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一种新型A超家族芋螺毒素的特性分析

Characterisation of a Novel A-Superfamily Conotoxin.

作者信息

Wilson David T, Bansal Paramjit S, Carter David A, Vetter Irina, Nicke Annette, Dutertre Sébastien, Daly Norelle L

机构信息

Centre for Molecular Therapeutics, Australian Institute of Tropical Health and Medicine, James Cook University, Smithfield, QLD 4878, Australia.

Centre for Pain Research, Institute for Molecular Bioscience, The University of Queensland, St Lucia, QLD 4072, Australia.

出版信息

Biomedicines. 2020 May 20;8(5):128. doi: 10.3390/biomedicines8050128.

Abstract

Conopeptides belonging to the A-superfamily from the venomous molluscs, , are typically α-conotoxins. The α-conotoxins are of interest as therapeutic leads and pharmacological tools due to their selectivity and potency at nicotinic acetylcholine receptor (nAChR) subtypes. Structurally, the α-conotoxins have a consensus fold containing two conserved disulfide bonds that define the two-loop framework and brace a helical region. Here we report on a novel α-conotoxin Pl168, identified from the transcriptome of , which has an unusual 4/8 loop framework. Unexpectedly, NMR determination of its three-dimensional structure reveals a new structural type of A-superfamily conotoxins with a different disulfide-stabilized fold, despite containing the conserved cysteine framework and disulfide connectivity of classical α-conotoxins. The peptide did not demonstrate activity on a range of nAChRs, or Ca and Na channels suggesting that it might represent a new pharmacological class of conotoxins.

摘要

来自有毒软体动物的属于A超家族的芋螺肽通常是α-芋螺毒素。由于α-芋螺毒素对烟碱型乙酰胆碱受体(nAChR)亚型具有选择性和效力,它们作为治疗先导物和药理学工具备受关注。在结构上,α-芋螺毒素具有一个共有折叠,包含两个保守的二硫键,这些二硫键定义了双环框架并支撑着一个螺旋区域。在此,我们报告一种从[具体物种]转录组中鉴定出的新型α-芋螺毒素Pl168,它具有不寻常的4/8环框架。出乎意料的是,通过核磁共振确定其三维结构发现,尽管它含有经典α-芋螺毒素保守的半胱氨酸框架和二硫键连接方式,但却是一种具有不同二硫键稳定折叠的A超家族芋螺毒素新结构类型。该肽在一系列nAChR以及钙通道和钠通道上均未表现出活性,这表明它可能代表了一类新的芋螺毒素药理学类别。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5d96/7277881/0f249df880f1/biomedicines-08-00128-g001.jpg

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