Kodani Yu, Furukawa Yasuo
Laboratory of Neurobiology, Graduate School of Integrated Arts and Sciences, Hiroshima University, Kagamiyama 1-7-1, Higashi-Hiroshima 739-8521, Japan.
Zoolog Sci. 2010 May;27(5):440-8. doi: 10.2108/zsj.27.440.
FMRFamide-gated Na(+) channel (FaNaC) is a peptide-gated sodium channel in the epithelial Na(+) channel/degenerin family. Although there are some data on the location of the putative peptide binding site, there is no structural information on the activation gating of FaNaC. Here, we addressed the function of a conserved aspartate residue in the second transmembrane domain of FaNaC. We used Aplysia kurodai FaNaC (AkFaNaC) and examined the function of the aspartate (D552) by site-directed mutagenesis and electrophysiological recording in Xenopus oocytes. We found that the macroscopic activation, desensitization, and potency of FMRFamide and its modification by external Ca(2+) and Mg(2+) are greatly affected by physicochemical properties of the amino acid at position 552. We conclude that D552 is situated in a key position that affects the gating properties of FaNaC.
FMRF酰胺门控钠离子通道(FaNaC)是上皮钠离子通道/退化素家族中的一种肽门控钠离子通道。尽管关于假定的肽结合位点的位置已有一些数据,但尚无关于FaNaC激活门控的结构信息。在此,我们研究了FaNaC第二个跨膜结构域中一个保守天冬氨酸残基的功能。我们使用了黑田锦鳚FaNaC(AkFaNaC),并通过定点诱变和非洲爪蟾卵母细胞中的电生理记录来研究天冬氨酸(D552)的功能。我们发现,552位氨基酸的物理化学性质极大地影响了FMRF酰胺的宏观激活、脱敏作用、效力以及其受细胞外Ca(2+)和Mg(2+)的修饰。我们得出结论,D552位于影响FaNaC门控特性的关键位置。
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