Purpose : This study was performed to elucidate that status epilepticus (SE) induces longterm neuronal damages in an immature brain and to evaluate that topiramate (TPM) has a protective effect. Metho ds : We investigated the changes in a subtype expression of glutamate and gammaamino butyric acid (GABA) receptors, and the structural integrity due to cell losses in the mouse pup hippocampus after SE using an immunoblot and confocal microscopy. Resu lts : SE induced significant cell losses with structural changes in the hippocampus 1 month later. SE up-regulated the glutamate receptor1 (GluR1) expression with an increased ratio of GluR1 to glutamate recptor2(GluR2), leading to the formation of Ca²+ permeable α-amino-3-hydroxy-5-methyl-4-isoxazoleepropionic acid (AMPA) receptors for the enhanced neurotoxicity. TPM prevented the SE-induced GluR1 expression. The expression of GABAA receptors was highly increased 1 month after SE, whereas that of GABAB receptors was not changed. The TPM treatment attenuated SE-induced upregulation of GABAA receptors. SE induced significant cell losses and disruption of structural integrity in the hippocampus CA1 and CA3 regions, but the TPM treatment for 1 month in developing brains reduced the SEinduced hippocampal damage. Conclusio n : TPM has a neuroprotective action, which might be mediated by the modulation of GluR1 and GABAA receptors.