首页> 外文期刊>Pfluegers Archiv: European Journal of Physiology >A basic residue in the proximal C-terminus is necessary for efficient activation of the M-channel subunit Kv7.2 by PI(4,5)P2
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A basic residue in the proximal C-terminus is necessary for efficient activation of the M-channel subunit Kv7.2 by PI(4,5)P2

机译:近端C-末端的基本残留物是通过PI(4,5)P2的高效激活M沟道亚基KV7.2所必需的

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摘要

All Kv7 potassium channels require membrane phosphatidylinositol-4,5- bisphosphate (PI(4,5)P2) for their normal function and hence can be physiologically regulated by neurotransmitters and hormones that stimulate phosphoinositide hydrolysis. Recent mutational analysis indicates that a cluster of basic residues in the proximal C-terminus (K354/K358/R360/K362) is crucial for PI(4,5)P2 activation of cardiac Kv7.1 channels. Since this cluster is largely conserved in all Kv7 subunits, we tested whether homologous residues are also required for activation of Kv7.2 (a subunit of neuronal M-channels). We found that the mutation Kv7.2 (R325A) (corresponding to R360 in Kv7.1) reduced Kv7.2 current amplitude by ~60 % (P 0.02) without change in voltage sensitivity and reduced the sensitivity of Kv7.2 channels to dioctanoyl-phosphatidylinositol-4,5-bisphosphate by ~eightfold (P 0.001). Taking into account previous experiments (Zhang et al., Neuron 37:963-75, 2003) implicating Kv7.2 (H328), and since R325 and H328 are conserved in homologous positions in all other Kv7 channels, we suggest that this proximal C-terminal domain adjacent to the last transmembrane domain that contains R325 and H328 (in Kv7.2) might play a major role in the activation of all members of the Kv7 channel family by PI(4,5)P2.
机译:所有KV7钾通道都需要膜磷脂酰肌醇-4,5-二磷酸(PI(4,5)P2)的正常功能,因此可以通过刺激磷酸阳性水解的神经递质和激素生理学上调节。最近的突变分析表明,近端C-末端(K354 / K358 / R360 / K366)中的一组基本残留物对于心脏KV7.1通道的PI(4,5)P2活化是至关重要的。由于该簇在所有KV7亚基中大大保存,因此我们测试了是否还需要kV7.2的激活同源残留物(神经元M-通道的亚基)。我们发现突变Kv7.2(R325A)(对应于KV7.1中的R360)减少了kV7.2电流幅度〜60%(P <0.02),而不会改变电压灵敏度并降低KV7.2通道的灵敏度通过〜8倍(P <0.001)的二辛酰基 - 磷脂酰肌醇-4,5-二磷酸酯。考虑到以前的实验(张等人,神经元37:963-75,2003)含有KV7.2(H328),并且由于R325和H328在所有其他KV7通道中的同源位置保守,我们建议这一近C - 含有R325和H328(在KV7.2中)的最后跨膜结构域相邻的脉冲域可能在通过PI(4,5)P2激活KV7通道家族的所有成员中发挥重要作用。

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