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人和兔红细胞的钙激活钾通道对毒液肽毒素表现出独特的抑制模式。

Ca(2+)-activated K+ channels of human and rabbit erythrocytes display distinctive patterns of inhibition by venom peptide toxins.

作者信息

Brugnara C, Armsby C C, De Franceschi L, Crest M, Euclaire M F, Alper S L

机构信息

Departments of Pathology and Laboratory Medicine, Children's Hospital, Boston, MA 02115, USA.

出版信息

J Membr Biol. 1995 Sep;147(1):71-82. doi: 10.1007/BF00235398.

Abstract

Despite recent progress in the molecular characterization of high-conductance Ca(2+)-activated K+ (maxi-K) channels, the molecular identities of intermediate conductance Ca(2+)-activated K+ channels, including that of mature erythrocytes, remains unknown. We have used various peptide toxins to characterize the intermediate conductance Ca(2+)-activated K+ channels (Gardos pathway) of human and rabbit red cells. With studies on K+ transport and on binding of 125I-charybdotoxin (ChTX) and 125I-kaliotoxin (KTX) binding in red cells, we provide evidence for the distinct nature of the red cell Gardos channel among described Ca(2+)-activated K+ channels based on (i) the characteristic inhibition and binding patterns produced by ChTX analogues, iberiotoxin (IbTX) and IbTX-like ChTX mutants, and KTX (1-37 and 1-38 variants); (ii) the presence of some properties heretofore attributed only to voltage-gated channels, including inhibition of K transport by margatoxin (MgTX) and by stichodactyla toxin (StK); (iii) and the ability of scyllatoxin (ScyTX) and apamin to displace bound 125I-charybdotoxin, a novel property for K+ channels. These unusual pharmacological characteristics suggest a unique structure for the red cell Gardos channel.

摘要

尽管近期在高电导钙激活钾(大电导钾)通道的分子特征研究方面取得了进展,但包括成熟红细胞在内的中电导钙激活钾通道的分子身份仍然未知。我们使用了各种肽毒素来表征人和兔红细胞的中电导钙激活钾通道(加尔多斯通路)。通过对红细胞中钾转运以及125I - 蝎毒素(ChTX)和125I - 钾毒素(KTX)结合的研究,基于以下几点,我们为红细胞加尔多斯通道在所描述的钙激活钾通道中具有独特性质提供了证据:(i)ChTX类似物、埃博毒素(IbTX)和IbTX样ChTX突变体以及KTX(1 - 37和1 - 38变体)产生的特征性抑制和结合模式;(ii)存在一些迄今仅归因于电压门控通道的特性,包括玛格毒素(MgTX)和刺尾鱼毒素(StK)对钾转运的抑制;(iii)以及刺参毒素(ScyTX)和蜂毒明肽能够置换结合的125I - 蝎毒素,这是钾通道的一种新特性。这些不同寻常的药理学特征表明红细胞加尔多斯通道具有独特的结构。

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