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  A dipteran’s novel sucker punch: Evolution of arthropod atypical venom with a neurotoxic component in robber flies (asilidae, diptera)

Drukewitz, S. H., Fuhrmann, N., Undheim, E. A. B., Blanke, A., Giribaldi, J., Mary, R., et al. (2018). A dipteran’s novel sucker punch: Evolution of arthropod atypical venom with a neurotoxic component in robber flies (asilidae, diptera). Toxins, 10(1): 29. doi:10.3390/toxins10010029.

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 Creators:
Drukewitz, Stephan Holger, Author
Fuhrmann, Nico1, Author           
Undheim, Eivind A. B., Author
Blanke, Alexander, Author
Giribaldi, Julien, Author
Mary, Rosanna, Author
Laconde, Guillaume, Author
Dutertre, Sébastien, Author
von Reumont, Björn Marcus, Author
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1Max Planck Research Group Biological Clocks, Max Planck Institute for Evolutionary Biology, Max Planck Society, ou_2355691              

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Free keywords: Arthropod venom evolution; Asilidae; Asilidin; Cysteine inhibitor knot peptide; Functional morphology; Neurotoxins; Synchrotron micro computed tomography
 Abstract: Predatory robber flies (Diptera, Asilidae) have been suspected to be venomous due to their ability to overpower well-defended prey. However, details of their venom composition and toxin arsenal remained unknown. Here, we provide a detailed characterization of the venom system of robber flies through the application of comparative transcriptomics, proteomics and functional morphology. Our results reveal asilid venoms to be dominated by peptides and non-enzymatic proteins, and that the majority of components in the crude venom is represented by just ten toxin families, which we have named Asilidin1–10. Contrary to what might be expected for a liquid-feeding predator, the venoms of robber flies appear to be rich in novel peptides, rather than enzymes with a putative pre-digestive role. The novelty of these peptides suggests that the robber fly venom system evolved independently from hematophagous dipterans and other pancrustaceans. Indeed, six Asilidins match no other venom proteins, while three represent known examples of peptide scaffolds convergently recruited to a toxic function. Of these, members of Asilidin1 closely resemble cysteine inhibitor knot peptides (ICK), of which neurotoxic variants occur in cone snails, assassin bugs, scorpions and spiders. Synthesis of one of these putative ICKs, U-Asilidin1-Mar1a, followed by toxicity assays against an ecologically relevant prey model revealed that one of these likely plays a role as a neurotoxin involved in the immobilization of prey. Our results are fundamental to address these insights further and to understand processes that drive venom evolution in dipterans as well as other arthropods. © 2018 by the authors. Licensee MDPI, Basel, Switzerland.

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Language(s): eng - English
 Dates: 2017-12-192017-12-042017-12-272018-01-052018
 Publication Status: Issued
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 Identifiers: DOI: 10.3390/toxins10010029
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Title: Toxins
Source Genre: Journal
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Publ. Info: Basel : Molecular Diversity Preservation International (MDPI)
Pages: - Volume / Issue: 10 (1) Sequence Number: 29 Start / End Page: - Identifier: ISSN: 2072-6651
CoNE: https://pure.mpg.de/cone/journals/resource/2072-6651