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Title

Molecular characterization of an acidic phospholipase A from Bothrops pirajai snake venom: synthetic C-terminal peptide identifies its antiplatelet region.

Authors

Teixeira, Sabrina; Silveira, Lucas; da Silva, Franco; Marchi-Salvador, Daniela; Silva, Floriano; Izidoro, Luiz; Fuly, André; Juliano, Maria; dos Santos, Camila; Murakami, Mário; Sampaio, Suely; da Silva, Saulo; Soares, Andreimar

Abstract

This paper describes a biochemical and pharmacological characterization of BpirPLA-I, the first acidic Asp49-PLA isolated from Bothrops pirajai. BpirPLA-I caused hypotension in vivo, presented phospholipolytic activity upon artificial substrates and inhibitory effects on platelet aggregation in vitro. Moreover, a synthetic peptide of BpirPLA-I, comprising residues of the C-terminal region, reproduced the antiplatelet activity of the intact protein. A cDNA fragment of 366 bp encompassing the mature form of BpirPLA-I was cloned by reverse transcriptase-PCR of B. pirajai venom gland total RNA. A Bayesian phylogenetic analysis indicated that BpirPLA-I forms a clade with other acid Asp49-PLA enzymes from the Bothrops genus, which are characterized by the high catalytic activity associated with anticoagulant or hypotensive activity or both. Comparison of the electrostatic potential (EP) on the molecular surfaces calculated from a BpirPLA-I homology model and from the crystallographic models of a group of close homologues revealed that the greatest number of charge inversions occurred on the face opposite to the active site entrance, particularly in the Ca ion binding loop. This observation suggests a possible relationship between the basic or acid character of PLA enzymes and the functionality of the Ca ion binding loop.

Subjects

PHOSPHOLIPASES; SNAKE venom; MOLECULAR pharmacology; CATALYST poisoning; ELECTROSTATICS; PHYLOGENY; BOTHROPS

Publication

Archives of Toxicology, 2011, Vol 85, Issue 10, p1219

ISSN

0340-5761

Publication type

Academic Journal

DOI

10.1007/s00204-011-0665-6

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