雄性大鼠重复性爆破创伤性脑损伤 1 个月后的焦虑样特征、前爪热敏性变化和神经胶质改变

IF 1.8 Q4 NEUROSCIENCES

Annals of Neurosciences Pub Date : 2024-08-12 DOI:10.1177/09727531241248976

Srinivasu Kallakuri, Nareen Sadik, Cameron J Davidson, Ali Gheidi, Kelly E Bosse, Cynthia A Bir, Alana C Conti, Shane A Perrine

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引用次数: 0

摘要

背景：许多军人都是重复性爆炸创伤性脑损伤（rbTBI）的受害者，在他们的一生中要忍受各种心理和行为状况的改变。其中包括焦虑、创伤后应激和疼痛。因此，本研究试图填补关于rbTBI一个月后持久行为和神经炎症标志物改变的知识空白。目的：尽管之前的rbTBI动物研究显示了创伤后几天（急性）或几个月（慢性）的行为和组织病理学变化，但与中间时间段（即rbTBI一个月后）创伤后变化有关的知识却不太清楚或无法获得：方法：将 Sprague-Dawley 大鼠（雄性；n = 12）分配到 rbTBI 或假体条件下。rbTBI组的动物连续三天每天暴露于一次爆炸，而假组的动物则暴露于相同的实验条件下，但不暴露于爆炸。所有动物都接受了基线焦虑测试。受伤后 30 天，再次对动物进行焦虑和爪热敏感性测试，然后取脑进行免疫组化分析：结果：受到 rbTBI 伤害的动物在高架加迷宫参数上表现出类似焦虑的行为迹象，前爪热退缩潜伏期缩短也表明动物有疼痛的行为迹象。从组织学角度看，暴露于 rbTBI 的动物的脑切片显示，内侧前额叶皮层的小胶质细胞/巨噬细胞和星形胶质细胞数量明显增加：这项初步临床前研究的数据证明，即使在 rbTBI 后 1 个月，假定的焦虑样行为、前爪热敏感性增强和神经胶质细胞数量增加的情况也很普遍。这些研究结果对评估受爆炸影响的军人和平民的治疗具有潜在影响，并强调了为易受单次或多次爆炸影响的人群制定保护措施的必要性。有必要进一步了解与 rbTBI 相关的慢性并发行为和神经病理后遗症。

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Anxiety-like Characteristics, Forepaw Thermal Sensitivity Changes and Glial Alterations 1 Month After Repetitive Blast Traumatic Brain Injury in Male Rats.

Background: Many military service members are victims of repetitive blast traumatic brain injuries (rbTBI) and endure diverse altered psychological and behavioural conditions during their lifetime. Some of these conditions include anxiety, post-traumatic stress and pain. Thus, this study attempts to fill the knowledge gap on enduring behavioural and neuroinflammatory marker alterations 1 month after rbTBI.

Purpose: Although previous rbTBI animal studies have shown behavioural and histopathological changes either a few days (acute) or many months (chronic) after trauma, knowledge related to post-traumatic changes during the intermediate timeframe, i.e. a month after rbTBI is less clear or unavailable.

Methods: Sprague-Dawley rats (male; n = 12) were assigned to either rbTBI or sham conditions. Animals assigned to the rbTBI group were subjected to 1 blast exposure per day for three consecutive days, while animals in the sham group were exposed to identical experimental conditions sans blast exposure. All animals were tested for anxiety at baseline. 30 days post-injury, animals were tested again for anxiety and paw thermal sensitivity, followed by brain harvest for immunohistochemical analyses.

Results: Animals exposed to rbTBI showed signs of anxiety-like behaviour on parameters of elevated plus-maze and behavioural signs of pain indicated by reduced thermal withdrawal latency of the forepaw. Histologically, brain sections from animals exposed to rbTBI showed a significantly increased number of microglial/macrophage and astrocytic counts in the medial prefrontal cortex.

Conclusion: Data from this initial preclinical study support the prevalence of putative anxiety-like behaviour, enhancement in forepaw thermal sensitivity and increase in the number of glial cells even 1 month after rbTBI. These findings have potential implications in the treatment evaluation of blast-exposed military and civilian populations and emphasise the need for devising protective measures for people susceptible to single or repeated exposures. A greater further understanding of rbTBI-related chronic concurrent behavioural and neuropathological sequela is warranted.

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Annals of Neurosciences NEUROSCIENCES-

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2.40

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0.00%

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