Namjoshi Dhananjay R, Cheng Wai Hang, McInnes Kurt A, Martens Kris M, Carr Michael, Wilkinson Anna, Fan Jianjia, Robert Jerome, Hayat Arooj, Cripton Peter A, Wellington Cheryl L
Department of Pathology and Laboratory Medicine, The University of British Columbia, Vancouver, BC, Canada.
Mol Neurodegener. 2014 Dec 1;9:55. doi: 10.1186/1750-1326-9-55.
Traumatic brain injury (TBI) is a major health care concern that currently lacks any effective treatment. Despite promising outcomes from many preclinical studies, clinical evaluations have failed to identify effective pharmacological therapies, suggesting that the translational potential of preclinical models may require improvement. Rodents continue to be the most widely used species for preclinical TBI research. As most human TBIs result from impact to an intact skull, closed head injury (CHI) models are highly relevant, however, traditional CHI models suffer from extensive experimental variability that may be due to poor control over biomechanical inputs. Here we describe a novel CHI model called CHIMERA (Closed-Head Impact Model of Engineered Rotational Acceleration) that fully integrates biomechanical, behavioral, and neuropathological analyses. CHIMERA is distinct from existing neurotrauma model systems in that it uses a completely non-surgical procedure to precisely deliver impacts of prescribed dynamic characteristics to a closed skull while enabling kinematic analysis of unconstrained head movement. In this study, we characterized head kinematics as well as functional, neuropathological, and biochemical outcomes up to 14d following repeated TBI (rTBI) in adult C57BL/6 mice using CHIMERA.
Head kinematic analysis showed excellent repeatability over two closed head impacts separated at 24h. Injured mice showed significantly prolonged loss of righting reflex and displayed neurological, motor, and cognitive deficits along with anxiety-like behavior. Repeated TBI led to diffuse axonal injury with extensive microgliosis in white matter from 2-14d post-rTBI. Injured mouse brains also showed significantly increased levels of TNF-α and IL-1β and increased endogenous tau phosphorylation.
Repeated TBI using CHIMERA mimics many of the functional and pathological characteristics of human TBI with a reliable biomechanical response of the head. This makes CHIMERA well suited to investigate the pathophysiology of TBI and for drug development programs.
创伤性脑损伤(TBI)是一个重大的医疗保健问题,目前缺乏有效的治疗方法。尽管许多临床前研究取得了有前景的结果,但临床评估未能确定有效的药物治疗方法,这表明临床前模型的转化潜力可能需要提高。啮齿动物仍然是临床前TBI研究中使用最广泛的物种。由于大多数人类TBI是由对完整颅骨的撞击引起的,闭合性颅脑损伤(CHI)模型具有高度相关性,然而,传统的CHI模型存在广泛的实验变异性,这可能是由于对生物力学输入的控制不佳所致。在这里,我们描述了一种名为CHIMERA(工程旋转加速度闭合性颅脑撞击模型)的新型CHI模型,该模型完全整合了生物力学、行为学和神经病理学分析。CHIMERA与现有的神经创伤模型系统不同,它使用完全非手术程序将规定动态特征的撞击精确地传递到闭合的颅骨,同时能够对无约束的头部运动进行运动学分析。在本研究中,我们使用CHIMERA对成年C57BL/6小鼠重复TBI(rTBI)后长达14天的头部运动学以及功能、神经病理学和生化结果进行了表征。
头部运动学分析显示,在24小时分开的两次闭合性颅脑撞击中具有出色的重复性。受伤小鼠的翻正反射丧失时间显著延长,并表现出神经、运动和认知缺陷以及焦虑样行为。重复TBI导致弥漫性轴索损伤,在rTBI后2-14天白质中出现广泛的小胶质细胞增生。受伤小鼠的大脑还显示TNF-α和IL-1β水平显著升高,内源性tau磷酸化增加。
使用CHIMERA进行重复TBI模拟了人类TBI的许多功能和病理特征,并具有可靠的头部生物力学反应。这使得CHIMERA非常适合研究TBI的病理生理学和药物开发项目。
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