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结肠上皮细胞中糖皮质激素对钠吸收的刺激作用是由糖皮质激素诱导型受体介导的。

Glucocorticoid stimulation of sodium absorption in colon epithelia is mediated by corticosteroid IB receptor.

作者信息

Bastl C P, Barnett C A, Schmidt T J, Litwack G

出版信息

J Biol Chem. 1984 Jan 25;259(2):1186-95.

PMID:6693382
Abstract

Studies with RU26988, a synthetic glucocorticoid which does not bind to aldosterone receptors, suggest glucocorticoid-induced colonic cation transport is affected through glucocorticoid-specific receptors. RU26988 produced a 700% increase in sodium absorption and doubled transmural potential difference in proximal and distal colon of adrenalectomized rats. Scatchard analysis suggested a single class of receptors with a KD of approximately 10(-9) M. Competition of unlabeled steroids for [3H]triamcinolone acetonide-binding sites paralleled the steroids' biologic potency as glucocorticoids. Heat treatment (25 degrees C, 30 min) markedly enhanced binding of the glucocorticoid-receptor complexes to DNA-cellulose. The activated receptor from both proximal and distal colon was eluted in the prewash from DEAE-Sephadex A-50 anion exchange columns both in the presence and absence of protease inhibitors and has an estimated molecular weight (Stokes radius) of 33,000-37,000 (25-26 A). These results identify the colonic receptor as glucocorticoid binder IB, a receptor previously identified as the major binder only in kidney cortex. The finding of an apparently unique receptor in the two tissues where glucocorticoids stimulate cation transport suggests that the phenotypic response mediated by glucocorticoids in different tissues might be determined by the structure of the receptor and that glucocorticoid binder IB is the glucocorticoid cation transport receptor.

摘要

使用RU26988(一种不与醛固酮受体结合的合成糖皮质激素)进行的研究表明,糖皮质激素诱导的结肠阳离子转运是通过糖皮质激素特异性受体受到影响的。RU26988使肾上腺切除大鼠近端和远端结肠的钠吸收增加了700%,跨壁电位差增加了一倍。Scatchard分析表明存在一类KD约为10(-9) M的受体。未标记类固醇对[3H]曲安奈德结合位点的竞争与这些类固醇作为糖皮质激素的生物活性平行。热处理(25摄氏度,30分钟)显著增强了糖皮质激素-受体复合物与DNA-纤维素的结合。在存在和不存在蛋白酶抑制剂的情况下,来自近端和远端结肠的活化受体均在DEAE-葡聚糖A-50阴离子交换柱的预洗脱中被洗脱,其估计分子量(斯托克斯半径)为33,000 - 37,000(25 - 26 Å)。这些结果将结肠受体鉴定为糖皮质激素结合蛋白IB,该受体先前仅在肾皮质中被鉴定为主要结合蛋白。在糖皮质激素刺激阳离子转运的两个组织中发现明显独特的受体表明,糖皮质激素在不同组织中介导的表型反应可能由受体结构决定,并且糖皮质激素结合蛋白IB是糖皮质激素阳离子转运受体。

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