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PKMζ is essential for spinal plasticity underlying the maintenance of persistent pain

机译:PKMζ对于维持持续性疼痛的脊柱可塑性至关重要

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Background Chronic pain occurs when normally protective acute pain becomes pathologically persistent. We examined here whether an isoform of protein kinase C (PKC), PKMζ, that underlies long-term memory storage in various brain regions, also sustains nociceptive plasticity in spinal cord dorsal horn (SCDH) mediating persistent pain. Results Cutaneous injury or spinal stimulation produced persistent increases of PKMζ, but not other atypical PKCs in SCDH. Inhibiting spinal PKMζ, but not full-length PKCs, reversed plasticity-dependent persistent painful responses to hind paw formalin and secondary mechanical hypersensitivity and SCDH neuron sensitization after hind paw capsaicin, without affecting peripheral sensitization-dependent primary heat hypersensitivity after hind paw capsaicin. Inhibiting spinal PKMζ, but not full-length PKCs, also reversed mechanical hypersensitivity in the rat hind paw induced by spinal stimulation with intrathecal dihydroxyphenylglycine. Spinal PKMζ inhibition also alleviated allodynia 3 weeks after ischemic injury in rats with chronic post-ischemia pain (CPIP), at a point when allodynia depends on spinal changes. In contrast, spinal PKMζ inhibition did not affect allodynia in rats with chronic contriction injury (CCI) of the sciatic nerve, or CPIP rats early after ischemic injury, when allodynia depends on ongoing peripheral inputs. Conclusions These results suggest spinal PKMζ is essential for the maintenance of persistent pain by sustaining spinal nociceptive plasticity.
机译:背景技术当正常的急性疼痛在病理上持续存在时,就会发生慢性疼痛。我们在这里检查了蛋白激酶C(PKC)的同工型PKMζ是否是在各个大脑区域中长期记忆存储的基础,是否还在介导持续性疼痛的脊髓背角(SCDH)中维持了伤害性可塑性。结果皮肤损伤或脊柱刺激导致SCDH中PKMζ持续增加,但其他非典型PKC却没有。抑制脊髓PKMζ,但不抑制全长PKCs,可逆转辣椒素后对后爪福尔马林的可塑性依赖性持久性疼痛反应和继发性机械性超敏反应以及SCDH神经元敏化,而不会影响后爪辣椒素后外周致敏依赖性的初级热超敏反应。抑制脊髓PKMζ,但不抑制全长PKC,也可以逆转鞘内注射二羟基苯基甘氨酸刺激大鼠后足引起的机械超敏反应。在患有慢性缺血后疼痛(CPIP)的大鼠中,脊髓PKMζ抑制也可减轻缺血性损伤后3周的异常性疼痛,此时异常性疼痛取决于脊髓的变化。相反,当异常性疼痛取决于持续的周围输入时,脊髓PKMζ的抑制作用不会影响坐骨神经慢性轻度损伤(CCI)大鼠或缺血性损伤后早期的CPIP大鼠的异常性疼痛。结论这些结果表明,脊柱PKMζ通过维持脊柱伤害感受性可塑性对于维持持续性疼痛至关重要。

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