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氨基酸对血管加压素刺激的水流动的重要性。

Importance of amino acids on vasopressin-stimulated water flow.

作者信息

Carvounis C P, Carvounis G, Wilk B J

出版信息

J Clin Invest. 1985 Aug;76(2):779-88. doi: 10.1172/JCI112035.

Abstract

The presence of several naturally occurring amino acids in the serosal bath of toad urinary bladder significantly alters the hydrosmotic response of this tissue to vasopressin. We found that histidine, glutamate, and lysine increase vasopressin-stimulated water flow by 75%, 60%, and 43%, respectively. In contrast, alanine did not alter vasopressin-stimulated water flow, whereas glutamine decreased it by 25%. The effect of each amino acid represents intracellular events because their effects on theophylline-stimulated water flow were similar to those found with vasopressin. However, the site of action of amino acids varied, with some operating at steps before and others at steps after cyclic AMP generation. The fact that the metabolically inactive D-histidine and D-glutamate are as effective as their metabolically active L-counterparts suggests that the action of amino acids depends upon some physicochemical properties of their molecules. The ability of amino acids to influence the hydrosmotic effects of vasopressin was shown to be independent of prostaglandin generation, ionic composition, and molecular charge. In the case of histidine, we were able to obtain some understanding of the mechanism responsible for its action. We first showed that the effect of histidine does not depend upon its metabolism. In addition to D-histidine being as effective as the metabolically active L-histidine, we also showed that histidine is effective when its metabolism is abolished by low ambient temperature and also when its incorporation into proteins was prevented by cycloheximide. These findings suggest that histidine operates through some physicochemical property localized on its molecule. We were able to show that this property resides on the imidazole part of histidine. Imidazole, similar to histidine, increases vasopressin-stimulated water flow. Methylation of histidine on the imidazole ring completely abolished its effectiveness in increasing vasopressin-stimulated water flow. In contrast, methylation of histidine at the side chain increased vasopressin action similar to that found for histidine. We provide evidence that the physicochemical property of the imidazole ring of histidine is that of chelating Zn++ intracellularly, and that the intracellular site of action of histidine is closely linked to microtubules formation and/or action.

摘要

蟾蜍膀胱浆膜浴中几种天然存在的氨基酸的存在显著改变了该组织对血管加压素的渗透反应。我们发现,组氨酸、谷氨酸和赖氨酸分别使血管加压素刺激的水流量增加了75%、60%和43%。相比之下,丙氨酸没有改变血管加压素刺激的水流量,而谷氨酰胺使其减少了25%。每种氨基酸的作用代表细胞内事件,因为它们对茶碱刺激的水流量的影响与对血管加压素的影响相似。然而,氨基酸的作用位点各不相同,一些在环磷酸腺苷生成之前起作用,另一些在环磷酸腺苷生成之后起作用。代谢无活性的D -组氨酸和D -谷氨酸与其代谢有活性的L -对应物一样有效,这一事实表明氨基酸的作用取决于其分子的某些物理化学性质。氨基酸影响血管加压素渗透作用的能力被证明与前列腺素生成、离子组成和分子电荷无关。就组氨酸而言,我们能够对其作用机制有一些了解。我们首先表明,组氨酸的作用不依赖于其代谢。除了D -组氨酸与代谢有活性的L -组氨酸一样有效外,我们还表明,当环境温度较低使其代谢被消除时,以及当环己酰亚胺阻止其掺入蛋白质时,组氨酸仍然有效。这些发现表明,组氨酸通过其分子上定位的某些物理化学性质起作用。我们能够表明,这种性质存在于组氨酸的咪唑部分。咪唑与组氨酸相似,能增加血管加压素刺激的水流量。组氨酸咪唑环上的甲基化完全消除了其增加血管加压素刺激水流量的有效性。相比之下,组氨酸侧链上的甲基化增加血管加压素作用的方式与组氨酸相似。我们提供的证据表明,组氨酸咪唑环的物理化学性质是在细胞内螯合Zn++,并且组氨酸在细胞内的作用位点与微管形成和/或作用密切相关。

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