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首页> 外文期刊>Antioxidants and redox signalling >Does Nrf2 gene transfer facilitate recovery after contusion spinal cord injury?
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Does Nrf2 gene transfer facilitate recovery after contusion spinal cord injury?

机译:Nrf2基因转移是否有助于挫伤性脊髓损伤后的恢复?

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Nuclear factor (erythroid-derived 2)-like 2 (Nrf2) modulates gene expression in response to oxidative damage in neurodegenerative diseases, including spinal cord injury (SCI). We noticed that activation of Nrf2 pathway persists for an extended time after clinically relevant contusion model of SCI. Injured Nrf2-/- mice were impaired in hindlimb function, exhibited increased atrophy, demyelination, and astrogliosis of the SC concomitant with altered expression of genes controlling apoptosis, inflammation, and neurotrophic factors suggesting the importance of Nrf2 for recovery. We used lentiviral gene transfer to increase Nrf2 expression and improve functional recovery after SCI. Although the transferred Nrf2 was expressed in neurons and astrocytes, we noticed hindlimb function impairment and elevated expression of pro-inflammatory cytokines as an adverse effect. These toxic effects were not reduced by including Nrf2 in the lentiviral vector. Augmenting the amount of delivered Nrf2 gene diminished toxic effects of the lentivirus, yet was not sufficient to improve functional recovery. Results of this study lead to the hypothesis that Nrf2 plays a crucial and multifaceted role in recovery from SCI, but even high overexpression of Nrf2 in injured SC may not offer extra benefit, providing protection only against lentivirus-induced toxicity that is manifested in the SC. Antioxid. Redox Signal. 20, 1313-1323.
机译:核因子(类胡萝卜素衍生的2)样2(Nrf2)调节基因表达,以响应神经退行性疾病(包括脊髓损伤(SCI))中的氧化损伤。我们注意到临床相关的SCI挫伤模型后,Nrf2途径的激活持续了较长时间。受伤的Nrf2-/-小鼠后肢功能受损,表现为SC萎缩,脱髓鞘和星形胶质增生,并伴有控制凋亡,炎症和神经营养因子的基因表达改变,提示Nrf2对恢复至关重要。我们使用慢病毒基因转移来增加Nrf2表达并改善SCI后的功能恢复。尽管转移的Nrf2在神经元和星形胶质细胞中表达,但我们注意到后肢功能受损和促炎性细胞因子表达升高是不利的。通过在慢病毒载体中包含Nrf2不会降低这些毒性作用。增加传递的Nrf2基因的数量减少了慢病毒的毒性作用,但不足以改善功能恢复。这项研究的结果得出这样的假设,即Nrf2在SCI的恢复中起着至关重要的和多方面的作用,但是即使在受伤的SC中高表达的Nrf2也可能无法提供额外的益处,只能针对SC中表现出的慢病毒诱导的毒性提供保护。 。抗氧化。氧化还原信号。 20,1313-1323。

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