)形成二硫键连接的异二聚体发挥功能。在这篇综述中,将阐述每种转运体的分子特征、催化机制和组织分布。尽管这些转运体中的大多数介导几种其他氨基酸的跨膜转运,但也将讨论它们在调节器官间谷氨酰胺通量方面的潜在作用。最重要的是,这些新分离的转运体基因提供了长期以来所期待的工具,用于研究在谷氨酰胺被认为是“条件必需”的分解代谢状态下它们的分子调节。

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