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Structure of the polypeptide crotamine from the Brazilian rattlesnake Crotalus durissus terrificus

机译:巴西响尾蛇Croctalus durissus terrificus的多肽巴豆胺的结构

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摘要

The crystal structure of the myotoxic, cell-penetrating, basic polypeptide crotamine isolated from the venom of Crotalus durissus terrificus has been determined by single-wavelength anomalous dispersion techniques and refined at 1.7 Å resolution. The structure reveals distinct cationic and hydrophobic surface regions that are located on opposite sides of the molecule. This surface-charge distribution indicates its possible mode of interaction with negatively charged phospholipids and other molecular targets to account for its diverse pharmacological activities. Although the sequence identity between crotamine and human β-defensins is low, the three-dimensional structures of these functionally related peptides are similar. Since crotamine is a leading member of a large family of myotoxic peptides, its structure will provide a basis for the design of novel cell-penetrating molecules.
机译:通过单波长异常分散技术确定了从毒猪屎毒液中分离出来的具有肌毒性的,可穿透细胞的碱性多肽巴豆胺的晶体结构,并以1.7Å的分辨率精制。该结构揭示了位于分子相对侧的不同阳离子和疏水表面区域。该表面电荷分布表明其与带负电荷的磷脂和其他分子靶标相互作用的可能模式,以说明其多种药理活性。尽管巴豆胺和人β-防御素之间的序列同一性较低,但是这些功能相关肽的三维结构相似。由于巴豆胺是大量肌毒性肽家族的主要成员,因此其结构将为设计新型细胞穿透分子提供基础。

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