Prostaglandin E(2) potentiates methylmalonate-induced seizures

Methylmalonic acidemias are inherited metabolic disorders characterized by methylmalonate (MMA) accumulation and neurologic dysfunction, including seizures. It is known that metabolic crises in affected patients are precipitated by infections. Although growing evidence supports that inflammation fac...

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Published in:Epilepsia (Copenhagen) 2012-01, Vol.53 (1), p.189-198
Main Authors: Salvadori, Mirian Graciela Silva Stiebbe, Banderó, Cristina Ruedell Reschke, Jesse, Ana Cláudia, Gomes, Anajara Teixeira, Rambo, Leonardo Magno, Bueno, Lívia Maronesi, Bortoluzzi, Vanessa Trindade, Oliveira, Mauro Schneider, Mello, Carlos Fernando
Format: Article
Language:English
Subjects:
Animals
Celecoxib
Cyclooxygenase 2 Inhibitors - pharmacology
Dinoprostone - pharmacology
Disease Models, Animal
Electrodes, Implanted
Electroencephalography
Male
Methylmalonic Acid
Parietal Lobe - drug effects
Parietal Lobe - physiopathology
Pyrazoles - pharmacology
Rats
Rats, Wistar
Seizures - drug therapy
Seizures - metabolism
Seizures - physiopathology
Sulfonamides - pharmacology
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Summary:Methylmalonic acidemias are inherited metabolic disorders characterized by methylmalonate (MMA) accumulation and neurologic dysfunction, including seizures. It is known that metabolic crises in affected patients are precipitated by infections. Although growing evidence supports that inflammation facilitates seizures, it is not known whether inflammatory mediators facilitate MMA-induced seizures. Therefore, in this study we investigate the involvement of cyclooxygenase-2 (COX-2) and prostaglandin E(2) (PGE(2)) in MMA-induced seizures. Adult male Wistar rats were implanted with electrodes over the parietal cortex for electroencephalography (EEG) recording and a cannula in the right lateral ventricle. Animals were injected with PGE(2) (100 ng/2 μl, i.c.v.) or phosphate-buffered saline (PBS) (2 μl, i.c.v.), 15 min before MMA (2.5 μmol/2.5 μl, i.c.v.) or NaCl (2.5 μmol/2.5 μl, i.c.v.). The anticonvulsant effect of celecoxib (0.2; 2 or 20 mg/kg, p.o., 60 min before MMA) on MMA-induced seizures, and whether PGE(2) (10 or 100 ng/2 μl, i.c.v.) prevented the anticonvulsant effect of celecoxib (2 mg/kg, p.o.) were also investigated. PGE(2) decreased the latency to MMA-induced jerks and generalized seizures, and increased the amplitude of generalized seizure EEG recordings. The selective COX-2 inhibitor celecoxib at the dose 2 mg/kg, but not at the dose 20 mg/kg, completely prevented MMA-induced seizures. The protective effect of celecoxib (2 mg/kg) against MMA-induced seizures was prevented by PGE(2). These results support a role for PGE(2) in the seizures elicited by MMA, which is in agreement with the view that infections may precipitate and exacerbate neurologic dysfunction in patients with MMA acidemic.
ISSN:1528-1167
DOI:10.1111/j.1528-1167.2011.03326.x