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海南捕鸟蛛海南毒素-III的序列特异性¹H-NMR归属及二级结构测定

Sequence-specific 1H-NMR assignment and determination of the secondary structure of hainantoxin-III from the spider Ornithoctonus hainana.

作者信息

Liu Zhonghua, Zhu Qi, Hu Weijun, Liang Songping

机构信息

College of Life Sciences, Hunan Normal University, Changsha, 410081, Hunan, P. R. China.

出版信息

Protein Pept Lett. 2013 Jul 1;20(7):761-6. doi: 10.2174/0929866511320070005.

Abstract

Hainantoxin-III (HNTX-III) purified from the venom of the spider Ornithoctonus hainana is a novel neurotoxin preferentially inhibiting tetrodotoxin-sensitive voltage-gated sodium channels in rat dorsal root ganglion cells. The structure of this toxin in aqueous solution was investigated using 2-D 1H-NMR techniques. The complete sequencespecific assignments of proton resonances in the 1H-NMR spectra were obtained by analyzing a series of 2-D spectra, including DQF-COSY, TOCSY and NOESY spectra, in H2O or D2O. All the backbone protons and more than 95% of the side-chain protons have been assigned by dαN, dβN, and dNN connectivities in NOESY spectrum. Furthermore, the secondary structure of HNTX-III was identified from NMR data. It consists mainly of a short triple-stranded antiparallel β-sheet formed by Asp7 to Cys9, Tyr21 to Ser23, and Lys27 to Val30. Because HNTX-III shares high sequence identity (>70%) with HWTX-I and HNTX-I, we proposed that they all share a structural scaffold known as the inhibitor cystine knot architectural motif. This study provides a basis for the further determination of the solution conformation of HNTX-III.

摘要

从海南捕鸟蛛毒液中纯化得到的海南毒素-III(HNTX-III)是一种新型神经毒素,它能优先抑制大鼠背根神经节细胞中对河豚毒素敏感的电压门控钠通道。利用二维¹H-NMR技术研究了该毒素在水溶液中的结构。通过分析一系列二维谱,包括在H₂O或D₂O中的双量子滤波相关谱(DQF-COSY)、全相关谱(TOCSY)和核Overhauser效应谱(NOESY),获得了¹H-NMR谱中质子共振的完整序列特异性归属。通过NOESY谱中的dαN、dβN和dNN连接关系,已对所有主链质子和超过95%的侧链质子进行了归属。此外,从NMR数据确定了HNTX-III的二级结构。它主要由由Asp7至Cys9、Tyr21至Ser23以及Lys27至Val30形成的短的三股反平行β-折叠组成。由于HNTX-III与HWTX-I和HNTX-I具有较高的序列同一性(>70%),我们提出它们都共享一种称为抑制剂胱氨酸结结构基序的结构支架。该研究为进一步确定HNTX-III的溶液构象提供了基础。

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