A 'conovenomic' Analysis of the Milked Venom from the Mollusk-hunting Cone Snail Conus Textile--the Pharmacological Importance of Post-translational Modifications
Overview
Authors
Affiliations
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.
Research into the Bioengineering of a Novel α-Conotoxin from the Milked Venom of .
Wiere S, Sugai C, Espiritu M, Aurelio V, Reyes C, Yuzon N Int J Mol Sci. 2022; 23(20).
PMID: 36292948 PMC: 9602734. DOI: 10.3390/ijms232012096.
Kasheverov I, Kudryavtsev D, Shelukhina I, Nikolaev G, Utkin Y, Tsetlin V Biomolecules. 2022; 12(2).
PMID: 35204690 PMC: 8961598. DOI: 10.3390/biom12020189.
Ebou A, Koua D, Addablah A, Kakou-Ngazoa S, Dutertre S Biomedicines. 2021; 9(4).
PMID: 33805497 PMC: 8066717. DOI: 10.3390/biomedicines9040344.
Mitochondrial DNA sequence of (Neogastropoda: Conidae).
Chen P, Hsiao S, Chen K, Tseng C, Wu W, Hwang D Mitochondrial DNA B Resour. 2021; 1(1):508-509.
PMID: 33473537 PMC: 7800489. DOI: 10.1080/23802359.2016.1192513.
Structural and Functional Analyses of Cone Snail Toxins.
Duque H, Dias S, Franco O Mar Drugs. 2019; 17(6).
PMID: 31234371 PMC: 6628382. DOI: 10.3390/md17060370.