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In vitro studies of primary explosive blast loading on neurons

机译:神经元上主要爆炸冲击波加载的体外研究

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In a military setting, traumatic brain injury (TBI) is frequently caused by blast waves that can trigger a series of neuronal biochemical changes. Although many animal models have been used to study the effects of primary blast waves, elucidating the mechanisms of damage in a whole-animal model is extremely complex. In vitro models of primary blast, which allow for the deconvolution of mechanisms, are relatively scarce. It is largely unknown how structural damage at the cellular level impacts the functional activity at variable time scales after the TBI event. A novel in vitro system was developed to probe the effects of explosive blast (ranging from approximate to 25 to 40 psi) on dissociated neurons. PC12 neurons were cultured on laminin-coated substrates, submerged underwater, and subjected to single and multiple blasts in a controlled environment. Changes in cell membrane permeability, viability, and cell morphology were evaluated. Significant increases in axonal beading were observed in the injured cells. In addition, although cell death was minimal after a single insult, cell viability decreased significantly following repeated blast exposure. (c) 2015 Wiley Periodicals, Inc.
机译:在军事环境中,颅脑外伤(TBI)通常是由爆炸波引起的,爆炸波可以触发一系列神经元生化变化。尽管已使用许多动物模型来研究原始冲击波的影响,但阐明全动物模型中的损伤机制却极为复杂。允许机制解卷积的原代爆炸的体外模型相对较少。在TBI事件发生后的可变时间尺度上,细胞水平的结构损伤如何影响功能活动在很大程度上是未知的。开发了一种新型的体外系统以探测爆炸冲击波(范围从大约25到40 psi)对解离的神经元的影响。在层粘连蛋白包被的基质上培养PC12神经元,将其浸没在水下,并在受控环境中进行一次或多次爆炸。评估了细胞膜通透性,生存力和细胞形态的变化。在受损细胞中观察到轴突珠粒的显着增加。此外,尽管单次受伤害后细胞死亡极少,但反复爆炸暴露后细胞活力却显着下降。 (c)2015年威利期刊有限公司

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