AI Article Synopsis

  • Discrepin is a scorpion peptide derived from the venom of Tityus discrepans that inhibits IA currents in voltage-dependent K+ channels of rat cerebellum granular cells.
  • Six mutants of Discrepin were created to identify key amino acid residues affecting its blocking ability, with V6K showing the most significant increase in blocking activity.
  • The study suggests that introducing basic residues, particularly in the N-terminal region, enhances the peptide's effectiveness, drawing parallels to the highly active peptide BmTx3 from Buthus martensi scorpion.

Article Abstract

Discrepin is a scorpion peptide that blocks preferentially the IA currents of the voltage-dependent K+ channel of rat cerebellum granular cells. It was isolated from the venom of the buthid scorpion Tityus discrepans and contains 38 amino acid residues with a pyroglutamic acid at the N-terminal site. Discrepin has the lowest sequence identity (approx. 50%) among the six members of the alpha-KTx15 sub-family of scorpion toxins. In order to find out which residues are important for the blocking effects of Discrepin, six mutants were chemically synthesized (V6K, I19R, D20K, T35V, I19R-D20K, I19R-D20K-R21V), correctly folded and their physiological properties were examined. Substitution of residues V6 and D20 for basically charged amino acids increases the blocking activity of Discrepin, specially the mutation V6K at the N-terminal segment of the toxin. Analysis of 3D-structure models of the mutants V6K and D20K supports the idea that basic residues improve their blocking activities, similarly to what happens with BmTx3, a toxic peptide obtained from Buthus martensi scorpion, which has the highest known blocking effects of IA currents in K+ channels of rat cerebellum granular cells.

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http://dx.doi.org/10.1016/j.bbagen.2008.01.012DOI Listing

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