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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Na,K-ATPase activity modulates Src activation: A role for ATP/ADP ratio
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Na,K-ATPase activity modulates Src activation: A role for ATP/ADP ratio

机译:Na,K-ATPase活性调节Src激活:ATP / ADP比的作用

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摘要

Digitalis-like compounds (DLCs), specific inhibitors of Na,K-ATPase, are implicated in cellular signaling. Exposure of cell cultures to ouabain, a well-known DLC, leads to up- or down regulation of various processes and involves activation of Src kinase. Since Na,K-ATPase is the only known target for DLC binding an in vitro experimental setup using highly purified Na,K-ATPase from pig kidney and commercially available recombinant Src was used to investigate the mechanism of coupling between the Na,K-ATPase and Src. Digoxin was used as a representative DLC for inhibition of Na,K-ATPase. The activation of Src kinase was measured as the degree of its autophosphorylation. It was observed that in addition to digoxin, Src activation was dependent on concentrations of other specific ligands of Na,K-ATPase: Na +, K +, vanadate, ATP and ADP. The magnitude of the steady-state ATPase activity therefore seemed to affect Src activation. Further experiments with an ATP regenerating system showed that the ATP/ADP ratio determined the extent of Src activation. Thus, our model system which represents the proposed very proximal part of the Na,K-ATPase-Src signaling cascade, shows that Src kinase activity is regulated by both ATP and ADP concentrations and provides no evidence for a direct interaction between Na,K-ATPase and Src.
机译:洋地黄样化合物(DLC)是Na,K-ATPase的特异性抑制剂,与细胞信号传导有关。将细胞培养物暴露于哇巴因(一种众所周知的DLC)会导致各种过程的上调或下调,并涉及Src激酶的激活。由于Na,K-ATPase是唯一已知的DLC结合靶标,因此使用了来自猪肾脏的高度纯化的Na,K-ATPase和市售重组Src的体外实验装置来研究Na,K-ATPase之间的偶联机制和Src。地高辛用作抑制Na,K-ATPase的代表性DLC。测量Src激酶的活化作为其自身磷酸化的程度。观察到除地高辛外,Src活化还取决于Na,K-ATPase的其他特定配体的浓度:Na +,K +,钒酸盐,ATP和ADP。因此,稳态ATPase活性的大小似乎影响Src激活。使用ATP再生系统进行的进一步实验表明,ATP / ADP比率决定了Src活化的程度。因此,我们的模型系统代表拟议的Na,K-ATPase-Src信号级联反应的最接近部分,显示Src激酶活性受ATP和ADP浓度的调节,并且没有提供Na,K-之间直接相互作用的证据ATPase和Src。

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