1. Primary structure, behavioral and electroencephalographic effects of an epileptogenic peptide from the sea anemone Bunodosoma cangicum
- Author
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Cunha, Ricardo B., Santana, Alfredo N.C., Amaral, Patrícia C., Carvalho, Maria D.F., Carvalho, Doris M.F., Cavalheiro, Esper A., Maigret, Bernard, Ricart, Carlos A.O., Cardi, Bruno A., Sousa, Marcelo V., and Carvalho, Krishnamurti M.
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ELECTROENCEPHALOGRAPHY , *DIAGNOSIS of brain diseases , *PEPTIDES , *SODIUM channels - Abstract
Abstract: The primary structure of cangitoxin (CGX), a 4958Da peptide from the sea anemone Bunodosoma cangicum, was determined: GVACRCDSDGPTVRGNSLSGTLWLTGGCPSGWHNCRGSGPFIGYCCKK. CGX contains all the 11 residues that are conserved and the 5 that are conservatively substituted within or between the type 1 and type 2 sequences of sea anemone peptides with specific action on voltage-sensitive sodium channels. Furthermore, it also has 6 identities (Asp9, Arg14, Asn16, Leu18, Trp33 and Lys48) and 1 homology (Arg36) in the 8 residues of the pharmacophore of the sea anemone ApB which are essential for interaction with mammalian sodium channels. The intrahippocampal injection of CGX induces several sequential behavioral alterations—episodes of akinesia alternating with facial automatisms and head tremor, salivation, rearing, jumping, barrel-rolling, wet dog shakes and forelimb clonic movements–and the electroencephalography analysis shows that they were followed by important seizure periods that gradually evolved to status epilepticus that lasted 8–12h, similar to that observed in the acute phase of the pilocarpine model of epilepsy. These results suggest that CGX may be an important tool to develop a new experimental model of status epilepticus which may contribute to understanding the etiology of epilepsy and to test the effects of new antiepileptic drugs. [Copyright &y& Elsevier]
- Published
- 2005
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