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Structure and activity analysis of two spider toxins that alter sodium channel inactivation kinetics. | LitMetric

Structure and activity analysis of two spider toxins that alter sodium channel inactivation kinetics.

Biochemistry

Department of Biochemistry and Immunology, Instituto de Ciências Biológicas, Universidade Federal de Minas Gerais, Belo Horizonte, MG, Brazil.

Published: April 2009

AI Article Synopsis

  • The study investigates the effects of Phoneutria nigriventer toxins PnTx2-5 and PnTx2-6 on sodium channels, revealing that both toxins significantly delay fast inactivation kinetics in neuronal-type sodium channels.
  • PnTx2-6 exhibits a much higher affinity for sodium channels compared to PnTx2-5 and shows irreversible effects for 10-15 minutes after washing, suggesting a unique interaction mechanism.
  • The research also confirms the amino acid sequences of both toxins, establishing their structural models, which indicate a low alpha-helix content and propose a potential binding region based on their affinity differences.

Article 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.

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Source
http://dx.doi.org/10.1021/bi802158pDOI Listing

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