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Membrane transporters for the special amino acid glutamine: structure/function relationships and relevance to human health

机译:特殊氨基酸谷氨酰胺的膜转运蛋白:结构/功能关系及其与人体健康的关系

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Glutamine together with glucose is essential for body’s homeostasis. It is the most abundant amino acid and is involved in many biosynthetic, regulatory and energy production processes. Several membrane transporters which differ in transport modes, ensure glutamine homeostasis by coordinating its absorption, reabsorption and delivery to tissues. These transporters belong to different protein families, are redundant and ubiquitous. Their classification, originally based on functional properties, has recently been associated with the SLC nomenclature. Function of glutamine transporters is studied in cells over-expressing the transporters or, more recently in proteoliposomes harboring the proteins extracted from animal tissues or over-expressed in microorganisms. The role of the glutamine transporters is linked to their transport modes and coupling with Na+ and H+. Most transporters share specificity for other neutral or cationic amino acids. Na+-dependent co-transporters efficiently accumulate glutamine while antiporters regulate the pools of glutamine and other amino acids. The most acknowledged glutamine transporters belong to the SLC1, 6, 7 and 38 families. The members involved in the homeostasis are the co-transporters B0AT1 and the SNAT members 1, 2, 3, 5 and 7; the antiporters ASCT2, LAT1 and 2. The last two are associated to the ancillary CD98 protein. Some information on regulation of the glutamine transporters exist, which, however, need to be deepened. No information at all is available on structures, besides some homology models obtained using similar bacterial transporters as templates. Some models of rat and human glutamine transporters highlight very similar structures between the orthologues. Moreover the presence of glycosylation and/or phosphorylation sites located at the extracellular or intracellular faces has been predicted. ASCT2 and LAT1 are over-expressed in several cancers, thus representing potential targets for pharmacological intervention.
机译:谷氨酰胺与葡萄糖一起对于人体的体内平衡至关重要。它是最丰富的氨基酸,参与许多生物合成,调节和能量生产过程。几种转运方式不同的膜转运蛋白可通过协调其吸收,再吸收和向组织的传递来确保谷氨酰胺体内稳态。这些转运蛋白属于不同的蛋白质家族,是多余的并且无处不在。它们的分类最初基于功能属性,最近已与SLC术语相关联。谷氨酰胺转运蛋白的功能在过表达转运蛋白的细胞中进行了研究,最近在含有从动物组织中提取的蛋白质或在微生物中过表达的蛋白脂质体中进行了研究。谷氨酰胺转运蛋白的作用与其转运模式有关,并与Na +和H +偶联。大多数转运蛋白对其他中性或阳离子氨基酸具有特异性。 Na +依赖性共转运蛋白有效地积累谷氨酰胺,而反转运蛋白调节谷氨酰胺和其他氨基酸的库。最知名的谷氨酰胺转运蛋白属于SLC1、6、7和38家族。参与体内平衡的成员是共同转运蛋白B0AT1和SNAT成员1,2,3,5和7;反转运蛋白ASCT2,LAT1和2。最后两个与辅助CD98蛋白相关。存在一些有关谷氨酰胺转运蛋白调节的信息,但是,需要深化。除了使用相似的细菌转运蛋白作为模板获得的某些同源性模型之外,关于结构的信息完全不可用。大鼠和人谷氨酰胺转运蛋白的某些模型突出了直向同源物之间非常相似的结构。此外,已经预测了位于细胞外或细胞内面的糖基化和/或磷酸化位点的存在。 ASCT2和LAT1在几种癌症中过表达,因此代表了药物干预的潜在靶标。

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