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大鼠、人类和兔钠-葡萄糖协同转运蛋白(SGLT-1)之间的动力学和特异性差异。

Kinetic and specificity differences between rat, human, and rabbit Na+-glucose cotransporters (SGLT-1).

作者信息

Hirayama B A, Lostao M P, Panayotova-Heiermann M, Loo D D, Turk E, Wright E M

机构信息

Department of Physiology, University of California School of Medicine, Los Angeles 90095-1751, USA.

出版信息

Am J Physiol. 1996 Jun;270(6 Pt 1):G919-26. doi: 10.1152/ajpgi.1996.270.6.G919.

Abstract

The Na+ activation and substrate specificity of human, rabbit, and rat Na+-glucose cotransporter (SGLT-1) isoforms were characterized using the Xenopus oocyte expression system and the two-electrode voltageclamp method. We find that there are differences, major and minor, in both the kinetics and substrate specificities between these isoforms; the substrate concentration at half-maximal current (K0.5) for hexoses varies from 0.2 to > 40 mM, depending on the species and sugar; the affinity constant (Ki) for phlorizin, the classic competitive inhibitor of SGLT-1, varies lover two orders of magnitude (rat Ki = 0.03 microM vs. rabbit Ki = 1.4 microM); and some glucoside inhibitors of the rabbit isoform, p-nitrophenyl glucose and beta-naphthyl glucose, are transported by the human and rat transporters. Na+ activation is more sensitive to membrane potential in the human and rat isoforms compared with rabbit. The rabbit isoform has a higher apparent affinity for alpha-methylglucose and 3-O-methylglucose by a factor of two than either human or rat. These results can be quantitatively fitted by our six-state kinetic model of SGLT-1, providing insight into the processes involved in these changes. For example, the model predicts that Na+ binding (rate constant, k12) in human and rat SGLT-1 is similar but is fourfold larger than in rabbit, whereas sugar binding (k23) in rabbit and rat is similar but double the value in human SGLT-1. The differences in the primary amino acid sequences between these three homologous proteins must account for the kinetic and substrate specificity differences, and comparisons of the functional properties and amino acid sequences of SGLT-1 isoforms provide useful information about structure/function relationships.

摘要

利用非洲爪蟾卵母细胞表达系统和双电极电压钳法,对人、兔和大鼠的钠 - 葡萄糖共转运体(SGLT - 1)亚型的钠离子激活作用和底物特异性进行了表征。我们发现,这些亚型在动力学和底物特异性方面均存在或大或小的差异;己糖的半数最大电流时的底物浓度(K0.5)因物种和糖类的不同而在0.2至>40 mM之间变化;SGLT - 1的经典竞争性抑制剂根皮苷的亲和常数(Ki)在两个数量级范围内变化(大鼠Ki = 0.03 μM,而兔Ki = 1.4 μM);兔亚型的一些葡萄糖苷抑制剂,对硝基苯基葡萄糖和β - 萘基葡萄糖,可被人和大鼠的转运体转运。与兔相比,人和大鼠亚型中的钠离子激活对膜电位更为敏感。兔亚型对α - 甲基葡萄糖和3 - O - 甲基葡萄糖的表观亲和力比人和大鼠高两倍。这些结果可以通过我们的SGLT - 1六态动力学模型进行定量拟合,从而深入了解这些变化所涉及的过程。例如,该模型预测,人和大鼠SGLT - 1中的钠离子结合(速率常数,k12)相似,但比兔中的大四倍,而兔和大鼠中的糖类结合(k23)相似,但在人SGLT - 1中的值是其两倍。这三种同源蛋白之间一级氨基酸序列的差异必定是造成动力学和底物特异性差异的原因,对SGLT - 1亚型的功能特性和氨基酸序列进行比较,可为结构/功能关系提供有用信息。

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