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Short-term effect of aldosterone on vasopressin-sensitive adenylate cyclase in rat collecting tubule.

作者信息

el Mernissi G, Barlet-Bas C, Khadouri C, Cheval L, Marsy S, Doucet A

机构信息

Laboratoire des Biomembranes, Faculté des Sciences, Université Cadi Ayyad, Marrakech, Morocco.

出版信息

Am J Physiol. 1993 May;264(5 Pt 2):F821-6. doi: 10.1152/ajprenal.1993.264.5.F821.

DOI:10.1152/ajprenal.1993.264.5.F821
PMID:8498534
Abstract

Because previous studies indicated that, in the rat collecting tubule, vasopressin (AVP)-sensitive adenylate cyclase (AC) is controlled by mineralocorticoids in the long term, the present study was designed to investigate whether such a control also exists in the short term. Therefore, we investigated the in vivo and in vitro effects of aldosterone on AC activity in cortical and outer medullary collecting tubules (CCD and OMCD, respectively) from adrenalectomized rats. Injection of aldosterone (10 micrograms/kg body wt) to adrenalectomized rats restored within 3 h AVP-sensitive AC activity in the CCD and OMCD up to the levels observed in the corresponding segments of adrenal intact rats. Similarly, incubating CCD or OMCD from adrenalectomized rats for 2.5 h in the presence of 10(-8) M aldosterone enhanced AVP-sensitive AC activity up to values similar to those found in normal rats. In vitro stimulation of AVP-sensitive AC activity was dose dependent with regard to aldosterone [apparent affinity constant (K0.5) approximately 10(-9) M], appeared after a 30-min lag period, and reached its maximum after 2-2.5 h. In addition, it was totally abolished by the antimineralocorticoid spironolactone, whereas the specific glucocorticoid antagonist RU 38486 had no effect. Finally, actinomycin D and cycloheximide totally abolished the in vitro action of aldosterone, demonstrating the involvement of protein synthesis in that process.

摘要

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引用本文的文献

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Vasopressin potentiates mineralocorticoid selectivity by stimulating 11 beta hydroxysteroid deshydrogenase in rat collecting duct.血管加压素通过刺激大鼠集合管中的11β-羟类固醇脱氢酶来增强盐皮质激素的选择性。
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