Intrathecal administration of neuronostatin induces an antinociceptive effect in a mouse visceral pain model

Tingji Shao, Shaobin Yang, Peng Yu
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引用次数: 1

Abstract

Neuronostatin (NST) is a peptide encoded by the somatostatin gene that serves important physiological functions in diverse tissues. Previous studies have shown that intracerebroventricular administration of NST induces antinociceptive effects and hyperalgesic effects as determined by the tail immersion assay and formalin test, respectively. In the present study, we aimed to evaluate the effects of intrathecal (i.t.) injection of NST on nociception in a model of visceral pain, and determine possible mechanisms of action in mice. NST (1, 3, 6, or 12 nmol) was administered to mice, leading to a dose‐dependent antinociceptive effect as determined by the acetic acid‐induced writhing test in mice. NST (1 nmol) also enhanced the antinociceptive effect of morphine (2.5 and 5 μg/kg) in the spine. Naloxone and β‐funaltrexamine hydrochloride significantly antagonized the antinociceptive effect of NST. The expression of G‐protein‐coupled receptor 107 (GPR107) protein and the phosphorylation of PKA at Thr197 were increased after i.t. administration of NST, suggesting that the μ‐opioid receptor and GPR107/PKA signaling pathway are involved in the analgesic response. In conclusion, i.t. injection of NST may potentially be used as a new approach in the mediation of visceral pain.
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在小鼠内脏疼痛模型中鞘内给予神经nostatin诱导抗伤害感受作用
神经生长抑素(NST)是生长抑素基因编码的一种肽,在多种组织中发挥重要的生理功能。先前的研究表明,通过尾部浸泡试验和福尔马林试验分别测定,侧脑室内给予NST可诱导抗伤害感受作用和痛觉过敏作用。在本研究中,我们旨在评估鞘内(i.t.)注射NST对内脏疼痛模型中伤害感受的影响,并确定小鼠的可能作用机制。对小鼠施用NST(1、3、6或12 nmol),通过醋酸诱导的小鼠扭体试验确定其具有剂量依赖性的镇痛作用。NST(1nmol)也增强了吗啡(2.5和5μg/kg)对脊柱的镇痛作用。纳洛酮和盐酸β-呋那沙明显著拮抗NST的镇痛作用。静脉注射NST后,G蛋白偶联受体107(GPR107)蛋白的表达和PKA在Thr197的磷酸化增加,表明μ阿片受体和GPR107/PKA信号通路参与了镇痛反应。总之,腹腔注射NST可能作为一种新的治疗内脏疼痛的方法。
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