Toxins (Apr 2020)

Neurotoxin Merging: A Strategy Deployed by the Venom of the Spider <i>Cupiennius salei</i> to Potentiate Toxicity on Insects

  • Benjamin Clémençon,
  • Lucia Kuhn-Nentwig,
  • Nicolas Langenegger,
  • Lukas Kopp,
  • Steve Peigneur,
  • Jan Tytgat,
  • Wolfgang Nentwig,
  • Benjamin P. Lüscher

DOI
https://doi.org/10.3390/toxins12040250
Journal volume & issue
Vol. 12, no. 4
p. 250

Abstract

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The venom of Cupiennius salei is composed of dozens of neurotoxins, with most of them supposed to act on ion channels. Some insecticidal monomeric neurotoxins contain an α-helical part besides their inhibitor cystine knot (ICK) motif (type 1). Other neurotoxins have, besides the ICK motif, an α-helical part of an open loop, resulting in a heterodimeric structure (type 2). Due to their low toxicity, it is difficult to understand the existence of type 2 peptides. Here, we show with the voltage clamp technique in oocytes of Xenopus laevis that a combined application of structural type 1 and type 2 neurotoxins has a much more pronounced cytolytic effect than each of the toxins alone. In biotests with Drosophila melanogaster, the combined effect of both neurotoxins was enhanced by 2 to 3 log units when compared to the components alone. Electrophysiological measurements of a type 2 peptide at 18 ion channel types, expressed in Xenopus laevis oocytes, showed no effect. Microscale thermophoresis data indicate a monomeric/heterodimeric peptide complex formation, thus a direct interaction between type 1 and type 2 peptides, leading to cell death. In conclusion, peptide mergers between both neurotoxins are the main cause for the high cytolytic activity of Cupiennius salei venom.

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