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首页> 外文期刊>Pain. >Voluntary wheel running reveals sex-specific nociceptive factors in murine experimental autoimmune encephalomyelitis
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Voluntary wheel running reveals sex-specific nociceptive factors in murine experimental autoimmune encephalomyelitis

机译:志愿车轮运行揭示了小鼠实验自身免疫脑膜炎术中的性别特异性伤害因素

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摘要

Multiple sclerosis (MS) is an inflammatory, neurodegenerative autoimmune disease associated with sensory and motor dysfunction. Although estimates vary, similar to 50% of patients with MS experience pain during their disease. The mechanisms underlying the development of pain are not fully understood, and no effective treatment for MS-related pain is available. Previous work from our laboratory demonstrated that voluntary exercise (wheel running) can reduce nociceptive behaviours at the disease onset in female mice with experimental autoimmune encephalomyelitis (EAE), an animal model used to study the immunopathogenesis of MS. However, given the established sex differences in the underlying mechanisms of chronic pain and MS, we wanted to investigate whether wheel running would also be effective at preventing nociceptive behaviours in male mice with EAE. C57BL/6 mice of both sexes were given access to running wheels for 1 hour/day until the disease onset, when nociceptive behaviour was assessed using von Frey hairs. Daily running effectively reduced nociceptive behaviour in female mice, but not in male mice. We explored the potential biological mechanisms for these effects and found that the reduction in nociceptive behaviour in female mice was associated with reduced levels of inflammatory cytokines from myelin-reactive T cells as well as reduced dorsal root ganglia excitability as seen by decreased calcium responses. These changes were not seen in male mice. Instead, running increased the levels of inflammatory cytokines and potentiated Ca2+ responses in dorsal root ganglia cells. Our results show that voluntary wheel running has sex-dependent effects on nociceptive behaviour and inflammatory responses in male and female mice with EAE.
机译:多发性硬化症(MS)是与感官和运动功能障碍相关的炎症,神经变性自身免疫疾病。虽然估计变化,但类似于50%的患者在疾病中患有MS体验疼痛的患者。疼痛的发展的机制尚不完全明白,没有有效的MS相关疼痛治疗。我们实验室的以前的工作表明,自愿运动(车轮运行)可以减少雌性小鼠疾病的伤害性行为,具有实验性自身免疫性脑脊髓炎(EAE),用于研究MS免疫病理学的动物模型。然而,鉴于慢性疼痛和MS的潜在机制的既定性差异,我们想调查车轮运行是否有效地防止雄性小鼠的伤害性行为。当使用von frey毛发评估伤害行为时,疾病发作,C57BL / 6小鼠均可进入运行轮1小时/天,直至疾病发作。每日跑步有效地减少了女性小鼠中的伤害性行为,但不是在雄性小鼠中。我们探讨了这些效果的潜在生物学机制,发现雌性小鼠的伤害性行为的减少与髓鞘反应性T细胞的炎性细胞因子的降低相关,以及通过降低的钙响应所见的减少的背根神经节兴奋性。在雄性小鼠中没有看到这些变化。相反,运行增加炎症细胞因子和具有潜能的CA2 +反应在背根神经节细胞中的含量。我们的研究结果表明,志愿车轮对与EAE的男性和女性小鼠的伤害性行为和炎症反应具有性依赖性影响。

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