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首页> 外文期刊>Pfluegers Archiv: European Journal of Physiology >Intracellular and extracellular amino acids that influence C-type inactivation and its modulation in a voltage-dependent potassium channel.
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Intracellular and extracellular amino acids that influence C-type inactivation and its modulation in a voltage-dependent potassium channel.

机译:细胞内和细胞外氨基酸影响C型失活及其在电压依赖性钾通道中的调节。

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摘要

The rate of C-type inactivation of the cloned voltage-gated potassium channel, Kv1.3, measured in membrane patches from Xenopus oocytes, increases when the patch is detached from the cell; the structural basis for this on-cell/off-cell change was examined. First, four serine and threonine residues, that are putative sites for phosphorylation by protein kinases A and C, were mutated to alanines. Mutating any one of these residues, or two or three of them simultaneously, does not eliminate the change in C-type inactivation. However, the basal rate of C-type inactivation in the cell-attached patch is markedly slower in the triple phosphorylation site mutant. Second, a homologous potassium channel, Kv 1.6, does not exhibit the on-cell/off-cell change. When an extracellular histidine at position 401 of Kv1.3 is replaced with tyrosine, the residue at the equivalent position (430) in Kv1.6, the resulting Kv1.3 H401Y mutant channel does not undergo the on-cell/off-cell change. The results indicate that severalpotentially phosphorylatable intracellular amino acids influence the basal rate of C-type inactivation, but are not essential for the on-cell/off-cell change in inactivation kinetics. In contrast, an extracellular amino acid is critical for this on-cell/off-cell change.
机译:在非洲爪蟾卵母细胞的膜片中测得的克隆的电压门控钾离子通道的C型失活率Kv1.3,当贴片从细胞中分离时增加。检验了这种电池上/电池外变化的结构基础。首先,将四个假定的蛋白激酶A和C磷酸化的丝氨酸和苏氨酸残基突变为丙氨酸。突变这些残基中的任何一个,或同时突变两个或三个,不能消除C型失活的变化。但是,在三重磷酸化位点突变体中,细胞附着的斑块中C型失活的基础速率明显变慢。其次,同源钾通道Kv 1.6不会显示细胞内/细胞外变化。当用酪氨酸替代Kv1.3的401位胞外组氨酸时,Kv1.6的等价位(430)处的残基,所得的Kv1.3 H401Y突变体通道不会发生细胞内/细胞外变化。结果表明,几种潜在的可磷酸化的细胞内氨基酸会影响C型失活的基础速率,但对于失活动力学中的细胞内/细胞外变化不是必需的。相反,细胞外氨基酸对于这种细胞内/细胞外变化至关重要。

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