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Interleukin-1 beta promotes sensory nerve regeneration after sciatic nerve injury.

机译:IL-1β促进坐骨神经损伤后感觉神经的再生。

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摘要

Nerve injury brings about axonal disconnection, and thus axonal extension is one of the important steps for nerve regeneration. Expression of the pro-inflammatory cytokine interleukin-1 beta (IL-1beta) is increased at the early stage of nervous system injury, and previously IL-1beta has been reported to promote neurite outgrowth by inhibiting RhoA activity in vitro. However, the effect of IL-1beta on axonal extension in vivo has not been obvious. Now we examine whether IL-1beta takes advantages on sciatic nerve regeneration. Sciatic nerves of rats are transected and sutured, and IL-1beta or PBS is locally administered for 2 weeks. Although IL-1beta does not influence on motor functional recovery, it promotes sensory functional recovery, estimated by toe pinch test, and increases the number and the area of neurofilament-positive axons at 12 weeks compared with PBS. Moreover IL-1beta, which promotes Schwann cell proliferation and thus may inhibit myelination, does not impair remyelination, estimated by myelin basic protein. These findings suggest that IL-1beta may contribute to sensory nerve regeneration following sciatic nerve injury by promoting axonal extension.
机译:神经损伤导致轴突断开,因此轴突伸展是神经再生的重要步骤之一。在神经系统损伤的早期,促炎性细胞因子白介素1β(IL-1beta)的表达增加,以前有报道称IL-1beta通过在体外抑制RhoA活性来促进神经突生长。但是,IL-1β对体内轴突延伸的作用尚不明显。现在我们检查IL-1β是否在坐骨神经再生中占据优势。切断并缝合大鼠坐骨神经,并局部施用IL-1beta或PBS 2周。尽管IL-1β不影响运动功能恢复,但与PBS相比,它可以促进感觉功能恢复(通过脚趾捏合试验估计),并在12周时增加了神经丝阳性轴突的数量和面积。此外,由髓磷脂碱性蛋白估计,IL-1beta可以促进雪旺细胞增殖并因此可能抑制髓鞘形成,而不会损害髓鞘再生。这些发现表明,IL-1β可能通过促进轴突延伸促进坐骨神经损伤后的感觉神经再生。

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