Protein kinase inhibitor as a potential candidate for epilepsy treatment

Summary Purpose:  Effects of the “VID‐82925” kinase inhibitor molecule were investigated both during the developing phase as well as during the stable phase of the focus with spontaneous recurrent seizures using the 4‐AP‐induced in vivo epilepsy model in anesthetized rats. Methods:  In electrophysio...

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Veröffentlicht in:Epilepsia (Copenhagen) 2011-03, Vol.52 (3), p.579-588
Hauptverfasser: Gajda, Zita, Török, Rita, Horváth, Zoltán, Szántai‐Kis, Csaba, Őrfi, László, Kéri, György, Szente, Magdolna
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Sprache:eng
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Zusammenfassung:Summary Purpose:  Effects of the “VID‐82925” kinase inhibitor molecule were investigated both during the developing phase as well as during the stable phase of the focus with spontaneous recurrent seizures using the 4‐AP‐induced in vivo epilepsy model in anesthetized rats. Methods:  In electrophysiologic experiments, VID‐82925 (0.85 mg/kg) was injected intravenously either before the induction (pretreatment) or after the development of the stable focus (treatment). Reference drugs carbamazepine (4.8 mg/kg) and levetiracetam (50 mg/kg) were employed using the same experimental paradigm. The antiepileptic effect of VID‐82925 was also compared to those of the broad‐spectrum gap junction channel blocker carbenoxolone (10 mm). Key Findings:  Pretreatment with VID‐82925 revealed an antiepileptogenic effect as it suppressed significantly the manifestation of the epileptiform activity not only during the developing phase, but also for a considerable long period during the stable phase of the focus. The current data do not allow us to differentiate an antiictal treatment effect from an antiepileptogenic effect of the compound during the stable phase of the focus. Treatment with VID‐82925 was also effective against ictogenesis during the stable phase of the focus. Pretreatment with levetiracetam failed to exert any antiepileptogenic effect. The antiepileptic effects of VID‐82925 and of the reference drugs on the epileptiform activity of the stable focus were comparable in intensity; however, the effect of VID‐82925 was 2–3 times longer. The effects of VID‐82925 and of carbenoxolone overlapped one another to some extent, suggesting that VID‐82925 may exert its effects at least partially through blocking of gap junctional communication. Significance:  Our results indicate that inhibition of protein kinases may also provide an effective strategy for the development of a drug that is not only antiepileptic but also depresses the course of epileptogenesis.
ISSN:0013-9580
1528-1167
DOI:10.1111/j.1528-1167.2011.02979.x