首页> 外文期刊>Osteoarthritis and cartilage >Surgically induced osteoarthritis in the rat results in the development of both osteoarthritis-like joint pain and secondary hyperalgesia.
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Surgically induced osteoarthritis in the rat results in the development of both osteoarthritis-like joint pain and secondary hyperalgesia.

机译:大鼠手术诱发的骨关节炎导致骨关节炎样关节疼痛和继发性痛觉过敏的发展。

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OBJECTIVE: In the present study, we sought to develop/characterize the pain profile of a rat model of surgically induced osteoarthritis (OA). METHODS: OA was surgically induced in male Lewis rats (200-225 g) by transection of the medial collateral ligament and medial meniscus of the femoro-tibial joint. In order to characterize the pain profile, animals were assessed for a change in hind paw weight distribution (HPWD), development of mechanical allodynia, and the presence of thermal and mechanical hyperalgesia. Rofecoxib and gabapentin were examined for their ability to decrease change in weight distribution and tactile allodynia. RESULTS: Transection of the medial collateral ligament and medial meniscus of male Lewis rats resulted in rapid (<3 days) changes in hind paw weight bearing and the development of tactile allodynia (secondary hyperalgesia). There was, however, no appreciable effect on thermal hyperalgesia or mechanical hyperalgesia. Treatment with a single dose of rofecoxib (10 mg/kg, PO, day21 post surgery) or gabapentin (100mg/kg, PO, day 21 post surgery) significantly attenuated the change in HPWD, however, only gabapentin significantly decreased tactile allodynia. CONCLUSION: The rat medial meniscal tear (MMT) model mimics both nociceptive and neuropathic OA pain and is responsive to both a selective cylooxygenase-2 (COX-2) inhibitor commonly utilized for OA pain (rofecoxib) and a widely prescribed drug for neuropathic pain (gabapentin). The rat MMT model may therefore represent a predictive tool for the development of pharmacologic interventions for the treatment of the symptoms associated with OA.
机译:目的:在本研究中,我们试图开发/表征外科手术性骨关节炎(OA)大鼠模型的疼痛特征。方法:手术切除雄性Lewis大鼠(200-225 g),方法是将股副胫骨内侧副韧带和内侧半月板横切。为了表征疼痛状况,评估动​​物后爪重量分布(HPWD)的变化,机械性异常性疼痛的发展以及热痛觉过敏和机械痛觉过敏的存在。检查了罗非昔布和加巴喷丁减轻体重分布变化和触觉异常性疼痛的能力。结果:雄性刘易斯大鼠的内侧副韧带和内侧半月板的横断导致后足负重快速变化(<3天),并产生触觉性异常性疼痛(继发性痛觉过敏)。但是,对热痛觉过敏或机械性痛觉过敏没有明显的作用。单独使用罗非考昔(10 mg / kg,PO,术后21天)或加巴喷丁(100mg / kg,PO,术后21天)治疗可显着减轻HPWD的变化,但是,只有加巴喷丁可显着降低触觉异常性疼痛。结论:大鼠半月板内侧撕裂(MMT)模型可模拟伤害性和神经性OA疼痛,并且对通常用于OA疼痛的选择性cylooxygenase-2(COX-2)抑制剂(rofecoxib)和广泛用于神经性疼痛的处方药均具有响应(加巴喷丁)。因此,大鼠MMT模型可能代表了开发用于治疗与OA相关的症状的药物干预措施的预测工具。

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