Biological activity of 8,11-dideoxytetrodotoxin: lethality to mice and the inhibitory activity to cytotoxicity of ouabain and veratridine in mouse neuroblastoma cells, Neuro-2a

Contribution of the C-8 hydroxyl group of tetrodotoxin to its sodium channel blocking activity has never been clearly evaluated. Isobe et al. recently synthesized 8,11-dideoxytetrodotoxin, the first 8-deoxy analog of tetrodotoxin. In this study, the biological activity of this compound was investiga...

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Veröffentlicht in:Toxicon (Oxford) 2003-10, Vol.42 (5), p.557-560
Hauptverfasser: Yotsu-Yamashita, Mari, Urabe, Daisuke, Asai, Masanori, Nishikawa, Toshio, Isobe, Minoru
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Sprache:eng
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Zusammenfassung:Contribution of the C-8 hydroxyl group of tetrodotoxin to its sodium channel blocking activity has never been clearly evaluated. Isobe et al. recently synthesized 8,11-dideoxytetrodotoxin, the first 8-deoxy analog of tetrodotoxin. In this study, the biological activity of this compound was investigated to compare with that of 11-deoxytetrodotoxin. Intraperitoneal injection of 8,11-dideoxytetrodotoxin at the level of 700 μg/kg did not kill a mouse (n=2), indicating that the lethal dose of this compound was more than 70 and 10 folds larger than LD50 of tetrodotoxin and 11-deoxytetrodotoxin, respectively. The inhibitory activity of 8,11-dideoxytetrodotoxin to cytotoxicity of ouabain and veratridine in mouse neuroblastoma cells (Neuro-2a) was also examined. The ED50 for 8,11-dideoxytetrodotoxin was estimated to be 9.3±3.3 μM (n=3), approximately 2000 and 34 folds larger than those of tetrodotoxin (4.6±0.70nM, n=3) and 11-deoxytetrodotoxin (270±74nM, n=4), respectively. These data suggest that the C-8 hydroxyl group of tetrodotoxin is also important for its activity, as well as all the other hydroxyl groups.
ISSN:0041-0101
1879-3150
DOI:10.1016/j.toxicon.2003.08.002