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有助于慢性创伤性脑病诊断的临床关联:来自新型啮齿动物重复性脑震荡模型的见解。

Clinical correlates to assist with chronic traumatic encephalopathy diagnosis: Insights from a novel rodent repeat concussion model.

作者信息

Thomsen Gretchen M, Ko Ara, Harada Megan Y, Ma Annie, Wyss Livia, Haro Patricia, Vit Jean-Philippe, Avalos Pablo, Dhillon Navpreet K, Cho Noell, Shelest Oksana, Ley Eric J

机构信息

From the Regenerative Medicine Institute (G.M.T., A.M., L.W., P.H., N.C., O.S.), Department of Biomedical Sciences (G.M.T., J-P.V.), and Biobehavioral Research Core (J-P.V.), and Division of Trauma and Critical Care, Department of Surgery (A.K., M.Y.H., N.D., E.J.L.), Cedars-Sinai Medical Center, Los Angeles, California.

出版信息

J Trauma Acute Care Surg. 2017 Jun;82(6):1039-1048. doi: 10.1097/TA.0000000000001443.

Abstract

INTRODUCTION

Chronic traumatic encephalopathy (CTE) is a neurodegenerative disease linked to repetitive head injuries. Chronic traumatic encephalopathy symptoms include changes in mood, behavior, cognition, and motor function; however, CTE is currently diagnosed only postmortem. Using a rat model of recurrent traumatic brain injury (TBI), we demonstrate rodent deficits that predict the severity of CTE-like brain pathology.

METHODS

Bilateral, closed-skull, mild TBI was administered once per week to 35 wild-type rats; eight rats received two injuries (2×TBI), 27 rats received five injuries (5×TBI), and 13 rats were sham controls. To determine clinical correlates for CTE diagnosis, TBI rats were separated based on the severity of rotarod deficits and classified as "mild" or "severe" and further separated into "acute," "short," and "long" based on age at euthanasia (90, 144, and 235 days, respectively). Brain atrophy, phosphorylated tau, and inflammation were assessed.

RESULTS

All eight 2×TBI cases had mild rotarod deficiency, 11 5×TBI cases had mild deficiency, and 16 cases had severe deficiency. In one cohort of rats, tested at approximately 235 days of age, balance, rearing, and grip strength were significantly worse in the severe group relative to both sham and mild groups. At the acute time period, cortical thinning, phosphorylated tau, and inflammation were not observed in either TBI group, whereas corpus callosum thinning was observed in both TBI groups. At later time points, atrophy, tau pathology, and inflammation were increased in mild and severe TBI groups in the cortex and corpus callosum, relative to sham controls. These injury effects were exacerbated over time in the severe TBI group in the corpus callosum.

CONCLUSIONS

Our model of repeat mild TBI suggests that permanent deficits in specific motor function tests correlate with CTE-like brain pathology. Assessing balance and motor coordination over time may predict CTE diagnosis.

摘要

引言

慢性创伤性脑病(CTE)是一种与重复性头部损伤相关的神经退行性疾病。慢性创伤性脑病的症状包括情绪、行为、认知和运动功能的改变;然而,CTE目前只能在死后进行诊断。使用复发性创伤性脑损伤(TBI)大鼠模型,我们证明了啮齿动物的缺陷可以预测类似CTE的脑病理严重程度。

方法

每周对35只野生型大鼠进行一次双侧闭合性颅骨轻度TBI;8只大鼠接受两次损伤(2×TBI),27只大鼠接受五次损伤(5×TBI),13只大鼠为假手术对照组。为了确定CTE诊断的临床相关性,根据转棒试验缺陷的严重程度将TBI大鼠分开,并分为“轻度”或“重度”,并根据安乐死时的年龄(分别为90、144和235天)进一步分为“急性”、“短期”和“长期”。评估脑萎缩、磷酸化tau蛋白和炎症。

结果

所有8例2×TBI病例均有轻度转棒试验缺陷,11例5×TBI病例有轻度缺陷,16例有重度缺陷。在一组约235日龄的大鼠中,重度组的平衡、竖毛和握力相对于假手术组和轻度组均明显较差。在急性期,两个TBI组均未观察到皮质变薄、磷酸化tau蛋白和炎症,而两个TBI组均观察到胼胝体变薄。在随后的时间点,相对于假手术对照组,轻度和重度TBI组的皮质和胼胝体中的萎缩、tau蛋白病理和炎症均增加。这些损伤效应在重度TBI组的胼胝体中随时间加剧。

结论

我们的重复性轻度TBI模型表明,特定运动功能测试中的永久性缺陷与类似CTE的脑病理相关。随着时间的推移评估平衡和运动协调性可能预测CTE诊断。

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