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蛋白质磷酸化对单个钙离子依赖性钾通道活性的调节。

Modulation of single Ca2+-dependent K+-channel activity by protein phosphorylation.

作者信息

Ewald D A, Williams A, Levitan I B

出版信息

Nature. 1985;315(6019):503-6. doi: 10.1038/315503a0.

Abstract

There is considerable evidence that cyclic AMP can modulate the electrical activity of excitable cells and that protein phosphorylation by the catalytic subunit (CS) of cAMP-dependent protein kinase is a necessary step in these modulatory effects. In analogy to alterations in enzyme activities following phosphorylation, it seems possible that direct phosphorylation of ion-channel proteins may alter their gating properties, giving rise to the observe changes in electrical activity. However, the results obtained so far do not indicate whether it is ion channels themselves that are phosphorylated, or whether phosphorylation is simply an early step in some cascade of events which leads ultimately to modulation of channel activity. The development of single-channel recording techniques has provided a way to investigate this question. Here we describe effects of CS on the activity of individual CA2+-dependent K+ channels from the nervous system of the land snail Helix measured in isolated membrane patches and in artificial phospholipid bilayers. The results demonstrate that cAMP-dependent protein phosphorylation produces long-lasting changes in the activity of individual channels, and indicate that the relevant phosphorylation site is closely associated with the channel.

摘要

有大量证据表明,环磷酸腺苷(cAMP)可调节可兴奋细胞的电活动,且依赖cAMP的蛋白激酶催化亚基(CS)介导的蛋白磷酸化是这些调节作用中的必要步骤。类似于磷酸化后酶活性的改变,离子通道蛋白的直接磷酸化可能会改变其门控特性,从而导致观察到的电活动变化,这似乎是有可能的。然而,目前所获得的结果并未表明被磷酸化的究竟是离子通道本身,还是磷酸化仅仅是某些最终导致通道活性调节的事件级联反应中的早期步骤。单通道记录技术的发展为研究这个问题提供了一种方法。在此,我们描述了CS对从陆地蜗牛Helix神经系统分离出的单个Ca2+依赖性K+通道活性的影响,这些通道活性是在分离的膜片和人工磷脂双分子层中测量的。结果表明,依赖cAMP的蛋白磷酸化会使单个通道的活性产生持久变化,并表明相关的磷酸化位点与通道紧密相关。

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