AI Article Synopsis

  • Cone snail venoms, particularly from Conus textile, are being explored as a source for new peptide drugs, prompting a study of venom from different regions.
  • A newly identified conopeptide, α-conotoxin TxIC, is part of the 4/7 α-conotoxin family, notable for its unique post-translational modifications, which make it chemically distinct from other conopeptides.
  • While it shows low activity against human acetylcholine receptors, it is highly effective in targeting invertebrate receptors, suggesting that its modifications may contribute to selectivity in toxin action across different species.

Article Abstract

Cone snail venoms provide a largely untapped source of novel peptide drug leads. To enhance the discovery phase, a detailed comparative proteomic analysis was undertaken on milked venom from the mollusk-hunting cone snail, Conus textile, from three different geographic locations (Hawai'i, American Samoa and Australia's Great Barrier Reef). A novel milked venom conopeptide rich in post-translational modifications was discovered, characterized and named α-conotoxin TxIC. We assign this conopeptide to the 4/7 α-conotoxin family based on the peptide's sequence homology and cDNA pre-propeptide alignment. Pharmacologically, α-conotoxin TxIC demonstrates minimal activity on human acetylcholine receptor models (100 μM, <5% inhibition), compared to its high paralytic potency in invertebrates, PD50 = 34.2 nMol kg(-1). The non-post-translationally modified form, [Pro](2,8)[Glu](16)α-conotoxin TxIC, demonstrates differential selectivity for the α3β2 isoform of the nicotinic acetylcholine receptor with maximal inhibition of 96% and an observed IC50 of 5.4 ± 0.5 μM. Interestingly its comparative PD50 (3.6 μMol kg(-1)) in invertebrates was ~100 fold more than that of the native peptide. Differentiating α-conotoxin TxIC from other α-conotoxins is the high degree of post-translational modification (44% of residues). This includes the incorporation of γ-carboxyglutamic acid, two moieties of 4-trans hydroxyproline, two disulfide bond linkages, and C-terminal amidation. These findings expand upon the known chemical diversity of α-conotoxins and illustrate a potential driver of toxin phyla-selectivity within Conus.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6013274PMC
http://dx.doi.org/10.1016/j.peptides.2013.09.004DOI Listing

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