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Pain modality and spinal glia expression by streptozotocin induced diabetic peripheral neuropathy in rats

机译:链脲佐菌素诱导的糖尿病周围神经病变的疼痛形态和脊髓胶质细胞表达

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摘要

Pain symptoms are a common complication of diabetic peripheral neuropathy or an inflammatory condition. In the most experiments, only one or two evident pain modalities are observed at diabetic peripheral neuropathy according to experimental conditions. Following diabetic peripheral neuropathy or inflammation, spinal glial activation may be considered as an important mediator in the development of pain. For this reason, the present study was aimed to address the induction of pain modalities and spinal glial expression after streptozotocin injection as compared with that of zymosan inflammation in the rat. Evaluation of pain behavior by either thermal or mechanical stimuli was performed at 3 weeks or 5 hours after either intravenous streptozotocin or zymosan. Degrees of pain were divided into 4 groups: severe, moderate, mild, and non-pain induction. On the mechanical allodynia test, zymosan evoked predominantly a severe type of pain, whereas streptozotocin induced a weak degree of pain (severe+moderate: 57.1%). Although zymosan did not evoke cold allodynia, streptozotocin evoked stronger pain behavior, compared with zymosan (severe+moderate: 50.0%). On the other hand, the high incidence of thermal hyperalgesia (severe+moderate: 90.0%) and mechanical hyperalgesia (severe+moderate: 85.7%) by streptozotocin was observed, as similar to that of zymosan. In the spinal cord, the increase of microglia and astrocyte was evident by streptozotocin, only microglia was activated by zymosan. Therefore, it is recommended that the selection of mechanical and thermal hyperalgesia is suitable for the evaluation of streptozotocin induced diabetic peripheral neuropathy. Moreover, spinal glial activation may be considered an important factor.
机译:疼痛症状是糖尿病性周围神经病或炎症性疾病的常见并发症。在大多数实验中,根据实验条件,在糖尿病周围神经病变中仅观察到一种或两种明显的疼痛方式。在糖尿病性周围神经病变或炎症之后,脊髓神经胶质激活可能被认为是疼痛发展的重要介质。由于这个原因,本研究的目的是与链脲佐菌素炎症相比,在注射链脲佐菌素后引起疼痛方式和脊髓神经胶质表达。静脉注射链脲佐菌素或酵母聚糖后3周或5小时,通过热刺激或机械刺激评估疼痛行为。疼痛程度分为4组:重度,中度,轻度和非疼痛诱导。在机械性异常性疼痛测试中,酵母聚糖主要引起严重的疼痛,而链脲佐菌素则引起较弱的疼痛(严重+中度:57.1%)。尽管酵母聚糖不引起感冒异常性疼痛,但与酵母聚糖相比,链脲佐菌素可引起更强的疼痛行为(严重+中度:50.0%)。另一方面,与zymosan相似,链脲佐菌素引起的热痛觉过敏(重度+中度:90.0%)和机械性痛觉过敏(重度+中度:85.7%)的发生率很高。在链球菌中,脊髓中小胶质细胞和星形胶质细胞的增加是明显的,酵母聚糖仅激活了小胶质细胞。因此,建议选择机械和热痛觉过敏适合评估链脲佐菌素诱发的糖尿病周围神经病变。此外,脊髓神经胶质激活可能被认为是重要的因素。

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