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首页> 外文期刊>The Journal of biological chemistry >A Helical Conotoxin from Conus imperialis Has a Novel Cysteine Framework and Defines a New Superfamily
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A Helical Conotoxin from Conus imperialis Has a Novel Cysteine Framework and Defines a New Superfamily

机译:来自Conus Imperialis的螺旋毒素具有新的半胱氨酸框架,并定义了一个新的超家族

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摘要

Cone snail venoms are a rich source of peptides, many of which are potent and selective modulators of ion channels and receptors. Here we report the isolation and characterization of two novel conotoxins from the venom of Conus imperialis. These two toxins contain a novel cysteine framework, C-C-C-CC-C, which has not been found in other conotoxins described to date. We name it framework XXIII and designate the two toxins im23a and im23b; cDNAs of these toxins exhibit a novel signal peptide sequence, which defines a new K-superfamily. The disulfide connectivity of im23a has been mapped by chemical mapping of partially reduced intermediates and by NMR structure calculations, both of which establish a I-II, III-IV, V-VI pattern of disulfide bridges. This pattern was also confirmed by synthesis of im23a with orthogonal protection of individual cysteine residues. The solution structure of im23a reveals that im23a adopts a novel helical hairpin fold. A cluster of acidic residues on the surface of the molecule is able to bind calcium. The biological activity of the native and recombinant peptides was tested by injection into mice intracranially and intravenously to assess the effects on the central and peripheral nervous systems, respectively. Intracranial injection of im23a or im23b into mice induced excitatory symptoms; however, the biological target of these new toxins has yet to be identified.
机译:锥蜗牛毒液是丰富的肽来源,其中许多是离子通道和受体的有效和选择性调节剂。在这里,我们报告了来自康菲斯毒液的两种新型细胞毒素的分离和表征。这两个毒素含有一种新型半胱氨酸框架,C-C-C-CC-C,其尚未发现于迄今为止的其他同胞毒素中。我们将IT框架XXIII命名并指定两个毒素IM23A和IM23B;这些毒素的CDNA表现出一种新的信号肽序列,其限定了一种新的K-超家族。 IM23A的二硫键已被部分减少的中间体和通过NMR结构计算的化学映射映射,其中两者都建立了二硫桥的I-II,III-IV,V-VI模式。还通过合成具有正交保护单个半胱氨酸残基的IM23A来证实该模式。 IM23A的溶液结构揭示了IM23A采用新型螺旋发夹折叠。分子表面上的酸性残基簇能够结合钙。通过甲状腺和静脉内注射到小鼠的原生和重组肽的生物活性,以分别评估对中枢神经和周围神经系统的影响。颅内注射IM23A或IM23B成小鼠诱导的兴奋性症状;然而,这些新毒素的生物学靶标尚未识别。

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