PKC stimulated by glucagon decreases UT-A1 urea transporter expression in rat IMCD

被引:0
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作者
Yuristella Yano
Adilson C. Rodrígues
Ana C. de Bragança
Lucia C. Andrade
Antonio J. Magaldi
机构
[1] Universidade de São Paulo,Laboratório de Pesquisa Básica
来源
Pflügers Archiv - European Journal of Physiology | 2008年 / 456卷
关键词
Glucagon; UT-A1; Membrane transport proteins/urea transport; Glucagon antagonist; Vasopressin; PKC; PMA; Staurosporin;
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学科分类号
摘要
It is well-known that glucagon increases fractional excretion of urea in rats after a protein intravenous infusion. This effect was investigated by using: (a) in vitro microperfusion technique to measure [14C]-urea permeability (Pu × 10−5cm/s) in inner medullary collecting ducts (IMCD) from normal rats in the presence of 10−7M of glucagon and in the absence of vasopressin and (b) immunoblot techniques to determine urea transporter expression in tubule suspension incubated with the same glucagon concentration. Seven groups of IMCDs (n = 47) were studied. Our results revealed that: (a) glucagon decreased urea reabsorption dose-dependently; (b) the glucagon antagonist des-His1-[Glu9], blocked the glucagon action but not vasopressin action; (c) the phorbol myristate acetate, decreased urea reabsorption but (d) staurosporin, restored its effect; e) staurosporin decreased glucagon action, and finally, (f) glucagon decreased UT-A1 expression. We can conclude that glucagon reduces UT-A1 expression via a glucagon receptor by stimulating PKC.
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页码:1229 / 1237
页数:8
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