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从大鼠肾内髓质分离的集合管细胞中的胆碱转运

Choline transport in collecting duct cells isolated from the rat renal inner medulla.

作者信息

Bevan C, Kinne R K

机构信息

Max-Planck-Institut für Systemphysiologie, Dortmund, Federal Republic of Germany.

出版信息

Pflugers Arch. 1990 Nov;417(3):324-8. doi: 10.1007/BF00370999.

Abstract

Glycerophosphorylcholine (GPC) plays an important role in the osmoregulation of the renal inner medulla. Under hyperosmotic conditions, a striking increase in cellular GPC content is observed. In order to characterize the cellular events involved in GPC metabolism, we have studied the uptake of choline, a precursor of GPC, by freshly isolated rat inner medullary collecting duct (IMCD) cells at 300 mosmol/l. Choline uptake occurred by a single transport system with an apparent affinity (Km) of 80 microM and a maximal velocity (Vmax) of 120 pmol/microliter cell water/min. Hemicholinium-3, ethanolamine and N,N-dimethylethanolamine were potent inhibitors, but betaine had no effect. Choline uptake was not altered by the replacement of Na+ with N-methylglucamine+, suggesting a sodium-independent process. Addition of 50 mM KCl to the incubation medium to reduce the cell membrane potential inhibited choline uptake by 19 +/- 4% after 10 min. Increasing the extracellular osmolarity to 600 or 900 mosmol/l had no effect on the kinetic parameters of choline uptake. These results suggest that choline uptake into IMCD cells occurs by a sodium-independent transport system driven by the inside negative cell membrane potential. Furthermore, the increase in the GPC content under hyperosmotic conditions is not associated with increased activity of the transport systems of biosynthetic precursors.

摘要

甘油磷酸胆碱(GPC)在肾内髓质的渗透调节中起重要作用。在高渗条件下,可观察到细胞内GPC含量显著增加。为了描述参与GPC代谢的细胞事件,我们研究了在300 mosmol/l时,新鲜分离的大鼠内髓集合管(IMCD)细胞对GPC前体胆碱的摄取。胆碱摄取通过单一转运系统进行,其表观亲和力(Km)为80 microM,最大速度(Vmax)为120 pmol/微升细胞水/分钟。半胱氨酸-3、乙醇胺和N,N-二甲基乙醇胺是有效的抑制剂,但甜菜碱没有作用。用N-甲基葡糖胺+替代Na+不会改变胆碱摄取,表明这是一个不依赖钠的过程。在孵育培养基中加入50 mM KCl以降低细胞膜电位,10分钟后胆碱摄取受到19±4%的抑制。将细胞外渗透压提高到600或900 mosmol/l对胆碱摄取的动力学参数没有影响。这些结果表明胆碱进入IMCD细胞是通过一个不依赖钠的转运系统进行的,该系统由细胞膜内侧的负电位驱动。此外,高渗条件下GPC含量的增加与生物合成前体转运系统活性的增加无关。

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