Characterization of three "Birtoxin-like" toxins from the Androctonus amoreuxi scorpion venom |
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Authors: | Abbas Najwa Rosso Jean-Pierre Céard Brigitte Belghazi Maya Lebrun Regine Bougis Pierre-Edouard Martin-Eauclaire Marie-France |
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Affiliation: | a CNRS UMR6231, CRN2M, Université de la Méditerranée, Faculté de Médecine secteur Nord, CS80011, Bd Pierre Dramard, F-13344 Marseille Cedex 15, France b CAPM, IFR11 Institut Jean Roche, Université de la Méditerranée, Faculté de Médecine secteur Nord, CS80011, Bd Pierre Dramard, F-13344 Marseille Cedex 15, France c Plate-forme Protéomique de l’IMM, Marseille Protéomique (IBiSA), CNRS, F-13402 Marseille Cedex 20, France |
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Abstract: | The venom of the North African scorpion Androctonus amoreuxi (Aam) was analyzed using a combination of gel filtration, C18 reverse phase HPLC together with mass spectrometry analysis and bioassays. Three novel Birtoxin-like (BTX-L) peptides of 58 amino acid residues comprising three disulfide bridges were isolated and chemically characterized. One peptide, AamBTX-L3, induced serious toxic symptoms in mice and was lethal at nanogram quantities using intracerebroventricular injection. The three BTX-L peptides were tested in competition experiments on rat brain synaptosomes against the 125I-labeled “classical” α- and β-toxins of reference, as well as with the 125I-KTX, a voltage-gated potassium channel blocker. Only AamBTX-L3 was able to prevent the equilibrium binding of the β-toxin 125I-Css IV to its receptor site 4 with a IC50 value of 189 nM. Even if previous electrophysiological data allowed the classification of other BTX-L peptides among the β-type toxins, this report clearly shows that AamBTX-L3 is pharmacologically a β-toxin, which recognizes the voltage-gated Na+ (Nav) channels from central mammalian neurons. In order to uncover the residues functionally essential for interaction between the AamBTX-L3 with the putative receptor site of 125I-Css IV on Nav1.2, molecular models of the three novel Aam BTX-L molecules were made and their surfaces were compared to the already described Css IV biologically interactive surfaces. A hypothesis is given that in BTX-L3, three residues found in the α-helix play a key role during target binding. |
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Keywords: | Birtoxin Scorpion toxin Sodium channel |
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