| Literature DB >> 19231838 |
Alessandra Matavel1, Cécile Fleury, Leida C Oliveira, Franck Molina, Maria Elena de Lima, Jader S Cruz, Marta N Cordeiro, Michael Richardson, Carlos H I Ramos, Paulo S L Beirão.
Abstract
In this work, Phoneutria nigriventer toxins PnTx2-5 and PnTx2-6 were shown to markedly delay the fast inactivation kinetics of neuronal-type sodium channels. Furthermore, our data show that they have significant differences in their interaction with the channel. PnTx2-6 has an affinity 6 times higher than that of PnTx2-5, and its effects are not reversible within 10-15 min of washing. PnTx2-6 partially (59%) competes with the scorpion alpha-toxin AaHII, but not with the scorpion beta-toxin CssIV, thus suggesting a mode of action similar to that of site 3 toxins. However, PnTx2-6 is not removed by strong depolarizing pulses, as in the known site 3 toxins. We have also established the correct PnTx2-5 amino acid sequence and confirmed the sequence of PnTx2-6, in both cases establishing that the cysteines are in their oxidized form. A structural model of each toxin is proposed. They show structures with poor alpha-helix content. The model is supported by experimental and theoretical tests. A likely binding region on PnTx2-5 and PnTx2-6 is proposed on the basis of their different affinities and sequence differences.Entities:
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Year: 2009 PMID: 19231838 DOI: 10.1021/bi802158p
Source DB: PubMed Journal: Biochemistry ISSN: 0006-2960 Impact factor: 3.162