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首页> 外文期刊>The Journal of Physiology >Protein kinase A induces recruitment of active Na+,K+-ATPase units to the plasma membrane of rat proximal convoluted tubule cells.
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Protein kinase A induces recruitment of active Na+,K+-ATPase units to the plasma membrane of rat proximal convoluted tubule cells.

机译:蛋白激酶A诱导活跃的Na +,K + -ATPase单元募集到大鼠近曲小管细胞的质膜。

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1. The aim of this study was to investigate the mechanism of control of Na+,K+-ATPase activity by the cAMP-protein kinase A (PKA) pathway in rat proximal convoluted tubules. For this purpose, we studied the in vitro action of exogenous cAMP (10-3 M dibutyryl-cAMP (db-cAMP) or 8-bromo-cAMP) and endogenous cAMP (direct activation of adenylyl cyclases by 10-5 M forskolin) on Na+,K+-ATPase activity and membrane trafficking. 2. PKA activation stimulated both the cation transport and hydrolytic activity of Na+,K+-ATPase by about 40%. Transport activity stimulation was specific to the PKA signalling pathway since (1) db-cAMP stimulated the ouabain-sensitive 86Rb+ uptake in a time- and dose-dependent fashion; (2) this effect was abolished by addition of H-89 or Rp-cAMPS, two structurally different PKA inhibitors; and (3) this stimulation was not affected by inhibition of protein kinase C (PKC) by GF109203X. The stimulatory effect of db-cAMP on the hydrolytic activity of Na+,K+-ATPase was accounted for by an increased maximal ATPase rate (Vmax) without alteration of the efficiency of the pump, suggesting that cAMP-PKA pathway was implicated in membrane redistribution control. 3. To test this hypothesis, we used two different approaches: (1) cell surface protein biotinylation and (2) subcellular fractionation. Both approaches confirmed that the cAMP-PKA pathway was implicated in membrane trafficking regulation. The stimulation of Na+,K+-ATPase activity by db-cAMP was associated with an increase (+40%) in Na+, K+-ATPase units expressed at the cell surface which was assessed by Western blotting after streptavidin precipitation of biotinylated cell surface proteins. Subcellular fractionation confirmed the increased expression in pump units at the cell surface which was accompanied by a decrease (-30%) in pump units located in the subcellular fraction corresponding to early endosomes. 4. In conclusion, PKA stimulates Na+,K+-ATPase activity, at least in part, by increasing the number of Na+-K+ pumps in the plasma membrane in proximal convoluted tubule cells.
机译:1.这项研究的目的是研究大鼠近曲小管中cAMP-蛋白激酶A(PKA)途径控制Na +,K + -ATPase活性的机制。为此,我们研究了外源性cAMP(10-3 M dibutyryl-cAMP(db-cAMP)或8-bromo-cAMP)和内源性cAMP(10-5 M毛喉素直接激活腺苷酸环化酶)的体外作用。 Na +,K + -ATPase活性和膜运输。 2. PKA激活可刺激Na +,K + -ATPase的阳离子转运和水解活性约40%。由于(1)db-cAMP以时间和剂量依赖性方式刺激了哇巴因敏感的86Rb +吸收,因此转运活性刺激对PKA信号传导通路具有特异性。 (2)通过加入两种结构不同的PKA抑制剂H-89或Rp-cAMPS消除了这种作用; (3)这种刺激不受GF109203X对蛋白激酶C(PKC)的抑制作用。 db-cAMP对Na +,K + -ATPase水解活性的刺激作用是通过增加最大ATPase速率(Vmax)而没有改变泵的效率来进行的,这表明cAMP-PKA途径与膜的重新分布控制有关。 。 3.为了检验这一假设,我们使用了两种不同的方法:(1)细胞表面蛋白生物素化和(2)亚细胞分级分离。两种方法均证实cAMP-PKA途径与膜运输调控有关。 db-cAMP对Na +,K + -ATPase活性的刺激与细胞表面表达的Na +,K + -ATPase单位的增加(+ 40%)有关,这是通过链霉亲和素沉淀生物素化的细胞表面蛋白后通过蛋白质印迹法评估的。亚细胞分级分离证实了在细胞表面上泵单位中表达的增加,同时伴随着位于早期内体的亚细胞部分中泵单位的减少(-30%)。 4.总之,PKA至少部分地通过增加近曲小管细胞质膜中Na + -K +泵的数量来刺激Na +,K + -ATPase活性。

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