糖尿病中脊髓介导性痛觉过敏的发病机制。
Pathogenesis of spinally mediated hyperalgesia in diabetes.
作者信息
Ramos Khara M, Jiang Yun, Svensson Camilla I, Calcutt Nigel A
机构信息
Department of Neurosciences, University of California, San Diego, California 92093-0612, USA.
出版信息
Diabetes. 2007 Jun;56(6):1569-76. doi: 10.2337/db06-1269. Epub 2007 Feb 7.
Hyperalgesia to noxious stimuli is accompanied by increased spinal cyclooxygenase (COX)-2 protein in diabetic rats. The present studies were initiated to establish causality between increased spinal COX-2 activity and hyperalgesia during diabetes and to assess the potential involvement of polyol pathway activity in the pathogenesis of spinally mediated hyperalgesia. Rats with 1, 2, or 4 weeks of streptozotocin-induced diabetes exhibited significantly increased levels of spinal COX-2 protein and activity, along with exaggerated paw flinching in response to 0.5% paw formalin injection. Increased flinching of diabetic rats was attenuated by intrathecal pretreatment with a selective COX-2 inhibitor immediately before formalin injection, confirming the involvement of COX-2 activity in diabetic hyperalgesia. Chronic treatment with insulin or ICI222155, an aldose reductase inhibitor (ARI) previously shown to prevent spinal polyol accumulation and formalin-evoked hyperalgesia in diabetic rats, prevented elevated spinal COX-2 protein and activity in diabetic rats. In contrast, the ARI IDD676 had no effect on spinal polyol accumulation, elevated spinal COX-2, or hyperalgesia to paw formalin injection. In the spinal cord, aldose reductase immunoreactivity was present solely in oligodendrocytes, which also contained COX-2 immunoreactivity. Polyol pathway flux in spinal oligodendrocytes provides a pathogenic mechanism linking hyperglycemia to hyperalgesia in diabetic rats.
在糖尿病大鼠中,对伤害性刺激的痛觉过敏伴随着脊髓环氧化酶(COX)-2蛋白增加。开展本研究是为了确定糖尿病期间脊髓COX-2活性增加与痛觉过敏之间的因果关系,并评估多元醇途径活性在脊髓介导的痛觉过敏发病机制中的潜在作用。链脲佐菌素诱导糖尿病1、2或4周的大鼠,脊髓COX-2蛋白水平和活性显著增加,同时对0.5%爪部福尔马林注射的爪部退缩反应增强。在福尔马林注射前立即鞘内注射选择性COX-2抑制剂预处理,可减轻糖尿病大鼠增强的退缩反应,证实COX-2活性参与了糖尿病性痛觉过敏。胰岛素或ICI222155(一种醛糖还原酶抑制剂(ARI),先前已证明可预防糖尿病大鼠脊髓多元醇蓄积和福尔马林诱发的痛觉过敏)长期治疗,可预防糖尿病大鼠脊髓COX-2蛋白和活性升高。相比之下,ARI IDD676对脊髓多元醇蓄积、脊髓COX-2升高或爪部福尔马林注射引起的痛觉过敏均无影响。在脊髓中,醛糖还原酶免疫反应仅存在于少突胶质细胞中,少突胶质细胞也含有COX-2免疫反应。脊髓少突胶质细胞中的多元醇途径通量提供了一种将高血糖与糖尿病大鼠痛觉过敏联系起来的致病机制。
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