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牛视网膜色素上皮中的主动离子转运途径。

Active ion transport pathways in the bovine retinal pigment epithelium.

作者信息

Miller S S, Edelman J L

机构信息

University of California, School of Optometry, Berkeley 94720.

出版信息

J Physiol. 1990 May;424:283-300. doi: 10.1113/jphysiol.1990.sp018067.

Abstract
  1. Radioactive tracer flux measurements demonstrate that active ion transport across the isolated bovine retinal pigment epithelium (RPE)-choroid preparation can be maintained for hours after the eye is enucleated and the tissue removed from the eye. 2. It has been shown that 86Rb tracer fluxes can be used to monitor potassium (K+) transport across bull-frog RPE. In bovine RPE, net 86Rb (K+) absorption is zero. Apical barium (Ba2+) elevated active K+ absorption from zero to approximately 0.3 mu equiv cm-2 h-1. This Ba2(+)-induced increase in active K+ absorption was inhibited either by ouabain or bumetanide in the apical bath. 3. In control Ringer solution, buffered with bicarbonate and CO2, the RPE-choroid actively absorbs chloride (Cl-) at a rate of approximately 0.5 mu equiv cm-2 h-1. In contrast, sodium (Na+) is secreted at a rate of approximately 0.5 mu equiv cm-2 h-1. Chloride absorption was inhibited by apical bumetanide, and Na+ secretion was inhibited by apical ouabain. These drugs were only effective when placed in the solution bathing the apical or retinal side of the tissue. 4. Net Cl- absorption requires an exit mechanism at the basolateral membrane. DIDS (4,4'-diisothiocyanostilbene-2,2'-disulphonic acid) in the basal bath completely inhibited net Cl- absorption in bicarbonate-free Ringer solution. 5. These experiments show that the chloride transport pathway contains at least two components: (1) a bumetanide-sensitive uptake mechanism at the apical membrane; and (2) an efflux mechanism at the basolateral membrane that is blocked by DIDS. 6. Three apical membrane mechanisms were identified that could help modulate [K+]o in the subretinal or extracellular space that separates the distal retina and the RPE apical membrane. They are: (1) an ouabain-sensitive Na(+)-K+ pump; (2) a bumetanide-sensitive mechanism, the putative Na(+)-K(+)-Cl- co-transporter; (3) a barium-sensitive K+ channel that recycles, to the apical bath, most or all of the potassium that is actively taken up by the Na(+)-K+ pump and the co-transporter. 7. These data suggest that light-induced alterations in subretinal potassium that occur in vivo can activate the chloride transport pathway and help modulate RPE intracellular Cl- during transitions between the light and dark.
摘要
  1. 放射性示踪剂通量测量表明,在眼球摘除且组织从眼中取出后数小时内,分离的牛视网膜色素上皮(RPE)-脉络膜制剂上的主动离子转运仍可维持。2. 已表明86Rb示踪剂通量可用于监测牛蛙RPE上的钾(K+)转运。在牛RPE中,86Rb(K+)的净吸收为零。顶端加入钡(Ba2+)可使主动K+吸收从零增加到约0.3微当量·厘米-2·小时-1。顶端浴中加入哇巴因或布美他尼可抑制这种由Ba2+诱导的主动K+吸收增加。3. 在用碳酸氢盐和CO2缓冲的对照林格溶液中,RPE-脉络膜以约0.5微当量·厘米-2·小时-1的速率主动吸收氯离子(Cl-)。相比之下,钠离子(Na+)以约0.5微当量·厘米-2·小时-1的速率分泌。顶端加入布美他尼可抑制Cl-吸收,顶端加入哇巴因可抑制Na+分泌。这些药物仅在置于组织顶端或视网膜侧的浴液中时才有效。4. Cl-的净吸收需要基底外侧膜上有一个排出机制。基底浴中加入4,4'-二异硫氰基芪-2,2'-二磺酸(DIDS)可完全抑制无碳酸氢盐林格溶液中的Cl-净吸收。5. 这些实验表明,氯离子转运途径至少包含两个成分:(1)顶端膜上对布美他尼敏感的摄取机制;(2)基底外侧膜上被DIDS阻断的流出机制。6. 确定了三种顶端膜机制,它们有助于调节视网膜下或细胞外空间(分隔远端视网膜和RPE顶端膜)中的[K+]o。它们是:(1)对哇巴因敏感的Na+-K+泵;(2)对布美他尼敏感的机制,即假定的Na+-K+-Cl-共转运体;(3)对钡敏感的K+通道,它将大部分或全部由Na+-K+泵和共转运体主动摄取的钾循环回顶端浴中。7. 这些数据表明,体内发生的光诱导视网膜下钾的变化可激活氯离子转运途径,并在明暗转换期间有助于调节RPE细胞内的Cl-。

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