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首页> 外文期刊>Comparative biochemistry and physiology, Part B. Biochemistry & molecular biology >Accelerated evolution and functional divergence of scorpion short-chain K ~+ channel toxins after speciation
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Accelerated evolution and functional divergence of scorpion short-chain K ~+ channel toxins after speciation

机译:加速进化和功能的散度蝎子短链K ~ +通道毒素物种形成

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摘要

The α-KTx14 subfamily of scorpion toxins is a group of short-chain polypeptides affecting K ~+ channels, including five known members which are restrictedly distributed in Mesobuthus martensii. Here, we describe seven new α-KTx14 peptides from M. martensii and its sibling species Mesobuthus eupeus, two of which (termed MarKTX-3 and MeuKTX-1) were chemically synthesized and refolded for structural and functional studies. Electrophysiological recordings of effects of these two peptides on an array of voltage-gated potassium channels revealed that MarKTX-3 was capable of inhibiting five mammalian K _v1 isoforms (rK _v1.1-rK _v1.5) and the Drosophila Shaker channel with low potency whereas MeuKTX-1 lacks such activity. Circular dichroism spectroscopy analysis combined with homology modeling demonstrates that MarKTX-3 and MeuKTX-1 both adopt a similar cysteine-stabilized α-helical and β-sheet fold. Evolutionary analysis indicates accelerated amino acid substitutions in the mature-peptide-encoding regions of orthologous α-KTx14 peptides after speciation, thereby providing evidences for adaptive evolution and functional divergence of this subfamily.
机译:的α-KTx14蝎子毒素是一个亚科影响K ~ +的短链多肽渠道,包括5个已知的成员限制地分布在Mesobuthus martensii。在这里,我们描述了七个新α-KTx14肽m . martensii Mesobuthus及其兄弟姐妹物种eupeus,其中两个(称为MarKTX-3和化学合成和MeuKTX-1)复合结构和功能研究。电生理记录的影响这两个肽对电压门控的数组钾离子通道显示MarKTX-3能够抑制5 K _v1哺乳动物亚型(rK _v1.1-rK _v1.5)和果蝇与低效力而MeuKTX-1瓶通道缺乏此类活动。光谱分析与同源性相结合建模表明,MarKTX-3和MeuKTX-1都采用类似的cysteine-stabilizedα螺旋和β片折叠。表明加速氨基酸替换mature-peptide-encoding地区的直向同源α-KTx14肽物种形成后,从而为适应提供证据进化和功能差异亚科。

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