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Antinociceptive action of a p38α MAPK inhibitor, SD-282, in a diabetic neuropathy model
66
Citations
34
References
2004
Year
Pain DisordersPain MedicineNeuropathic PainP38α Mapk InhibitorMolecular PharmacologyMechanical AllodyniaDiabetic NeuropathyPain ManagementNeurologyP38alpha Mapk InhibitorsHealth SciencesPharmacological AgentNeuropharmacologyPharmacologyAntinociceptive ActionP38alpha Mapk InhibitorDiabetic Neuropathy ModelPain ResearchPhysiologyDiabetesNeurosciencePain MechanismMedicineDrug Discovery
Diabetes can induce a bewildering list of sensory changes, including alteration in pain sensitivity. Painful diabetic neuropathy is refractory to most common analgesics. This study examined the effect of a p38alpha MAPK inhibitor, SD-282, on mechanical allodynia, thermal hyperalgesia, and formalin-evoked nociception in streptozotocin-induced diabetic rats. Four-week diabetic rats exhibited mechanical allodynia, decreased mechanical thresholds, and C- and Adelta-fiber mediated thermal hyperalgesia. Mechanical and thermal responses were measured in diabetic rats following acute and repeated intraperitoneal administration of vehicle, 15 or 45 mg/kg SD-282. Mechanical allodynia was reversed by acute and repeated administration of 15 and 45 mg/kg SD-282. Repeated administration of 15 or 45 mg/kg SD-282 prevented the exacerbation of C-, but not Adelta-fiber, mediated thermal hyperalgesia. Repeated administration of 45 mg/kg SD-282 attenuated flinching behaviors during the quiescent period and the second phase of the formalin response in diabetic rats. Acute and repeated administration of 15 or 45 mg/kg SD-282 had no effect on mechanical, thermal or formalin responses in age-matched control rats. These results indicate a potential therapeutic value of p38alpha MAPK inhibitors in the treatment of aberrant pain sensitivity produced by diabetes.
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