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肾脏氨基酸转运:从清除率研究到蛙卵的细胞与分子事件

Renal amino acid transport: cellular and molecular events from clearance studies to frog eggs.

作者信息

Chesney R W, Jones D, Zelikovic I

机构信息

Department of Pediatrics, University of Tennessee, Memphis College of Medicine.

出版信息

Pediatr Nephrol. 1993 Oct;7(5):574-84. doi: 10.1007/BF00852553.

Abstract

This article reviews recent advances in the mechanisms of renal amino acid transport. Renal amino acid transport is necessary to efficiently reclaim approximately 450 mmol amino acids from the glomerular ultrafiltrate each day in man. In general, individual amino acids are transported across the epithelial membrane of the proximal tubule by a sodium (Na+) dependent mechanism. This cotransport process utilizes the energy of the Na+ gradient to enter the cell. The amino acid then exits the basolateral surface and Na+ is pumped out by the Na(+)-K(+)-ATPase located in the basolateral membrane. In addition to the cellular accumulation of amino acids across the luminal membrane, these compounds may be taken up by the cell from the basolateral surface. Most amino acids are transported both individually and in a series of seven group specific processes. Human disorders of amino acid transport have been described for six of the seven transport systems. The process of ontogeny of amino acid accumulation by the proximal tubule is a complex one and will be further discussed in this review. A number of factors including pH, ion dependency, electrogenicity of transport process, as well as a variety of hormonal factors, may contribute to the regulation of amino acid transport. Gene expression of several amino acid transporters has been successfully performed using the oocyte of the frog Xenopus laevis. Using this system, a number of transporters have been cloned. Such a strategy will permit the cloning of virtually all transporter molecules, and thus we can anticipate the elucidation of the structure of the transporters. However, for a comprehensive understanding of cytoskeletal interactions protein phosphorylation and phospholipid domains and their linkage to the primary structure of the transporter need to be studied. The future for research in this area is indeed a bright one.

摘要

本文综述了肾脏氨基酸转运机制的最新进展。在人类中,肾脏氨基酸转运对于每天从肾小球超滤液中有效回收约450 mmol氨基酸是必要的。一般来说,单个氨基酸通过钠(Na+)依赖性机制跨近端小管的上皮膜转运。这种共转运过程利用Na+梯度的能量进入细胞。然后氨基酸从基底外侧表面排出,Na+由位于基底外侧膜的Na(+)-K(+)-ATP酶泵出。除了氨基酸通过管腔膜在细胞内积累外,这些化合物也可能从基底外侧表面被细胞摄取。大多数氨基酸既可以单独转运,也可以通过一系列七个组特异性过程转运。已经描述了七个转运系统中的六个系统存在人类氨基酸转运障碍。近端小管积累氨基酸的个体发生过程是一个复杂的过程,将在本综述中进一步讨论。包括pH、离子依赖性、转运过程的电生性以及多种激素因素在内的许多因素可能有助于氨基酸转运的调节。使用非洲爪蟾的卵母细胞已经成功地进行了几种氨基酸转运体的基因表达。利用这个系统,已经克隆了许多转运体。这样的策略将允许几乎所有转运体分子的克隆,因此我们可以预期转运体结构的阐明。然而,为了全面理解细胞骨架相互作用、蛋白质磷酸化和磷脂结构域以及它们与转运体一级结构的联系,还需要进行研究。该领域的未来研究前景确实光明。

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