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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >gp130 cytokines, leukemia inhibitory factor and interleukin-6, induce neuropeptide expression in intact adult rat sensory neurons in vivo: time-course, specificity and comparison with sciatic nerve axotomy.
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gp130 cytokines, leukemia inhibitory factor and interleukin-6, induce neuropeptide expression in intact adult rat sensory neurons in vivo: time-course, specificity and comparison with sciatic nerve axotomy.

机译:gp130细胞因子,白血病抑制因子和白介素6在体内完整的成年大鼠感觉神经元中诱导神经肽表达:时程,特异性以及与坐骨神经轴突切开术的比较。

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摘要

The gp130 cytokines leukemia inhibitory factor and interleukin-6 are neuroactive cytokines associated with peripheral nerve injury. Here we show that exogenous administration of these factors selectively regulates neuropeptide phenotype in intact sensory neurons in a manner consistent with their role as injury-induced factors. Intraneural injection of leukemia inhibitory factor into the intact sciatic nerve of adult rats induces a significant increase in the percentage of neuronal profiles immunoreactive for galanin in the L4 and L5 dorsal root ganglia without altering the percentage profiles immunoreactive for vasoactive intestinal polypeptide or neuropeptide Y. Galanin-immunoreactivity was predominantly confined to those neurons which retrogradely transported and accumulated leukemia inhibitory factor. The up-regulation of galanin-immunoreactivity observed in L4 and L5 dorsal root ganglia following unilateral axotomy of the sciatic nerve was significantly reduced following continuous treatment for two weeks with a monoclonal antibody against the gp130 receptor motif. Intraneural injection of interleukin-6 into the intact sciatic nerve also significantly increased the percentage of neuronal profiles which displayed galanin-immunoreactivity but not vasoactive intestinal polypeptide or neuropeptide Y-immunoreactivity. Our results indicate that cytokines which interact with the gp130 receptor at the site of peripheral nerve injury contribute to the cell body response to axotomy. Changes in the levels of such cytokines however are insufficient to account for the complete repertoire of neuropeptide phenotypic changes associated with peripheral nerve injury.
机译:gp130细胞因子白血病抑制因子和白细胞介素6是与周围神经损伤相关的神经活性细胞因子。在这里,我们显示这些因子的外源性给药选择性地调节完整的感觉神经元中的神经肽表型,其方式与它们作为损伤诱导因子的作用一致。向成年大鼠完整的坐骨神经神经内注射白血病抑制因子可显着增加L4和L5背根神经节中对甘丙肽具有免疫反应性的神经元分布百分比,而不会改变对血管活性肠多肽或神经肽Y具有免疫反应性的分布百分比。 -免疫反应性主要限于逆行转运和积累白血病抑制因子的那些神经元。用抗gp130受体基序的单克隆抗体连续治疗两周后,坐骨神经单侧轴突切开后,L4和L5背根神经节中甘丙肽免疫反应性的上调显着降低。向完整的坐骨神经神经内注射白细胞介素6也显着增加了神经元分布的百分比,这些分布显示了甘丙肽免疫反应性,但没有血管活性肠多肽或神经肽Y免疫反应性。我们的结果表明,与周围神经损伤部位的gp130受体相互作用的细胞因子有助于细胞体对轴突切开的反应。但是,这种细胞因子水平的变化不足以说明与周围神经损伤相关的神经肽表型变化的全部组成。

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