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首页> 外文期刊>The European Journal of Neuroscience >Sustained cell body reactivity and loss of NeuN in a subset of axotomized bulbospinal neurons after a chronic high cervical spinal cord injury
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Sustained cell body reactivity and loss of NeuN in a subset of axotomized bulbospinal neurons after a chronic high cervical spinal cord injury

机译:慢性高宫颈脊髓损伤后,持续的细胞体内反应性和Neun的损失在慢性高宫颈脊髓损伤后

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摘要

Following central nervous system lesion, the ability of injured axons to regrowth may depend on the level and duration of the injured cell body response (CBR). Therefore, to investigate whether axotomized brainstem neurons maintain a durable growth-competent state after spinal cord injury, we studied the effect of a chronic C2 hemisection in rats on the expression of various CBR markers involved in axon regeneration, such as c-Jun, ATF-3, HSP27, NO synthase (NOS), and also of the neural mature phenotype marker NeuN, in the bulbospinal respiratory neurons as compared to the gigantocellularis nucleus. Both at 7 and 30 days post-lesion (DPL), c-Jun and HSP27 were present in, respectively, -60 and -20% of the axotomized respiratory neurons, whereas the apoptotic factor caspase 3 was not detected in these cells. NOS appeared belatedly, and it was detected in -20% of the axotomized respiratory neurons at 30DPL. At 30DPL, these different CBR markers were strongly colocalized in a sub-population of axotomized respiratory neurons and also in a sub-population of injured neurons within the gigantocellularis nucleus. Such CBR was also accompanied by a sustained alteration of the neural mature phenotype, as indicated by a loss of NeuN immunore-activity selectively in HSP27+ bulbospinal neurons at 7DPL and 30DPL. Altogether, this study shows that a subset of axotomized medullary respiratory neurons remains in a growth-competent state after a chronic injury, suggesting that they may play a preferential role in long-lasting respiratory neuroplasticity processes.
机译:在中枢神经系统病变之后,受伤轴突再次生育的能力可能取决于受伤细胞体内反应(CBR)的水平和持续时间。因此,为了探讨坐落化脑干神经元是否保持脊髓损伤后耐用的生长态度,我们研究了慢性C2在大鼠中慢性C2的效果对轴突再生的各种CBR标志物的表达,如C-Jun,ATF -3,HSP27,没有合成酶(NOS),也没有神经成熟表型标志物NeUN,在球茎呼吸道神经元中与千酮核细胞核相比。在病变后7和30天,分别存在于-60和-20%的官方化呼吸道神经元的7和30天,而在这些细胞中未检测到凋亡因子Caspase 3。 NOS出现姗姗来迟,它在30dpl下检测到-20%的轴突呼吸道神经元。在30dpl时,这些不同的CBR标记物在轴向呼吸道神经元的亚群中强烈分解,并且在Gigantocellularis核内的受损神经元的亚群中。这种CBR还伴随着神经成熟表型的持续改变,如在7DPL和30DPL在HSP27 +球茎神经元中选择性地在HSP27 +球茎神经元中的损失。该研究总共表明,在慢性损伤后,腋瘤髓质呼吸道神经元的子集仍处于生长态度,表明它们可能在长期呼吸道神经塑性过程中发挥优势作用。

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