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Spinal CX3CL1/CX3CR1 may not directly participate in the development of morphine tolerance in rats

机译:脊髓CX3CL1 / CX3CR1可能不直接参与大鼠吗啡耐受性的发展

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CX3CL1 (fractalkine), the sole member of chemokine CX3C family, is implicated in inflammatory and neuropathic pain via activating its receptor CX3CR1 on neural cells in spinal cord. However, it has not been fully elucidated whether CX3CL1 or CX3CR1 contributes to the development of morphine tolerance. In this study, we found that chronic morphine exposure did not alter the expressions of CX3CL1 and CX3CR1 in spinal cord. And neither exogenous CX3CL1 nor CX3CR1 inhibitor could affect the development of morphine tolerance. The cellular localizations of spinal CX3CL1 and CX3CR1 changed from neuron and microglia, respectively, to all the neural cells during the development of morphine tolerance. A microarray profiling revealed that 15 members of chemokine family excluding CX3CL1 and CX3CR1 were up-regulated in morphine-treated rats. Our study provides evidence that spinal CX3CL1 and CX3CR1 may not be involved in the development of morphine tolerance directly.
机译:趋化因子CX3C家族的唯一成员CX3CL1(fractalkine)通过激活脊髓神经细胞上的受体CX3CR1参与炎症性和神经性疼痛。但是,尚未完全阐明CX3CL1或CX3CR1是否有助于吗啡耐受性的发展。在这项研究中,我们发现慢性吗啡暴露不会改变脊髓中CX3CL1和CX3CR1的表达。外源CX3CL1和CX3CR1抑制剂均不会影响吗啡耐受性的发展。在吗啡耐受性发展过程中,脊髓CX3CL1和CX3CR1的细胞定位分别从神经元和小胶质细胞改变为所有神经细胞。微阵列分析显示,吗啡治疗的大鼠中除CX3CL1和CX3CR1外的15个趋化因子家族成员上调。我们的研究提供证据表明脊髓CX3CL1和CX3CR1可能不直接参与吗啡耐受性的发展。

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