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受膳食磷酸盐调节的兔肾钠-磷共转运体的克隆

Cloning of a rabbit renal Na-Pi cotransporter, which is regulated by dietary phosphate.

作者信息

Verri T, Markovich D, Perego C, Norbis F, Stange G, Sorribas V, Biber J, Murer H

机构信息

Institute of Physiology, University of Zürich, Switzerland.

出版信息

Am J Physiol. 1995 Apr;268(4 Pt 2):F626-33. doi: 10.1152/ajprenal.1995.268.4.F626.

Abstract

Previously, we isolated a cDNA (NaPi-1) related to a rabbit renal proximal tubular Na-Pi cotransporter (A. Werner, M.L. Moore, N. Mantei, J. Biber, G. Semenza, and H. Murer. Proc. Natl. Acad. Sci. USA 88:9608-9612, 1991.). In this study, we isolated an additional (rabbit renal) cDNA (NaPi-6), which induces Na-dependent Pi uptake in Xenopus laevis oocytes. Substrate specificity and kinetic properties corresponded to those known for rabbit renal brush-border membrane (BBM) Na-Pi cotransport. NaPi-6 was cloned by homology using NaPi-2 cDNA, a rat renal BBM Na-Pi cotransporter (S. Magagnin, A. Werner, D. Markovich, V. Sorribas, G. Stange, J. Biber, and H. Murer. Proc. Natl. Acad. Sci. USA 90: 5979-5983, 1993). NaPi-6 encodes a protein of 642 amino acids, exhibiting at least eight transmembrane domains. NaPi-6 mRNA and protein in kidneys of rabbits fed a low-Pi diet (LPD; 0.11% Pi) for 1 wk were increased by 1.5- and 4-fold, respectively, compared with those of rabbits fed a high-Pi diet (HPD; 1.20% Pi). This effect was correlated with an increase in Na-Pi cotransport of BBM vesicles isolated from animals adapted to LPD (2.5-fold with respect to HPD). In contrast, NaPi-1 mRNA and protein were not altered in response to LPD. Thus rabbit proximal tubular BBMs contain two different Na-Pi cotransport systems: NaPi-1 (type I) and NaPi-6 (type II). Only the type II transport system seems to be under regulatory control in response to low-Pi dietary intake.

摘要

此前,我们分离出了一种与兔肾近端小管钠-磷共转运体相关的cDNA(NaPi-1)(A. 维尔纳、M.L. 摩尔、N. 曼泰、J. 比伯、G. 塞门扎和H. 穆勒。《美国国家科学院院刊》88:9608 - 9612,1991年)。在本研究中,我们又分离出了一个(兔肾)cDNA(NaPi-6),它能在非洲爪蟾卵母细胞中诱导钠依赖性磷摄取。底物特异性和动力学特性与兔肾刷状缘膜(BBM)钠-磷共转运已知的特性相符。利用大鼠肾BBM钠-磷共转运体NaPi-2 cDNA(S. 马加宁、A. 维尔纳、D. 马尔科维奇、V. 索里巴斯、G. 施坦格、J. 比伯和H. 穆勒。《美国国家科学院院刊》90:5979 - 5983,1993年)通过同源性克隆出了NaPi-6。NaPi-6编码一种含642个氨基酸的蛋白质,具有至少八个跨膜结构域。与喂食高磷饮食(HPD;1.20%磷)的兔子相比,喂食低磷饮食(LPD;0.11%磷)1周的兔子肾脏中的NaPi-6 mRNA和蛋白质分别增加了1.5倍和4倍。这种效应与从适应LPD的动物中分离出的BBM囊泡的钠-磷共转运增加相关(相对于HPD增加了2.5倍)。相比之下,NaPi-1 mRNA和蛋白质对LPD没有反应。因此,兔近端小管BBM含有两种不同的钠-磷共转运系统:NaPi-1(I型)和NaPi-6(II型)。似乎只有II型转运系统在低磷饮食摄入时受到调节控制。

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