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2.0埃分辨率下的蛇毒神经毒素(vipoxin)晶体结构:分子进化产生的毒性功能调控实例

Crystal structure of vipoxin at 2.0 A: an example of regulation of a toxic function generated by molecular evolution.

作者信息

Perbandt M, Wilson J C, Eschenburg S, Mancheva I, Aleksiev B, Genov N, Willingmann P, Weber W, Singh T P, Betzel C

机构信息

Institute of Biochemistry, Free University of Berlin, Germany.

出版信息

FEBS Lett. 1997 Aug 4;412(3):573-7. doi: 10.1016/s0014-5793(97)00853-3.

Abstract

Vipoxin is the main toxic component in the venom of the Bulgarian snake Vipera ammodytes meridionalis, the most toxic snake in Europe. Vipoxin is a complex between a toxic phospholipase A2 (PLA2) and a non-toxic protein inhibitor. The structure is of genetic interest due to the high degree of sequence homology (62%) between the two functionally different components. The structure shows that the formation of the complex in vipoxin is significantly different to that seen in many known structures of phospholipases and contradicts the assumptions made in earlier studies. The modulation of PLA2 activity is of great pharmacological interest, and the present structure will be a model for structure-based drug design.

摘要

蝰蛇毒素是欧洲毒性最强的蛇——保加利亚蛇南欧蝰蛇毒液中的主要毒性成分。蝰蛇毒素是一种有毒的磷脂酶A2(PLA2)与一种无毒蛋白质抑制剂之间形成的复合物。由于这两种功能不同的成分之间具有高度的序列同源性(62%),其结构具有遗传学研究价值。该结构表明,蝰蛇毒素中复合物的形成与许多已知磷脂酶结构中的情况显著不同,这与早期研究中的假设相矛盾。PLA2活性的调节具有重大药理学研究价值,目前的结构将成为基于结构的药物设计的模型。

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