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锂和钾在人体红细胞中的协同转运。

Cotransport of lithium and potassium in human red cells.

作者信息

Canessa M, Bize I, Adragna N, Tosteson D

出版信息

J Gen Physiol. 1982 Jul;80(1):149-68. doi: 10.1085/jgp.80.1.149.

Abstract

This paper reports the presence of human red cells of an additional ouabain-insensitive transport pathway for lithium ions, the Li-K cotransport. Several kinds of observations support this conclusion. Cells loaded to contain only K, Na, or Li do not exhibit furosemide-sensitive efflux. Simultaneous presence of K and Li on the same side of the membrane mutually stimulates furosemide-sensitive Li and K fluxes from that side. Cells loaded with both Na and Li exhibit no furosemide-sensitive Li efflux. Thus, Li can apparently replace Na but not K on the outward Na-K cotransport system in human red cells. Furthermore, Lio, like Ko, inhibits outward Na-K cotransport. Additional proof for coupled Li-K cotransport is provided by the observation that an outwardly directed K electrochemical potential gradient can drive net outwardly directed K electrochemical potential gradient can drive net outward Li movement against its gradient. There are several differences between Li-K cotransport and Li-Na countertransport. The cotransport system has an apparent affinity for Li that is about one-half that for Na and 30 times lower than the counter-transport system. Furosemide and chloride replacement inhibit cotransport but do not affect countertransport. The PCMBS loading procedure irreversibly inhibits countertransport but not cotransport. Furthermore, the two systems can apparently function at maximal rates simultaneously. Present evidence, than, indicates that the two pathways can be separated operationally as two different systems.

摘要

本文报道了人类红细胞中存在一种额外的对哇巴因不敏感的锂离子转运途径,即锂 - 钾协同转运。有几种观察结果支持这一结论。装载后仅含有钾、钠或锂的细胞不表现出对速尿敏感的外流。膜同一侧同时存在钾和锂会相互刺激该侧对速尿敏感的锂和钾通量。同时装载钠和锂的细胞不表现出对速尿敏感的锂外流。因此,在人类红细胞的外向钠 - 钾协同转运系统中,锂显然可以取代钠,但不能取代钾。此外,锂离子与钾离子一样,会抑制外向钠 - 钾协同转运。观察到外向的钾电化学势梯度可以驱动净外向的锂移动,使其逆着自身梯度移动,这为锂 - 钾协同转运提供了额外的证据。锂 - 钾协同转运和锂 - 钠逆向转运之间存在几个差异。协同转运系统对锂的表观亲和力约为对钠的一半,比对逆向转运系统低30倍。速尿和氯离子替代会抑制协同转运,但不影响逆向转运。对氯汞苯甲酸(PCMBS)装载程序会不可逆地抑制逆向转运,但不影响协同转运。此外,这两个系统显然可以同时以最大速率发挥作用。因此,目前的证据表明,这两种途径在操作上可以作为两个不同的系统分开。

相似文献

6
Lithium transport pathways in human red blood cells.人类红细胞中的锂转运途径。
J Gen Physiol. 1978 Aug;72(2):233-47. doi: 10.1085/jgp.72.2.233.

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