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丝氨酸/苏氨酸激酶SGK2和SGK3是上皮钠离子通道α、β、γ-ENaC的强效刺激因子。

The serine/threonine kinases SGK2 and SGK3 are potent stimulators of the epithelial Na+ channel alpha,beta,gamma-ENaC.

作者信息

Friedrich B, Feng Y, Cohen P, Risler T, Vandewalle A, Bröer S, Wang J, Pearce D, Lang F

机构信息

Physiologisches Institut der Universität Tübingen, Gmelinstrasse 5, 72076 Tübingen, Germany.

出版信息

Pflugers Arch. 2003 Mar;445(6):693-6. doi: 10.1007/s00424-002-0993-8. Epub 2003 Jan 21.

Abstract

The serum- and glucocorticoid-inducible kinase 1 (SGK1) has been identified as a signalling molecule up-regulated by aldosterone, which stimulates the renal epithelial Na(+) channel ENaC. It is therefore thought to participate in the antinatriuretic action of this hormone. More recently, two isoforms, SGK2 and SGK3, have been cloned. The present study was performed to establish whether SGK2 and SGK3 influence ENaC activity similarly to SGK1. Dual-electrode voltage-clamp experiments in Xenopus laevis oocytes expressing alpha,ss,gamma-ENaC with or without SGK1, SGK2 or SGK3 revealed a stimulatory effect of all three kinases on the amiloride-sensitive current (I(Na)). To establish whether the SGK isoforms exert their effects through direct phosphorylation, we replaced the serine at the SGK consensus site of alphaENaC (alpha(S622A)ENaC) by site-directed mutagenesis. alpha(S622A),beta,gamma-ENaC was up-regulated similar to wild-type ENaC, suggesting that SGK isoforms do not act via direct phosphorylation of the transport proteins. In conclusion, SGK2 and SGK3 mimic the function of SGK1 and are likely to participate in the regulation of ENaC activity.

摘要

血清和糖皮质激素诱导激酶1(SGK1)已被确定为一种受醛固酮上调的信号分子,醛固酮可刺激肾上皮钠通道ENaC。因此,人们认为它参与了这种激素的利钠作用。最近,已克隆出两种同工型,即SGK2和SGK3。本研究旨在确定SGK2和SGK3对ENaC活性的影响是否与SGK1相似。在表达α、β、γ-ENaC且有或没有SGK1、SGK2或SGK3的非洲爪蟾卵母细胞中进行的双电极电压钳实验显示,这三种激酶对氨氯地平敏感电流(I(Na))均有刺激作用。为了确定SGK同工型是否通过直接磷酸化发挥作用,我们通过定点诱变将αENaC的SGK共有位点的丝氨酸(α(S622A)ENaC)进行了替换。α(S622A)、β、γ-ENaC的上调与野生型ENaC相似,这表明SGK同工型并非通过直接磷酸化转运蛋白发挥作用。总之,SGK2和SGK3模拟了SGK1的功能,可能参与了ENaC活性的调节。

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