Biochemical and physiological characterization of a new Na(+)-channel specific peptide from the venom of the Argentinean scorpion Tityus trivittatus

Coronas, Fredy I. V.; Diego-Garcia, Elia; Restano-Cassulini, Rita; de Roodt, Adolfo Rafael; Possani, Lourival D.

doi:10.1016/j.peptides.2014.05.002

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Biochemical and physiological characterization of a new Na(+)-channel specific peptide from the venom of the Argentinean scorpion Tityus trivittatus
Citation	Coronas FIV, Diego-Garcia E, Restano-Cassulini R, de Roodt AR, Possani LD. Peptides 2014; 68: 11-16.
Affiliation	Departamento de Medicina Molecular y Bioprocesos, Instituto de Biotecnología, Universidad Nacional Autónoma de México, Mexico. Electronic address: possani@ibt.unam.mx.
Copyright	(Copyright © 2014, Elsevier Publishing)
DOI	10.1016/j.peptides.2014.05.002
PMID	24862827
Abstract	A new peptide with 61 amino acids cross-linked by 4 disulfide bridges, with molecular weight of 6938.12Da, and an amidated C-terminal amino acid residue was purified and characterized. The primary structure was obtained by direct Edman degradation and sequencing its gene. The peptide is lethal to mammals and was shown to be similar (95% identity) to toxin Ts1 (gamma toxin) from the Brazilian scorpion Tityus serrulatus; it was named Tt1g (from T. trivittatus toxin 1 gamma-like). Tt1g was assayed on several sub-types of Na(+)-channels showing displacement of the currents to more negative voltages, being the hNav1.3 the most affected channel. This toxin displays characteristics typical to the β-type sodium scorpion toxins. Lethality tests and physiological assays indicate that this peptide is probably the most important toxic component of this species of scorpion, known for causing human fatalities in the South American continent. Language: en