Ｏｂｊｅｃｔｉｖｅ　To investigate the effects of intrathecal injection of Neuropeptide S and Gabapentin on pain behavior and anxiety behavior in rats with neuropathic pain， and to explore the possible mechanisms of of N-methyl-D-aspartic acid（NMDA） receptor 1.　Methods　Seventy-two male Sprague-Dawley （SD） rats， which were successfully deployed intrathecal catheter， were randomly divided into six groups（n=12）， including sham group， CCI group， neuropeptide S low-dose group（NPSl group）， neuropeptide S high-dose group （NPSh group）， gabapentin low dose group （Gbl group） and gabapentin high dose group（Gbh group）. Pain-related behaviors， depression-related behaviors， and expression of NMDA receptor1 in the dorsal horn of the spinal cord were measured at 14 d after 7 d via intrathecal injection.　Results　Compared with the sham group， the rats suffering CCI demonstrated significant pain and anxiety behavior（P<0.01）. High dose NPS and each dose gabapentin（but not low dose NPS） can significantly reduce mechanical withdrawal threshold（MWT） ［（2.7±1.3） g vs （4.5±1.7），（5.4±1.0），（8.1±3.6） g］and thermal hyperalgesia foot withdrawal lantency（FWL） ［（3.9±0.6） s vs （5.8±1.5），（6.3±1.2），（7.6±1.6） s］compared with CCI group（P<0.05）.In the EPM test， compared with CCI group， only high dose NPS significantly extended numbers entries into the open arms（6.3±1.6 vs 2.9±1.5）（P<0.05） and time spent in the open arms（22.4±4.3）% vs （10.9±2.7）%（P<0.05）. In the open field test， each dose NPS and gabapentin added the proportion of central Zone cross（P<0.05） and time spent（P<0.05）. Immunofluorescence and western blot experiments showed that， regardless of the level measurement group， both drugs can suppress the increase NR1 receptor expression in the dorsal horn of the spinal cord， and has a statistical significance.　Conclusions　Neuropeptide S and gabapentin dose-dependent pain and anxiety behavior reversal CCI rats， which may be related NMDA receptor pathway.