老年会加剧闭合性头部损伤后的白质神经炎症和认知缺陷,对雌性小鼠尤为如此

IF 1.8 Q3 CLINICAL NEUROLOGY
Neurotrauma reports Pub Date : 2024-08-22 eCollection Date: 2024-01-01 DOI:10.1089/neur.2024.0074
Teresa Macheda, Margaret R Andres, Lydia Sanders, Kelly N Roberts, Ryan K Shahidehpour, Josh M Morganti, Adam D Bachstetter
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引用次数: 0

摘要

老年人创伤性脑损伤(TBI)的发病率越来越高,尤其是跌倒造成的轻度脑损伤,这凸显了研究与年龄相关的结果以及对 TBI 反应的潜在性别差异的必要性。尽管之前的研究已在开颅中重度创伤性脑损伤模型中定义了衰老-创伤性脑损伤特征(神经胶质反应增强和认知功能障碍),但这种特征是否也存在于轻度闭合性头部损伤(CHIs)中还不得而知。本研究探讨了年龄和性别对 4 个月大和 18 个月大的 C57BL/6 小鼠在电磁撞击器诱导的小鼠脑损伤模型中恢复的影响。我们评估了小鼠的向右转反射、体重、行为(径向臂水迷宫和主动回避)以及新皮质、胼胝体和海马的炎症(GFAP、IBA1、CD45)。我们观察到,老年雌性小鼠表现出更严重的创伤性脑损伤引起的认知障碍。此外,随着年龄的增长,白质区域的反应性神经炎症反应更加明显。与此相反,老年动物的灰质区域要么对损伤没有表现出增强的病理变化,要么老年小鼠表现出神经胶质细胞反应低下和萎缩性神经胶质细胞变性的迹象,而年轻小鼠在脑损伤后则没有这些迹象。这些研究结果表明,衰老会影响脊髓损伤的结果,部分反映了白质中更严重损伤的衰老-创伤特征,而在灰质中则发现了明显的衰老和轻度创伤特征。女性更容易受到年龄和轻度脑损伤的共同影响,这为进一步研究衰老女性的性别双态反应机制奠定了基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Old Age Exacerbates White Matter Neuroinflammation and Cognitive Deficits Following Closed-Head Injury, Particularly in Female Mice.

The increasing incidence of traumatic brain injury (TBI) among older adults, particularly mild injuries from falls, underscores the need to investigate age-related outcomes and potential sex differences in response to TBI. Although previous research has defined an aging-TBI signature (heightened glial responses and cognitive impairment) in open-skull moderate-to-severe TBI models, it is unknown whether this signature is also present in mild closed-head injuries (CHIs). This study explores the influences of age and sex on recovery in a mouse CHI model induced by an electromagnetic impactor device in 4-month-old and 18-month-old C57BL/6 mice. We assessed the righting reflex, body weight, behavior (radial arm water maze and active avoidance), and inflammation (GFAP, IBA1, CD45) in the neocortex, corpus callosum, and hippocampus. We observed that aged female mice exhibited more severe TBI-induced cognitive deficits. In addition, a more pronounced reactive neuroinflammatory response with age was noted within white matter regions. Conversely, gray matter regions in aged animals either showed no enhanced pathological changes in response to injury or the aged mice displayed hyporesponsive glia and signs of dystrophic glial degeneration that were not evident in their younger counterparts following CHI. These findings suggest that aging influences CHI outcomes, partially reflecting the aging-TBI signature seen in more severe injuries in white matter, while a distinct aging and mild-TBI signature was identified in gray matter. The heightened vulnerability of females to the combined effects of age and mild CHI establishes a foundation for further investigation into the mechanisms underlying the sexually dimorphic response in aging females.

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CiteScore
2.40
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