首页> 外文期刊>American Journal of Physiology >Na(+)-D-glucose cotransporter in the kidney of Squalus acanthias: molecular identification and intrarenal distribution.
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Na(+)-D-glucose cotransporter in the kidney of Squalus acanthias: molecular identification and intrarenal distribution.

机译:Na(+)-D-葡萄糖共转运蛋白在棘角棘鱼肾中:分子鉴定和肾内分布。

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摘要

Using primers against conserved regions of mammalian Na(+)-d-glucose cotransporters (SGLT), a cDNA was cloned from the kidney of spiny dogfish shark (Squalus acanthias). On the basis of comparison of amino acid sequence, membrane topology, and putative glycosylation and phosphorylation sites, the cDNA could be shown to belong to the family of sglt genes. Indeed, Na(+)-dependent d-glucose uptake could be demonstrated after expression of the gene in Xenopus laevis oocytes. In a dendrogram, the SGLT from shark kidney has a high homology to the mammalian SGLT2. Computer analysis revealed that the elasmobranch protein is most similar to the mammalian proteins in the transmembrane regions and contains already all the amino acids identified to be functionally important, suggesting early conservation during evolution. Extramembraneous loops show larger variations. This holds especially for loop 13, which has been implied as a phlorizin-binding domain. Antibodies were generated and the intrarenal distribution of the SGLT was studied in cryosections. In parallel, the nephron segments were identified by lectins. Positive immunoreactions were found in the proximal tubule in the early parts PIa and PIb and the late segment PIIb. The large PIIa segment of the proximal tubule showed no reaction. In contrast to the mammalian kidney also the late distal tubule, the collecting tubule, and the collecting duct showed immunoreactivity. The molecular information confirms previous vesicle studies in which a low affinity SGLT with a low stoichiometry has been observed and supports the notion of a similarity of the shark kidney SGLT to the mammalian SGLT2. Despite its presence in the late parts of the nephron, the absence of SGLT in the major part of the proximal tubule, the relatively low affinity, and in particular the low stoichiometry might explain the lack of a T(m) for d-glucose in the shark kidney.
机译:使用针对哺乳动物Na(+)-d-葡萄糖共转运蛋白(SGLT)保守区域的引物,从多刺狗鲨(Squalus acanthias)的肾脏中克隆了一个cDNA。通过比较氨基酸序列,膜拓扑结构以及假定的糖基化和磷酸化位点,可以证明该cDNA属于sglt基因家族。确实,在非洲爪蟾卵母细胞中表达该基因后,可以证明依赖Na(+)的d-葡萄糖摄取。在树状图中,来自鲨鱼肾的SGLT与哺乳动物SGLT2具有高度同源性。计算机分析表明,弹性分支蛋白与跨膜区的哺乳动物蛋白最相似,并且已经包含所有被鉴定为功能重要的氨基酸,表明在进化过程中的早期保存。膜外循环显示较大的变化。这尤其适用于环13,其被暗示为phlorizin结合域。产生了抗体,并在冰冻切片中研究了SGLT在肾脏内的分布。平行地,通过凝集素鉴定肾单位段。在早期部分PIa和PIb和晚期部分PIIb中的近端小管中发现了阳性免疫反应。近端小管的大PIIa节段未显示反应。与哺乳动物肾脏相反,远端末梢小管,收集小管和收集管也显示出免疫反应性。分子信息证实了先前的囊泡研究,其中已观察到具有低化学计量的低亲和力SGLT,并支持鲨鱼肾SGLT与哺乳动物SGLT2相似的观点。尽管它存在于肾的晚期,但在近端肾小管的主要部分不存在SGLT,亲和力相对较低,特别是化学计量比较低,这可能解释了d-葡萄糖缺乏T(m)的原因。鲨鱼肾。

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