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皮质类固醇激素对大鼠远端结肠电生理学的影响:对钠和钾转运的意义。

Effects of corticosteroid hormones on the electrophysiology of rat distal colon: implications for Na+ and K+ transport.

作者信息

Binder H J, McGlone F, Sandle G I

机构信息

Department of Medicine, Hope Hospital (University of Manchester School of Medicine), Salford.

出版信息

J Physiol. 1989 Mar;410:425-41. doi: 10.1113/jphysiol.1989.sp017542.

DOI:10.1113/jphysiol.1989.sp017542
PMID:2795485
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1190488/
Abstract
  1. Conventional microelectrodes, the Na+ channel blocker amiloride (0.1 mM), and the K+ channel blocker tetraethylammonium chloride (TEA, 30 mM) were used to examine the effects of corticosteroid hormones administered in vivo on the Na+ and K+ transport properties of isolated rat distal colon. The cell membrane changes induced by aldosterone (a specific mineralocorticoid), RU 28362 (a synthetic glucocorticoid with negligible affinity for mineralocorticoid receptors), and dexamethasone (an activator of both mineralocorticoid and glucocorticoid receptors) were compared. 2. In control animals, there was no amiloride-sensitive apical Na+ conductance, and only a relatively small TEA-sensitive apical K+ conductance. 3. Hyperaldosteronism secondary to dietary Na+ depletion for 10-14 days, dexamethasone (600 micrograms 100 g-1 day-1 for 3 days), and RU 28362 (600 micrograms 100 g-1 day-1 for 3 days) induced amiloride-sensitive electrogenic Na+ transport, with the potency of aldosterone greater than dexamethasone greater than RU 28362. 4. With each corticosteroid, increased electrogenic Na+ transport reflected enhanced apical Na+ conductance, and in the case of aldosterone and dexamethasone, 3.3-fold and 2-fold increases respectively in the maximum activity of the basolateral Na+-K+ pump. In contrast, RU 28362 suppressed the maximum activity of the basolateral Na+-K+ pump by 45%. 5. All three corticosteroids enhanced the K+ conductance of the apical membrane, with the potency of aldosterone greater than dexamethasone greater than RU 28362. 6. Co-administration of spironolactone (5 mg 100 g-1 day-1) inhibited the effects of aldosterone on Na+ and K+ transport, but in dexamethasone-treated animals spironolactone resulted in a pattern of response similar to that found in RU 28362-treated animals. 7. The results support the view that mineralocorticoid receptors mediate changes in colonic Na+ and K+ transport which differ quantitatively and qualitatively from those mediated by glucocorticoid receptors. Dexamethasone and similar 'glucocorticoids' activate both types of receptor, with an overall epithelial response which mimics that induced by aldosterone.
摘要
  1. 使用传统微电极、Na⁺通道阻滞剂氨氯吡咪(0.1 mM)和K⁺通道阻滞剂氯化四乙铵(TEA,30 mM)来研究体内给予皮质类固醇激素对分离的大鼠远端结肠Na⁺和K⁺转运特性的影响。比较了醛固酮(一种特异性盐皮质激素)、RU 28362(一种对盐皮质激素受体亲和力可忽略不计的合成糖皮质激素)和地塞米松(盐皮质激素和糖皮质激素受体的激活剂)诱导的细胞膜变化。2. 在对照动物中,不存在氨氯吡咪敏感的顶端Na⁺电导,仅存在相对较小的TEA敏感的顶端K⁺电导。3. 因饮食中Na⁺缺乏10 - 14天导致的醛固酮增多症、地塞米松(600微克/100克体重/天,共3天)和RU 28362(600微克/100克体重/天,共3天)诱导了氨氯吡咪敏感的电生性Na⁺转运,醛固酮的效力大于地塞米松大于RU 28362。4. 每种皮质类固醇激素作用下,电生性Na⁺转运增加反映了顶端Na⁺电导增强,就醛固酮和地塞米松而言,基底外侧Na⁺ - K⁺泵的最大活性分别增加了3.3倍和2倍。相比之下,RU 28362使基底外侧Na⁺ - K⁺泵的最大活性降低了45%。5. 所有三种皮质类固醇激素均增强了顶端膜的K⁺电导,醛固酮的效力大于地塞米松大于RU 28362。6. 同时给予螺内酯(5毫克/100克体重/天)可抑制醛固酮对Na⁺和K⁺转运的影响,但在地塞米松处理的动物中,螺内酯导致的反应模式与RU 28362处理的动物相似。7. 结果支持以下观点:盐皮质激素受体介导结肠Na⁺和K⁺转运的变化,这些变化在数量和质量上与糖皮质激素受体介导的变化不同。地塞米松和类似的“糖皮质激素”激活两种类型的受体,产生的整体上皮反应类似于醛固酮诱导的反应。

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Properties of sodium pumps in internally perfused barnacle muscle fibers.内部灌注藤壶肌纤维中钠泵的特性
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