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关于寡聚状态对响尾蛇毒素生物学活性作用的见解:由巴西矛头蝮蛇毒中两种响尾蛇毒素B同工型形成的四聚体磷脂酶A2的晶体结构

Insights into the role of oligomeric state on the biological activities of crotoxin: crystal structure of a tetrameric phospholipase A2 formed by two isoforms of crotoxin B from Crotalus durissus terrificus venom.

作者信息

Marchi-Salvador Daniela P, Corrêa Luiz C, Magro Angelo J, Oliveira Clayton Z, Soares Andreimar M, Fontes Marcos R M

机构信息

Departamento de Física e Biofísica, Instituto de Biociências, UNESP, Botucatu, SP, Brazil.

出版信息

Proteins. 2008 Aug 15;72(3):883-91. doi: 10.1002/prot.21980.

Abstract

Crotoxin B (CB or Cdt PLA(2)) is a basic Asp49-PLA(2) found in the venom of Crotalus durissus terrificus and it is one of the subunits that constitute the crotoxin (Cro). This heterodimeric toxin, main component of the C. d. terrificus venom, is completed by an acidic, nontoxic, and nonenzymatic component (crotoxin A, CA or crotapotin), and it is related to important envenomation effects such as neurological disorders, myotoxicity, and renal failure. Although Cro has been crystallized since 1938, no crystal structure of this toxin or its subunits is currently available. In this work, the authors present the crystal structure of a novel tetrameric complex formed by two dimers of crotoxin B isoforms (CB1 and CB2). The results suggest that these assemblies are stable in solution and show that Ser1 and Glu92 of CB1 and CB2, respectively, play an important role in the oligomerization. The tetrameric and dimeric conformations resulting from the association of the isoforms may increase the neurotoxicity of the toxin CB by the creation of new binding sites, which could improve the affinity of the molecular complexes to the presynaptic membrane.

摘要

响尾蛇毒素B(CB或Cdt PLA₂)是一种在南美巨蝮毒液中发现的碱性天冬氨酸49 - PLA₂,它是构成响尾蛇毒素(Cro)的亚基之一。这种异二聚体毒素是南美巨蝮毒液的主要成分,由一种酸性、无毒且无酶活性的成分(响尾蛇毒素A,CA或crotapotin)补充完整,它与诸如神经紊乱、肌毒性和肾衰竭等重要的中毒效应有关。尽管自1938年以来Cro已被结晶,但目前尚无该毒素或其亚基的晶体结构。在这项研究中,作者展示了由两个响尾蛇毒素B亚型(CB1和CB2)二聚体形成的新型四聚体复合物的晶体结构。结果表明这些组装体在溶液中是稳定的,并表明CB1和CB2的Ser1和Glu92分别在寡聚化过程中发挥重要作用。由这些亚型缔合产生的四聚体和二聚体构象可能通过产生新的结合位点来增加毒素CB的神经毒性,这可能会提高分子复合物对突触前膜的亲和力。

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