RESUMO
The central nervous system (CNS) depressant and anticonvulsant activities of Citrus limon (L.) Osbeck, Rutaceae, essential oil (EO) were investigated in animal models. The EO (50, 100 and 150 mg/kg) injected by oral route (p.o.) in mice caused a significant decrease in the motor activity of animals when compared with the control group, up to thirty days after the administration and the dose of 150 mg/kg significantly reduced the remaining time of the animals on the Rota-rod apparatus. Additionally, C. limon essential oil was also capable to promote an increase of latency for development of convulsions induced by pentylenetetrazole (PTZ). The administration of FLU (10 mg/kg, i.p.), GABA A-benzodiazepine (GABA-BZD) receptor antagonist, antagonized the effect of C. limon essential oil at higher dose. This C. limon essential oil was also capable to promote an increase of latency for development of convulsions induced by picrotoxin (PIC) at higher dose. In the same way, the anticonvulsant effect of the EO was affected by pretreatment with flumazenil, a selective antagonist of benzodiazepine site of GABA A receptor. These results suggest a possible CNS depressant and anticonvulsant activities in mice that needs further investigation.
RESUMO
The seizures can produce neuronal damage in several brain structures. The aim of this study was to investigate the potential neuroprotective effect of essential oil of Citrus limon (EOCL) on the histopathological changes observed in the hippocampus and striatum of mice after seizures induced by pilocarpine. Adult Swiss mice were 2 months old. The animals were divided into four groups. The first group was treated with 0.05 percent Tween 80 (control group) and the second with pilocarpine (400 mg/kg group P400). The third and fourth group were treated with EOCL (150 mg/kg) and 30 min after received P400 (P400 +/- EOCL group) or 0.05 percent Tween 80, respectively. After treatment, all groups were observed for 24 h, then sacrificed and their brains removed for histopathological analysis. The group P400, presented with seizures that progressed to status epilepticus in 75 percent of animals. Pretreatment with OECL produced a 25 percent reduction in this index. Groups P400 and P400 + EOCL showed 83.33 percent and 25 percent of animals with brain damage in the hippocampus, respectively. In the striatum of group P400 was a compromise of 75 percent. In turn, in the striatal region of group EOCL P400 + was seen a decrease of 58.34 percent in this neuronal damage. The seizures induced by pilocarpine are installed by the cholinergic system and produce brain damage. According to our results we suggest that the EOCL may modulate epileptogenesis and promote neuroprotective effects during the seizures in the model investigated.
As convulsões podem produzir danos neuronais em diversas estruturas cerebrais. O objetivo desse estudo foi investigar o potencial efeito neuroprotetor do óleo essencial de Citrus limon (OECL) nas alterações histopatológicas observadas no hipocampo e corpo estriado de camundongos após convulsão induzida por pilocarpina. Foram utilizados camundongos Swiss adultos com 2 meses de idade. Os animais foram divididos em 4 grupos. O primeiro grupo foi tratado com Tween 80 0,05 por cento (grupo controle) e o segundo com pilocarpina (400 mg/kg, grupo P400). Já o terceiro e quarto grupo foram tratados com OECL (150 mg/kg), e 30 min depois receberam P400 (grupo OECL + P400) ou Tween 80 0,05 por cento 0.9 por cento (grupo OECL), respectivamente. Após os tratamentos, todos os grupos foram observados durante 24 h e em seguida sacrificados e seus cérebros removidos para as análises histopatológicas. O grupo P400, apresentou convulsões que progrediram para o estado epiléptico em 75 por cento dos animais. O pré-tratamento com OECL produziu uma redução de 25 por cento nesse índice. Os grupos P400 e OECL + P400 apresentaram 83,33 por cento e 25 por cento de animais com lesão cerebral no hipocampo, respectivamente. No corpo estriado dos animais do grupo P400 houve um comprometimento de 75 por cento. Por sua vez, na região estriatal dos animais do grupo OECL + P400 foi visto uma redução de 58,34 por cento nesse comprometimento. As convulsões induzidas pela pilocarpina são instaladas pelo sistema colinérgico e produzem dano cerebral. De acordo com nossos resultados podemos sugerir que o OECL pode modular a epileptogênese e promover ação neuroprotetora durante as convulsões no modelo investigado.