Objective:To investigate the relationship between the excitotoxicity and serum- inducible kinase(SNK)and spine-associated Rap GTPase-activating protein(SPAR)pathway in primary hippocampal neuron injury induced by glutamate and furthermore,to explore the molecular mechanism of neuroprotection of Zibu Piyin Recipe(滋补脾阴方药,ZBPYR)and the relationship between ZBPYR and the morphological regulation of dendritic spines.Methods:The serum containing ZBPYR was prepared by seropharmacology.Reverse transcription and polymerase chain reaction(RT-PCR)was used to detect the expression of mRNA for SNK,SPAR,postsynaptic density protein 95(PSD-95)and N-methyl-D-aspartate(NMDA)receptor subunits(NR1,NR2A and NR2B)in primary rat hippocampal neuron cultures after pretreatment with 10μmol/L glutamate and ZBPYR serum.Results:ZBPYR serum pretreatment resulted in a significant down-regulation of glutamate-induced SNK mRNA expression(P<0.05).Significant up-regulation was seen on the mRNA expression of SPAR and PSD-95(P<0.05).All these changes were dose-dependent.The mRNA expression of NR1,NR2A and NR2B was down-regulated to different degrees(P<0.05). Conclusion:The mechanism of effect of ZBPYR on glutamate-induced excitotoxicity may be related to the regulation of SNK-SPAR signal pathway.ZBPYR may play a role in protecting and maintaining the normal morphology and structure of dendritic spines,which may be achieved by inhibiting the excessive activation of NMDA receptors. Objective:To investigate the relationship between the excitotoxicity and serum- inducible kinase(SNK) and spine-associated Rap GTPase-activating protein(SPAR)pathway in primary hippocampal neuron injury induced by glutamate and fan,to explore the molecular mechanism of neuroprotection of Zibu Piyin Recipe(ZBPYR) and the relationship between ZBPYR and the morphological regulation of dendritic spines.Methods:The serum containing ZBPYR was prepared by seropharmacology.Reverse transcription and polymerase chain reaction(RT-PCR)was used to detect the Expression of mRNA for SNK,SPAR,postsynaptic density protein 95(PSD-95) and N-methyl-D-aspartate(NMDA) receptor subunits(NR1,NR2A and NR2B)in primary rat hippocampal neuron cultures after pretreatment with 10μmol/L glutamate And ZBPYR serum.Results:ZBPYR serum pretreatment resulted in a significant down-regulation of glutamate-induced SNK mRNA expression(P<0.05).Significant up-regulation was seen on the mRNA expression o f SPAR and PSD-95 (P<0.05). All these changes were dose-dependent. The mRNA expression of NR1, NR2A and NR2B was down-regulated to different degrees (P<0.05). Conclusion: The mechanism of effect of ZBPYR. On glutamate-induced excitotoxicity may be related to the regulation of SNK-SPAR signaling pathway. ZBPYR may play a role in protecting and maintaining the normal morphology and structure of dendritic spines, which may be achieved by inhibiting the excessive activation of NMDA receptors.