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Solution conformation of alpha-conotoxin GIC a novel potent antagonist of alpha3beta2 nicotinic acetylcholine receptors.

机译:α-芋螺毒素GIC的溶液构象一种新型的α3beta2烟碱乙酰胆碱受体拮抗剂。

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摘要

Alpha-conotoxin GIC is a 16-residue peptide isolated from the venom of the cone snail Conus geographus. Alpha-conotoxin GIC potently blocks the alpha3beta2 subtype of human nicotinic acetylcholine receptor, showing a high selectivity for neuronal versus muscle subtype [McIntosh, Dowell, Watkins, Garrett, Yoshikami, and Olivera (2002) J. Biol. Chem. 277, 33610-33615]. We have now determined the three-dimensional solution structure of alpha-conotoxin GIC by NMR spectroscopy. The structure of alpha-conotoxin GIC is well defined with backbone and heavy atom root mean square deviations (residues 2-16) of 0.53 A and 0.96 A respectively. Structure and surface comparison of alpha-conotoxin GIC with the other alpha4/7 subfamily conotoxins reveals unique structural aspects of alpha-conotoxin GIC. In particular, the structural comparison between alpha-conotoxins GIC and MII indicates molecular features that may confer their similar receptor specificity profile, as well as those that provide the unique binding characteristics of alpha-conotoxin GIC.
机译:α-芋螺毒素GIC是一种16残基的多肽,是从圆锥蜗牛Conus geographus的毒液中分离出来的。 α-芋螺毒素GIC可以有效阻断人烟碱型乙酰胆碱受体的alpha3beta2亚型,对神经元和肌肉亚型显示出高选择性[McIntosh,Dowell,Watkins,Garrett,Yoshikami和Olivera(2002)J. Biol。Acad。Sci.Sci.USA,88:1111-88。化学277,33610-33615]。现在,我们已经通过NMR光谱法确定了α-芋螺毒素GIC的三维溶液结构。 α-芋螺毒素GIC的结构定义明确,骨架和重原子均方根偏差(残基2-16)分别为0.53 A和0.96A。 α-芋螺毒素GIC与其他α4/ 7亚家族芋螺毒素的结构和表面比较揭示了α-芋螺毒素GIC的独特结构方面。特别是,α-伴毒素GIC和MII之间的结构比较表明,分子特征可赋予它们相似的受体特异性谱,以及提供α-伴毒素GIC独特结合特征的分子特征。

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