Fahlke C, Beck C L, George A L
Department of Medicine, Vanderbilt University School of Medicine, Nashville, TN 37232, USA.
Proc Natl Acad Sci U S A. 1997 Mar 18;94(6):2729-34. doi: 10.1073/pnas.94.6.2729.
Autosomal dominant myotonia congenita is an inherited disorder of skeletal muscle caused by mutations in a voltage-gated Cl- channel gene (CLCN1, 7q35). Here, we report that a mutation predicting the substitution of Gly 230 by glutamic acid (G230E) between segments D3 and D4 dramatically alters the pore properties of a recombinant human muscle Cl- channel (hCIC-1) expressed in a mammalian cell line (tsA201). The G230E mutation causes substantial changes in anion and cation selectivity as well as a fundamental change in rectification of the current-voltage relationship. Whereas wild-type channels are characterized by pronounced inward rectification and a Cl > thiocyanate > Br > NO(3) > I > CH(3)SO(3) selectivity, G230E exhibits outward rectification at positive potentials and a thiocyanate > NO(3) > I > Br > Cl > CH(3)SO(3) selectivity. Furthermore, the cation-to-anion permeability ratio of the mutant is much greater than that of the wild-type channel. Voltage-dependent blocks by intracellular and extracellular iodide help to distinguish two distinct ion binding sites within the hClC-1 conduction pathway. Both binding sites are preserved in the mutant but have decreased affinities for iodide. These findings suggest that Gly 230 is critical for normal ion conductance in hClC-1 and that this residue resides within the channel pore.
常染色体显性遗传性先天性肌强直是一种由电压门控氯离子通道基因(CLCN1,7q35)突变引起的骨骼肌遗传性疾病。在此,我们报告,预测在D3和D4片段之间将甘氨酸230替换为谷氨酸(G230E)的突变,显著改变了在哺乳动物细胞系(tsA201)中表达的重组人肌肉氯离子通道(hCIC-1)的孔道特性。G230E突变导致阴离子和阳离子选择性发生实质性变化,以及电流-电压关系整流的根本改变。野生型通道的特征是明显的内向整流以及Cl>硫氰酸盐>Br>NO(3)>I>CH(3)SO(3)选择性,而G230E在正电位时表现出外向整流以及硫氰酸盐>NO(3)>I>Br>Cl>CH(3)SO(3)选择性。此外,突变体的阳离子与阴离子渗透率之比远大于野生型通道。细胞内和细胞外碘化物的电压依赖性阻断有助于区分hClC-1传导途径内两个不同的离子结合位点。两个结合位点在突变体中均得以保留,但对碘化物的亲和力降低。这些发现表明,甘氨酸230对于hClC-1中的正常离子传导至关重要,并且该残基位于通道孔内。
