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首页> 外文期刊>The Journal of Membrane Biology: An International Journal for Studies on the Structure, Function & Genesis of Biomembranes >TWO NOVEL TOXINS FROM THE VENOM OF THE SCORPION PANDINUS IMPERATOR SHOW THAT THE N-TERMINAL AMINO ACID SEQUENCE IS IMPORTANT FOR THEIR AFFINITIES TOWARDS SHAKER B K+ CHANNELS
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TWO NOVEL TOXINS FROM THE VENOM OF THE SCORPION PANDINUS IMPERATOR SHOW THAT THE N-TERMINAL AMINO ACID SEQUENCE IS IMPORTANT FOR THEIR AFFINITIES TOWARDS SHAKER B K+ CHANNELS

机译:蝎COR天王病毒毒液中的两种新型毒素表明,N末端氨基酸序列对摇床B K +通道的亲和力很重要

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Two novel peptides were purified from the venom of the scorpion Pandinus imperator, and were named Pi2 and Pi3. Their complete primary structures were determined and their blocking effects on Shaker B K+ channels were studied. Both peptides contain 35 amino acids residues, compacted by three disulfide bridges, and reversibly block the Shaker B K+ channels. They have only one amino acid changed in their sequence, at position 7 (a proline for a glutamic acid). Whereas peptide Pi2, containing the Pro7, binds the Shaker B KC channels with a K-d of 8.2 nM, peptide Pi3 containing the Clu7 residue has a much lower affinity of 140 nM. Both peptides are capable of displacing the binding of I-125-noxiustoxin to brain synaptosome membranes. Since these two novel peptides are about 50% identical to noxiustoxin, the present results support previous data published by our group showing that the amino-terminal region of noxiustoxin, and also the amino-terminal sequence of the newly purified homologues: Pi2, and Pi3, are important for the recognition of potassium channels. [References: 22]
机译:从蝎子Pandinus imperator的毒液中纯化了两个新肽,分别命名为Pi2和Pi3。确定了它们的完整一级结构,并研究了其对Shaker B K +通道的阻断作用。两种肽均包含35个氨基酸残基,由三个二硫键压紧,可逆地阻断了Shaker B K +通道。它们的序列中只有一个氨基酸发生变化,位于7位(谷氨酸的脯氨酸)。含有Pro7的肽Pi2以8.2 nM的K-d与Shaker B KC通道结合,而含有Clu7残基的肽Pi3的亲和力低得多,为140 nM。两种肽都能够取代I-125-诺克毒素与脑突触体膜的结合。由于这两个新肽与诺克斯毒素约有50%相同,因此本研究结果支持了我们小组先前发布的数据,该数据表明诺克斯毒素的氨基末端区域以及新纯化的同系物的氨基末端序列:Pi2和Pi3对钾通道的识别很重要。 [参考:22]

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