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alpha-conotoxin EpI, a novel sulfated peptide from Conus episcopatus that selectively targets neuronal nicotinic acetylcholine receptors

机译:alpha-conotoxin EpI,一种来自圆锥壳猴的新型硫酸化肽,可选择性靶向神经元烟碱型乙酰胆碱受体

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摘要

We have isolated and characterized ol-conotoxin EpI, a novel sulfated peptide from the venom of the molluscivorous snail, Conus episcopatus, The peptide was classified as an cy-conotoxin based on sequence, disulfide connectivity, and pharmacological target. EpI has ho mology to sequences of previously described cu-conotoxins, particularly PnIA, PnIB, and ImI, However, EpI differs from previously reported conotoxins in that it has a sulfotyrosine residue, identified by amino acid analysis and mass spectrometry, Native EpI was shown to coelute with synthetic EpI, The peptide sequence is consistent with most, but not all, recognized criteria for predicting tyrosine sulfation sites in proteins and peptides, The activities of synthetic EpI and its unsulfated analogue [Tyr(15)]EpI were similar. Both peptides caused competitive inhibition of nicotine action on bovine adrenal chromaffin cells (neuronal nicotinic ACh receptors) but had no effect on the rat phrenic nerve-diaphragm (muscle nicotinic ACh receptors), Both EpI and [Tyr(15)]EpI partly inhibited acetylcholine-evoked currents in isolated parasympathetic neurons of rat intracardiac ganglia, These results indicate that EPI and [Tyr(15)]EpI selectively inhibit alpha 3 beta 2 and alpha 3 beta 4 nicotinic acetylcholine receptors.
机译:我们已经分离和表征了ol-conotoxin EpI,这是一种从食肉蜗牛的毒液Conus episcopatus的毒液中提取的新型硫酸化肽。根据序列,二硫键连接性和药理学目标,该肽被分类为cy-conotoxin。 EpI对先前描述的铜-肠毒素,特别是PnIA,PnIB和ImI的序列具有同源性。然而,EpI与先前报道的铜毒素的不同之处在于,它具有磺基酪氨酸残基(通过氨基酸分析和质谱鉴定),显示为天然EpI为了与合成EpI共洗脱,该肽序列与大多数(但不是全部)公认的预测蛋白质和肽中酪氨酸硫酸化位点的标准一致。合成EpI及其未硫酸化类似物[Tyr(15)] EpI的活性相似。两种肽均对烟碱对牛肾上腺嗜铬细胞(神经元烟碱ACh受体)产生竞争性抑制作用,但对大鼠神经隔膜(肌肉烟碱ACh受体)无影响,EpI和[Tyr(15)] EpI均部分抑制了乙酰胆碱在大鼠心内神经节的副交感神经元中诱发的电流,这些结果表明,EPI和[Tyr(15)] EpI选择性抑制α3β2和α3β4烟碱乙酰胆碱受体。

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