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藜芦碱与KIFMK之间的结合竞争:一种RIIA钠通道的开放通道阻断肽。

Competition for binding between veratridine and KIFMK: an open channel blocking peptide of the RIIA sodium channel.

作者信息

Ghatpande A S, Sikdar S K

机构信息

Molecular Biophysics Unit, Indian Institute of Science, Bangalore, India.

出版信息

J Membr Biol. 1997 Dec 1;160(3):177-82. doi: 10.1007/s002329900306.

Abstract

Veratridine, an alkaloid isolated from the rhizome of V. album, binds and slows the inactivation of the brain sodium channels. The synthetic pentapeptide KIFMK causes a voltage- and use-dependent open-channel block of the RIIA (rat brain type IIA) sodium channel (Eaholtz, Scheuer & Catterall, 1994). Our studies on the RIIA sodium channel expressed in CHO cells reveal that the fraction of veratridine modified sodium channels decreases linearly with increasing KIFMK concentration. However, the time constant for dissociation of veratridine from the channel remains unchanged in the presence of a high concentration of KIFMK, as opposed to that in the presence of QX314 where the dissociation appears to be more complex. These data are consistent with mutually exclusive binding of the open channel blocking peptide and veratridine to the brain sodium channel.

摘要

藜芦定是从白藜芦根茎中分离出的一种生物碱,它能结合并减缓脑钠通道的失活。合成五肽KIFMK会导致RIIA(大鼠脑IIA型)钠通道出现电压和使用依赖性的开放通道阻滞(埃霍尔茨、舍尔和卡特拉尔,1994年)。我们对CHO细胞中表达的RIIA钠通道的研究表明,随着KIFMK浓度的增加,藜芦定修饰的钠通道比例呈线性下降。然而,与QX314存在时解离情况似乎更复杂不同,在高浓度KIFMK存在的情况下,藜芦定从通道解离的时间常数保持不变。这些数据与开放通道阻断肽和藜芦定在脑钠通道上的互斥结合一致。

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