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Axonal transport rate decreased at the onset of optic neuritis in EAE mice

机译:EAE小鼠视神经炎发作时轴突转运速率降低

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Optic neuritis is frequently the first symptom of multiple sclerosis (MS), an inflammatory demyelinating neuro-degenerative disease. Impaired axonal transport has been considered as an early event of neurodegenerative diseases. However, few studies have assessed the integrity of axonal transport in MS or its animal models. We hypothesize that axonal transport impairment occurs at the onset of optic neuritis in experimental autoimmune encephalomyelitis (EAE) mice. In this study, we employed manganese-enhanced MRI (MEMRI) to assess axonal transport in optic nerves in EAE mice at the onset of optic neuritis. Axonal transport was assessed as (a) optic nerve Mn~(2+) accumulation rate (in % signal change/h) by measuring the rate of increased total optic nerve signal enhancement, and (b) Mn~(2+) transport rate (in mm/h) by measuring the rate of change in optic nerve length enhanced by Mn~(2+) . Compared to sham-treated healthy mice, Mn~(2+) accumulation rate was significantly decreased by 19% and 38% for EAE mice with moderate and severe optic neuritis, respectively. The axonal transport rate of Mn~(2+) was significantly decreased by 43% and 65% for EAE mice with moderate and severe optic neuritis, respectively. The degree of axonal transport deficit correlated with the extent of impaired visual function and diminished microtubule-associated tubulins, as well as the severity of inflammation, demyelination, and axonal injury at the onset of optic neuritis.
机译:视神经炎通常是多发性硬化症(MS)的第一种症状,多发性硬化症是一种脱髓鞘性神经退行性疾病。轴突运输受损被认为是神经退行性疾病的早期事件。但是,很少有研究评估MS或其动物模型中轴突运输的完整性。我们假设在实验性自身免疫性脑脊髓炎(EAE)小鼠视神经炎发作时发生轴突运输障碍。在这项研究中,我们采用锰增强MRI(MEMRI)来评估视神经炎发作时EAE小鼠视神经中的轴突运输。轴突运输评估为(a)视神经Mn〜(2+)积累率(以%信号变化/ h为单位),方法是测量总的视神经信号增强率,以及(b)Mn〜(2+)传输率通过测量由Mn〜(2+)增强的视神经长度的变化率(毫米/小时)。与假治疗的健康小鼠相比,中度和重度视神经炎的EAE小鼠的Mn〜(2+)积累率分别降低了19%和38%。对于中度和重度视神经炎的EAE小鼠,Mn〜(2+)的轴突转运率分别降低了43%和65%。视神经炎发作时,轴突运输缺陷的程度与视觉功能受损的程度和与微管相关的微管蛋白减少以及炎症,脱髓鞘和轴突损伤的严重程度有关。

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