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Altered Hippocampal Neurogenesis during the First 7 Days after a Fluid Percussion Traumatic Brain Injury

机译:液压打击创伤性脑损伤后的前7天海马神经发生改变

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摘要

Traumatic brain injury (TBI) is a devastating disorder causing negative outcomes in millions of people each year. Despite the alarming number of brain injuries and the long-term detrimental outcomes that can be associated with TBI, treatment options are lacking. Extensive investigation is underway, in hopes of identifying effective treatment strategies. Among the most state-of-the-art strategies is cell replacement therapy. TBI is a seemingly good candidate for cell replacement studies because there is often loss of neurons. However, translation of this therapy has not yet been successful. It is possible that a better understanding of endogenous neurogenic mechanisms after TBI could lead to more efficacious study designs using exogenous cell replacement strategies. Therefore, this study was designed to examine the number and migration of immature neurons at 1 and 7 d after a fluid percussion TBI. The results show that the number of immature neurons increases from 7 d after a fluid percussion injury (FPI), and there is ectopic migration of doublecortin (DCX+) immature neurons into the hilar region of the dentate gyrus. These results add important data to the current understanding of the endogenous neurogenic niche after TBI. Follow-up studies are needed to better understand the functional significance of elevated neurogenesis and aberrant migration into the hilus.
机译:颅脑外伤(TBI)是一种破坏性疾病,每年都会在数百万人中造成负面后果。尽管脑外伤的数量令人震惊,而且TBI可能带来长期有害的结果,但仍缺乏治疗选择。正在进行广泛的调查,以期找出有效的治疗策略。细胞替代疗法是最先进的策略之一。 TBI似乎是细胞替代研究的良好候选者,因为通常会丢失神经元。但是,该疗法的翻译尚未成功。 TBI后对内源性神经发生机制的更好理解可能会导致使用外源细胞替代策略进行更有效的研究设计。因此,本研究旨在检查液体冲击TBI后1和7 d时未成熟神经元的数量和迁移。结果表明,液体撞击伤(FPI)后7 d,未成熟神经元的数量增加,双皮质素(DCX +)未成熟神经元向异位迁移到齿状回的肺门区域。这些结果为TBI后内源性神经源利基的当前理解提供了重要的数据。需要进行后续研究,以更好地了解神经发生增高和异常迁移到hilus中的功能意义。

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