Increased phosphorylation of cyclic AMP response element binding protein(CREB)in the dorsal root gan

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Objective To investigate whether chronic constriction injury(CCI)of the sciatic nerve of rats could produce alterations in the phosphorylation of cyclic AMP response element binding(CREB)protein in dorsal root ganglia(DRG)and superficial dorsal horn neurons of the spinal cord.Methods Chronic constriction injury(CCI)of the sciatic nerve was employed as a model of neuropathic pain.Thirty-two Sprague-Dawley rats were randomly divided into Na⒍ve,Sham,CCI2w(received CCI for2weeks)and CCI4w(received CCI for4weeks)groups.Hind pawwithdrawal threshold to mechanical stimuli and withdrawal latency to thermal stimuli were used to determine the mechanical and thermal hyperalgesia.Then all the rats were deeply anesthetized and perfused intracardially with paraformaldehyde.The fixed L 4-5 spinal cord and the L 5 DRG ipsilateral to CCI were harvested for fixation.The pCREB-immunoreactive(pCREB-IR)cells in both DRG and superficial dorsal horn neurons were quantified for analysis using immunohistochemistry methods.Results On the14th day after sciatic nerve injury,all the rats exhibited significant mechanical and thermal hyperalgesia.The mechanical withdrawal thresholds to von Frey filament from CCI2w group decreased significantly compared to both baseline values and those of Sham group(P<0.01);Thermal withdwal latencies from CCI2w group decreased significantly compared to both baseline values and those of Sham group(P<0.01).Some rats from Sham group also showed mechanical hyperalgesia compared to both baseline values and those of Na⒍ve group(P<0.01).28days after CCI,both mechanical and thermal hypersensitivity were significantly alleviated,with no statistical significance compared to those of Sham group.On the14th day after CCI,the number of pCREB-IR cells significantly increased in ipsilateral L 5 DRGs and superficial dorsal horns(P<0.01)compared to Sham group.The number of phosphorylated CREB-IR cells in the ipsilateral DRGs from Sham group also increased compared to that of Naive rats(P<0.05).There were no significant statistical differences of numbers of CREB-IR neuron between Sham group and CCI4wgroup.Conclusion CCI increases CREB phosphorylation both in DRG and superficial dorsal horn neurons of the lumbar spinal cord,and may be one of the key molecular mechanisms of central and peripheral sensitization following peripheral nerve injury. Objective To investigate whether chronic constriction injury (CCI) of the sciatic nerve of rats could produce alterations in the phosphorylation of cyclic AMP response element binding (CREB) protein in dorsal root ganglia (DRG) and superficial dorsal horn neurons of the spinal cord. Methods Chronic constriction injury (CCI) of the sciatic nerve was employed as a model of neuropathic pain. Three-two Sprague-Dawley rats were differentiated into Na⒍ve, Sham, CCI2w (received CCI for2weeks) and CCI4w (received CCI for4weeks) pawwithdrawal threshold to mechanical stimuli and withdrawal latency to thermal stimuli were used to determine the mechanical and thermal hyperalgesia. All of the rats were deeply anesthetized and perfused intracardially with paraformaldehyde. The fixed L 4-5 spinal cord and the L 5 DRG ipsilateral to CCI were harvested for fixation. The pCREB-immunoreactive (pCREB-IR) cells in both DRG and superficial dorsal horn neurons were quantified for analysis using immunohistochem istry methods. Results on the 14th day after sciatic nerve injury, all the rats exhibiting significant mechanical and thermal hyperalgesia. mechanical drop thresholds to vonths. ; Thermal withdwaltenten from CCI2w group was significantly decreased to both baseline values ​​and those of Sham group (P <0.01) .Some rats from Sham group also showed mechanical hyperalgesia compared to both baseline values ​​and those of Naheve group (P <0.01). 28 days after CCI, both mechanical and thermal hypersensitivity were significantly alleviated, with no statistical significance compared to those of Sham group. On the 14th day after CCI, the number of pCREB-IR cells significantly increased in ipsilateral L 5 DRGs and superficial dorsal horns (P <0.01) compared to Sham group. The number of phosphorylated CREB-IR cells in the ipsilateral DRGs from Sham group also increased compared to that of Na iverats (P <0.05). There were no significant statistical differences of numbers of CREB-IR neurons between Sham group and CCI4wgroup. Confocal CCI increases CREB phosphorylation both in DRG and superficial dorsal horn neurons of the lumbar spinal cord, and may be one of the key molecular mechanisms of central and peripheral sensitization following peripheral nerve injury.
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