首页> 外文期刊>American Journal of Physiology >The betaine-GABA transporter (BGT1, slc6a12) is predominantly expressed in the liver and at lower levels in the kidneys and at the brain surface
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The betaine-GABA transporter (BGT1, slc6a12) is predominantly expressed in the liver and at lower levels in the kidneys and at the brain surface

机译:甜菜碱-GABA转运蛋白(BGT1,slc6a12)主要在肝脏中表达,并在肾脏和脑表面较低水平表达

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摘要

The Na +- and Cl --dependent GABA-betaine transporter (BGT1) has received attention mostly as a protector against osmolarity changes in the kidney and as a potential controller of the neurotransmitter GABA in the brain. Nevertheless, the cellular distribution of BGT1, and its physiological importance, is not fully understood. Here we have quantified mRNA levels using TaqMan real-time PCR, produced a number of BGT1 antibodies, and used these to study BGT1 distribution in mice. BGT1 (protein and mRNA) is predominantly expressed in the liver (sinusoidal hepatocyte plasma membranes) and not in the endothelium. BGT1 is also present in the renal medulla, where it localizes to the basolateral membranes of collecting ducts (particularly at the papilla tip) and the thick ascending limbs of Henle. There is some BGT1 in the leptomeninges, but brain parenchyma, brain blood vessels, ependymal cells, the renal cortex, and the intestine are virtually BGT1 deficient in 1- to 3-mo-old mice. Labeling specificity was assured by processing tissue from BGT1-deficient littermates in parallel as negative controls. Addition of 2.5% sodium chloride to the drinking water for 48 h induced a two- to threefold upregulation of BGT1, tonicity-responsive enhancer binding protein, and sodiummyo- inositol cotransporter 1 (slc5a3) in the renal medulla, but not in the brain and barely in the liver. BGT1-deficient and wild-type mice appeared to tolerate the salt treatment equally well, possibly because betaine is one of several osmolytes. In conclusion, this study suggests that BGT1 plays its main role in the liver, thereby complementing other betaine-transporting carrier proteins (e.g., slc6a20) that are predominantly expressed in the small intestine or kidney rather than the liver.
机译:依赖Na +和Cl的GABA-甜菜碱转运蛋白(BGT1)在大多数情况下已引起人们的注意,它是防止肾脏渗透压变化的保护剂,也是大脑神经递质GABA的潜在控制者。但是,尚未完全了解BGT1的细胞分布及其生理重要性。在这里,我们使用TaqMan实时PCR定量了mRNA水平,产生了许多BGT1抗体,并用它们来研究BGT1在小鼠中的分布。 BGT1(蛋白质和mRNA)主要在肝脏(正弦肝细胞质膜)中表达,而不在内皮中表达。 BGT1也存在于肾髓质中,它位于收集管的基底外侧膜(特别是在乳头顶端)和Henle的较厚的上升肢体。在软脑膜中有一些BGT1,但是在1至3个月大的小鼠中,脑实质,脑血管,室管膜细胞,肾皮质和肠实际上缺乏BGT1。通过平行处理来自BGT1缺陷的同窝幼仔的组织作为阴性对照来确保标记特异性。在饮用水中添加2.5%氯化钠,持续48 h会导致肾脏髓质中BGT1,张力调节增强剂结合蛋白和肌醇钠共转运蛋白1(slc5a3)的表达上调两倍至三倍,但在大脑和大脑中却没有几乎不在肝脏中。缺乏BGT1的野生型小鼠似乎同样耐受盐处理,这可能是因为甜菜碱是几种渗透液之一。总之,这项研究表明BGT1在肝脏中起主要作用,从而补充了主要在小肠或肾脏而非肝脏中表达的其他甜菜碱运输载体蛋白(例如slc6a20)。

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