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肾刷状缘膜囊泡中的胆碱转运体:能量学与结构特异性

A choline transporter in renal brush-border membrane vesicles: energetics and structural specificity.

作者信息

Wright S H, Wunz T M, Wunz T P

机构信息

Department of Physiology, College of Medicine, University of Arizona, Tucson 85724.

出版信息

J Membr Biol. 1992 Feb;126(1):51-65. doi: 10.1007/BF00233460.

Abstract

Choline is a quaternary ammonium compound that is normally reabsorbed by the renal proximal tubule, despite its acknowledged role as a substrate for the renal organic cation (OC) secretory pathway. The basis for choline reabsorption was examined in studies of transport in rabbit renal brush-border membrane vesicles (BBMV). Although an outwardly directed H+ gradient (pH 6.0in: 7.5out) stimulated uptake of tetraethylammonium (TEA), a model substrate of the OC/H+ exchanger in renal BBMV, it had no effect on uptake of 1 microM choline. A 5 mM trans concentration gradient of choline did, however, drive countertransport of both TEA and choline, although trans TEA had no effect on choline accumulation in BBMV. A 20 mM concentration of unlabeled choline blocked uptake of both choline and TEA by greater than 85%, whereas 20 mM TEA blocked only TEA uptake. The kinetics of choline uptake into vesicles preloaded with 1 mM unlabeled choline appeared to involve two, saturable transport processes, one of high affinity for choline (Kt of 97 microM) and a second of low affinity (Kt of approximately 10 mM), the latter presumably reflecting a weak interaction of choline with the OC/H+ exchanger. An inside-negative electrical PD stimulated the rate of uptake and supported the transient concentrative accumulation of choline in BBMV. The high affinity transporter showed a marked specificity for choline and closely related analogues. A model of the molecular determinants of substrate-transporter interaction is described. We conclude that the electrogenic high affinity pathway plays a central role in renal reabsorption of choline.

摘要

胆碱是一种季铵化合物,尽管它被认为是肾脏有机阳离子(OC)分泌途径的底物,但通常会被肾近端小管重吸收。在对兔肾刷状缘膜囊泡(BBMV)转运的研究中,对胆碱重吸收的基础进行了研究。虽然外向的H⁺梯度(pH 6.0内:7.5外)刺激了四乙铵(TEA)的摄取,TEA是肾BBMV中OC/H⁺交换体的模型底物,但它对1微摩尔胆碱的摄取没有影响。然而,5毫摩尔的胆碱跨浓度梯度确实驱动了TEA和胆碱的反向转运,尽管反式TEA对BBMV中胆碱的积累没有影响。20毫摩尔未标记的胆碱浓度使胆碱和TEA的摄取受阻超过85%,而20毫摩尔TEA仅阻止TEA的摄取。将胆碱摄取到预先装载1毫摩尔未标记胆碱的囊泡中的动力学似乎涉及两个可饱和的转运过程,一个对胆碱具有高亲和力(Kt为97微摩尔),另一个具有低亲和力(Kt约为10毫摩尔),后者可能反映了胆碱与OC/H⁺交换体的弱相互作用。内向负电的膜电位差刺激了摄取速率,并支持了胆碱在BBMV中的瞬时浓缩积累。高亲和力转运体对胆碱和密切相关的类似物表现出明显的特异性。描述了底物-转运体相互作用的分子决定因素模型。我们得出结论,电生性高亲和力途径在肾脏胆碱重吸收中起核心作用。

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