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电压门控钾通道的分子特性

Molecular properties of voltage-gated K+ channels.

作者信息

Dolly J O, Parcej D N

机构信息

Department of Biochemistry, Imperial College, London, United Kingdom.

出版信息

J Bioenerg Biomembr. 1996 Jun;28(3):231-53. doi: 10.1007/BF02110698.

Abstract

Subfamilies of voltage-activated K+ channels (Kv1-4) contribute to controlling neuron excitability and the underlying functional parameters. Genes encoding the multiple alpha subunits from each of these protein groups have been cloned, expressed and the resultant distinct K+ currents characterized. The predicted amino acid sequences showed that each alpha subunit contains six putative membrane-spanning alpha-helical segments (S1-6), with one (S4) being deemed responsible for the channels' voltage sensing. Additionally, there is an H5 region, of incompletely defined structure, that traverses the membrane and forms the ion pore; residues therein responsible for K+ selectively have been identified. Susceptibility of certain K+ currents produced by the Shaker-related subfamily (Kv1) to inhibition by alpha-dendrotoxin has allowed purification of authentic K+ channels from mammalian brain. These are large (M(r) approximately 400 kD), octomeric sialoglycoproteins composed of alpha and beta subunits in a stoichiometry of (alpha)4(beta)4, with subtypes being created by combinations of subunit isoforms. Subsequent cloning of the genes for beta 1, beta 2 and beta 3 subunits revealed novel sequences for these hydrophilic proteins that are postulated to be associated with the alpha subunits on the inner side of the membrane. Coexpression of beta 1 and Kv1.4 subunits demonstrated that this auxiliary beta protein accelerates the inactivation of the K+ current, a striking effect mediate by an N-terminal moiety. Models are presented that indicate the functional domains pinpointed in the channel proteins.

摘要

电压激活钾离子通道(Kv1 - 4)的亚家族有助于控制神经元兴奋性及相关功能参数。编码这些蛋白家族中多个α亚基的基因已被克隆、表达,并对由此产生的不同钾离子电流进行了表征。预测的氨基酸序列表明,每个α亚基包含六个假定的跨膜α螺旋片段(S1 - 6),其中一个(S4)被认为负责通道的电压感应。此外,存在一个结构尚未完全明确的H5区域,它横穿细胞膜并形成离子孔;已确定其中负责钾离子选择性的残基。震颤相关亚家族(Kv1)产生的某些钾离子电流对α - 树眼镜蛇毒素抑制作用的敏感性,使得能够从哺乳动物大脑中纯化出真正的钾离子通道。这些通道很大(相对分子质量约为400 kD),是由α和β亚基按化学计量比(α)4(β)4组成的八聚体唾液酸糖蛋白,通过亚基异构体的组合产生亚型。随后对β1、β2和β3亚基基因的克隆揭示了这些亲水性蛋白的新序列,推测它们与膜内侧的α亚基相关。β1和Kv1.4亚基的共表达表明,这种辅助性β蛋白可加速钾离子电流的失活,这是一种由N端部分介导的显著效应。文中还展示了一些模型,这些模型指出了通道蛋白中确定的功能域。

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