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一种新型的Kv1.6通道和烟碱型乙酰胆碱受体亚型的芋螺毒素抑制剂定义了一个新的芋螺毒素超家族。

A novel conotoxin inhibitor of Kv1.6 channel and nAChR subtypes defines a new superfamily of conotoxins.

作者信息

Imperial Julita S, Bansal Paramjit S, Alewood Paul F, Daly Norelle L, Craik David J, Sporning Annett, Terlau Heinrich, López-Vera Estuardo, Bandyopadhyay Pradip K, Olivera Baldomero M

机构信息

Department of Biology, University of Utah, Salt Lake City, Utah 84112, USA.

出版信息

Biochemistry. 2006 Jul 11;45(27):8331-40. doi: 10.1021/bi060263r.

Abstract

Using assay-directed fractionation of the venom from the vermivorous cone snail Conus planorbis, we isolated a new conotoxin, designated pl14a, with potent activity at both nicotinic acetylcholine receptors and a voltage-gated potassium channel subtype. pl14a contains 25 amino acid residues with an amidated C-terminus, an elongated N-terminal tail (six residues), and two disulfide bonds (1-3, 2-4 connectivity) in a novel framework distinct from other conotoxins. The peptide was chemically synthesized, and its three-dimensional structure was demonstrated to be well-defined, with an alpha-helix and two 3(10)-helices present. Analysis of a cDNA clone encoding the prepropeptide precursor of pl14a revealed a novel signal sequence, indicating that pl14a belongs to a new gene superfamily, the J-conotoxin superfamily. Five additional peptides in the J-superfamily were identified. Intracranial injection of pl14a in mice elicited excitatory symptoms that included shaking, rapid circling, barrel rolling, and seizures. Using the oocyte heterologous expression system, pl14a was shown to inhibit both a K+ channel subtype (Kv1.6, IC50 = 1.59 microM) and neuronal (IC50 = 8.7 microM for alpha3beta4) and neuromuscular (IC50 = 0.54 microM for alpha1beta1 epsilondelta) subtypes of the nicotinic acetylcholine receptor (nAChR). Similarities in sequence and structure are apparent between the middle loop of pl14a and the second loop of a number of alpha-conotoxins. This is the first conotoxin shown to affect the activity of both voltage-gated and ligand-gated ion channels.

摘要

通过对食虫圆锥蜗牛Conus planorbis毒液进行定向分析分离,我们得到了一种新的芋螺毒素,命名为pl14a,它对烟碱型乙酰胆碱受体和一种电压门控钾通道亚型均具有强效活性。pl14a含有25个氨基酸残基,C末端酰胺化,N末端有一个延长的尾巴(6个残基),并在一个与其他芋螺毒素不同的新型结构框架中有两个二硫键(1-3、2-4连接)。该肽经化学合成,其三维结构明确,存在一个α螺旋和两个3(10)螺旋。对编码pl14a前原肽前体的cDNA克隆进行分析,发现了一个新的信号序列,表明pl14a属于一个新的基因超家族——J-芋螺毒素超家族。在J-超家族中还鉴定出另外5种肽。给小鼠颅内注射pl14a会引发兴奋症状,包括颤抖、快速转圈、翻滚和癫痫发作。利用卵母细胞异源表达系统,pl14a被证明可抑制一种钾通道亚型(Kv1.6,IC50 = 1.59微摩尔)以及烟碱型乙酰胆碱受体(nAChR)的神经元亚型(α3β4的IC50 = 8.7微摩尔)和神经肌肉亚型(α1β1εδ的IC50 = 0.54微摩尔)。pl14a的中间环与许多α-芋螺毒素的第二个环在序列和结构上存在明显相似性。这是首个被证明能影响电压门控和配体门控离子通道活性的芋螺毒素。

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