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Effects of transgene-mediated endomorphin-2 in inflammatory pain

机译:转基因介导的内啡肽2在炎性疼痛中的作用

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摘要

We examined the analgesic properties of endomorphin-2 expressed in DRG neurons transduced with a non-replicating herpes simplex virus (HSV)-based vector containing a synthetic endomorphin-2 gene construct. HSV-mediated endomorphin-2 expression reduced nocisponsive behaviors in response to mechanical and thermal stimuli after injection of complete Freund’s adjuvant (CFA) into the paw, and reduced peripheral inflammation measured by paw swelling after injection of CFA. The analgesic effect of the vector was blocked by either intraperitoneal or intrathecal administration of naloxone methiodide, blocking peripheral and central μ opioid receptors, respectively. Endomorphin-2 vector injection also reduced spontaneous pain-related behaviors in the delayed phase of the formalin test and in both CFA and formalin models suppressed spinal c-fos expression. The magnitude of the vector-mediated analgesic effect on the delayed phase of the formalin test was similar in naïve animals and in animals with opiate tolerance induced by twice daily treatment with morphine, suggesting that there was no cross-tolerance between vector-mediated endomorphin-2 and morphine. These results suggest that transgene-mediated expression of endomorphin-2 in transduced DRG neurons in vivo acts both peripherally and centrally through mu opioid receptors to reduce pain perception.
机译:我们检查了DRG神经元中表达的endomorphin-2的镇痛特性,该DRG神经元通过含有合成endomorphin-2基因构建体的非复制性单纯疱疹病毒(HSV)为基础的载体转导。在将完全弗氏佐剂(CFA)注射到爪中后,HSV介导的endomorphin-2表达减少了对机械和热刺激的无反应行为,并在注射CFA后通过爪肿胀减少了周围炎症。通过腹膜内或鞘内施用纳洛酮甲硫醇阻断载体的镇痛作用,分别阻断外周和中枢μ阿片受体。 Endomorphin-2载体注射在福尔马林测试的延迟阶段以及CFA和福尔马林模型中均抑制了脊髓c-fos表达,从而减少了自发性疼痛相关行为。媒介动物对福尔马林测试延迟期的镇痛作用的程度在纯朴的动物和通过每天两次吗啡治疗诱导的鸦片耐受的动物中相似,这表明媒介物介导的吗啡-内啡肽之间没有交叉耐受性。 2,吗啡。这些结果表明,转导的DRG神经元体内转基因介导的endomorphin-2的表达通过μ阿片受体在外周和中央起作用,以减轻疼痛感。

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