dc.contributorUniv Hamburg
dc.contributorBulgarian Acad Sci
dc.contributorUniv Med Ctr Hamburg Eppendorf
dc.contributorBUL BIO NCIPD Ltd
dc.contributorUniversidade Estadual Paulista (Unesp)
dc.date.accessioned2014-05-20T14:02:31Z
dc.date.accessioned2022-10-05T14:50:43Z
dc.date.available2014-05-20T14:02:31Z
dc.date.available2022-10-05T14:50:43Z
dc.date.created2014-05-20T14:02:31Z
dc.date.issued2012-01-01
dc.identifierMolecular Biosystems. Cambridge: Royal Soc Chemistry, v. 8, n. 5, p. 1405-1411, 2012.
dc.identifier1742-206X
dc.identifierhttp://hdl.handle.net/11449/22037
dc.identifier10.1039/c2mb05490f
dc.identifierWOS:000302368600003
dc.identifier9162508978945887
dc.identifier0000-0003-2460-1145
dc.identifier.urihttp://repositorioslatinoamericanos.uchile.cl/handle/2250/3895720
dc.description.abstractMyotoxicity and membrane damage play a central role in the life-threatening effects of the viper envenomation. Myotoxins are an important part of the viper venomics. A Ser49 PLA(2)-like myotoxin from the venom of Vipera ammodytes meridionalis, the most venomous snake in Europe, was crystallized and its three-dimensional structure determined. The toxin is devoid of phospholipolytic activity. The structure demonstrates a formation of dimers. In the dimers functionally important peptide segments, located on the protein surface, point in the same direction which can strengthen the pharmacological effect. This supports the hypothesis about the physiological importance of the toxin oligomerization for the myotoxicity and membrane damage. The crystallographic model revealed that the structural determinants of myotoxicity (a positively charged C-terminal region and a hydrophobic knuckle) are fully exposed on the protein surface and accessible for interactions with target membranes. Distortion of the catalytic site region explains the absence of enzymatic activity. The structure reveals anion-binding sites which can be considered as possible sites of interactions of the toxin with a negatively charged membrane surface. The high structural similarity of the Ser49 myotoxin and Asp49 PLA(2) from the same venom suggests an evolutionary relationship: probably, the Ser49 myotoxin is a product of evolution of the catalytically active phospholipase A(2). The first toxin lost the enzymatic activity which is not necessary for the myotoxicity but preserved the cytotoxicity and membrane damaging activity as important components of the venom toxicity.
dc.languageeng
dc.publisherRoyal Soc Chemistry
dc.relationMolecular Biosystems
dc.relation2.759
dc.rightsAcesso restrito
dc.sourceWeb of Science
dc.titleCrystal structure of a dimeric Ser49 PLA(2)-like myotoxic component of the Vipera ammodytes meridionalis venomics reveals determinants of myotoxicity and membrane damaging activity
dc.typeArtigo


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