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吲哚胺对氨氯吡咪敏感的钠电导的抑制作用。

Inhibition of amiloride-sensitive sodium conductance by indoleamines.

作者信息

Legris G J, Will P C, Hopfer U

出版信息

Proc Natl Acad Sci U S A. 1982 Mar;79(6):2046-50. doi: 10.1073/pnas.79.6.2046.

Abstract

To examine a possible role of indoleamines in the regulation of epithelial sodium absorption, the effect of serotonin (5-hydroxytryptamine) and several derivatives on electrolyte transport was measured in vitro in the baboon bronchus and in the trachea and colon of sodium-deficient rats. Serotonin, melatonin (N-acetyl-5-hydroxytryptamine), and harmaline (1-methyl-7-methoxy-3,4-dihydro-beta-carboline) inhibited sodium transport in all three preparations in a similar manner to the natriuretic agent amiloride. In all three epithelia, sodium absorption via the amiloride-sensitive pathway constitutes a substantial portion of total electrolyte transport, measured as the amiloride-sensitive short-circuit current. Thus 25 microM amiloride inhibited the short-circuit current 21% in the rat trachea, 63% in the baboon bronchus, and 90% in the rat colon. Serotonin, melatonin, and harmaline inhibited the amiloride-sensitive portion of the short-circuit current from the luminal side of the epithelium. The inhibition was rapid, requiring only seconds, and maximal inhibition by serotonin was identical to that by amiloride. When sodium was omitted from the luminal solution, the short-circuit current was reduced a similar amount, suggesting that sodium absorption was being inhibited by both amiloride and the indoles. The IC50 value for amiloride was 50 nM in the baboon bronchus and 500 nM in the rat colon. In contrast, the IC50 value for serotonin was 0.4 mM in the baboon bronchus and 8 mM in the rat colon. These results, together with the wide distribution of amine-precursor-uptake-and-decarboxylation (APUD) cells in the respiratory and intestinal tract, suggest that certain indoleamines could play a role as local regulators of fluid and electrolyte transport. For example, in the airways, indoleamines may be one of the factors involved in regulation of the depth of the periciliary fluid layer.

摘要

为了研究吲哚胺在上皮钠吸收调节中的可能作用,在体外测量了血清素(5-羟色胺)及其几种衍生物对狒狒支气管以及缺钠大鼠的气管和结肠中电解质转运的影响。血清素、褪黑素(N-乙酰-5-羟色胺)和骆驼蓬碱(1-甲基-7-甲氧基-3,4-二氢-β-咔啉)在所有这三种制剂中均以与利钠剂阿米洛利相似的方式抑制钠转运。在所有这三种上皮组织中,通过阿米洛利敏感途径的钠吸收占总电解质转运的很大一部分,总电解质转运以阿米洛利敏感短路电流来衡量。因此,25微摩尔的阿米洛利在大鼠气管中使短路电流抑制21%,在狒狒支气管中抑制63%,在大鼠结肠中抑制90%。血清素、褪黑素和骆驼蓬碱从上皮组织的管腔侧抑制短路电流的阿米洛利敏感部分。这种抑制迅速,仅需数秒,血清素的最大抑制作用与阿米洛利相同。当从管腔溶液中去除钠时,短路电流降低的幅度相似,这表明阿米洛利和吲哚类化合物均抑制钠吸收。在狒狒支气管中,阿米洛利的半数抑制浓度(IC50)值为50纳摩尔,在大鼠结肠中为500纳摩尔。相比之下,血清素在狒狒支气管中的IC50值为0.4毫摩尔,在大鼠结肠中为8毫摩尔。这些结果,连同胺前体摄取和脱羧(APUD)细胞在呼吸道和肠道中的广泛分布,表明某些吲哚胺可能作为液体和电解质转运的局部调节因子发挥作用。例如,在气道中,吲哚胺可能是参与调节纤毛周围液层深度的因素之一。

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