Smith Colin J, Johnson Brian N, Elkind Jaclynn A, See Jill M, Xiong Guoxiang, Cohen Akiva S
Division of Neurology, Children's Hospital of Philadelphia, USA
J Vis Exp. 2012 Nov 19(69):e4411. doi: 10.3791/4411.
Traumatic Brain Injury (TBI) afflicts more than 1.7 million people in the United States each year and even mild TBI can lead to persistent neurological impairments. Two pervasive and disabling symptoms experienced by TBI survivors, memory deficits and a reduction in seizure threshold, are thought to be mediated by TBI-induced hippocampal dysfunction. In order to demonstrate how altered hippocampal circuit function adversely affects behavior after TBI in mice, we employ lateral fluid percussion injury, a commonly used animal model of TBI that recreates many features of human TBI including neuronal cell loss, gliosis, and ionic perturbation. Here we demonstrate a combinatorial method for investigating TBI-induced hippocampal dysfunction. Our approach incorporates multiple ex vivo physiological techniques together with animal behavior and biochemical analysis, in order to analyze post-TBI changes in the hippocampus. We begin with the experimental injury paradigm along with behavioral analysis to assess cognitive disability following TBI. Next, we feature three distinct ex vivo recording techniques: extracellular field potential recording, visualized whole-cell patch-clamping, and voltage sensitive dye recording. Finally, we demonstrate a method for regionally dissecting subregions of the hippocampus that can be useful for detailed analysis of neurochemical and metabolic alterations post-TBI. These methods have been used to examine the alterations in hippocampal circuitry following TBI and to probe the opposing changes in network circuit function that occur in the dentate gyrus and CA1 subregions of the hippocampus (see Figure 1). The ability to analyze the post-TBI changes in each subregion is essential to understanding the underlying mechanisms contributing to TBI-induced behavioral and cognitive deficits. The multi-faceted system outlined here allows investigators to push past characterization of phenomenology induced by a disease state (in this case TBI) and determine the mechanisms responsible for the observed pathology associated with TBI.
创伤性脑损伤(TBI)在美国每年影响超过170万人,即使是轻度TBI也可能导致持续性神经功能障碍。TBI幸存者普遍存在且致残的两种症状,即记忆缺陷和癫痫阈值降低,被认为是由TBI诱导的海马功能障碍介导的。为了证明海马回路功能改变如何对小鼠TBI后的行为产生不利影响,我们采用了侧脑室液压冲击伤,这是一种常用的TBI动物模型,它再现了人类TBI的许多特征,包括神经元细胞丢失、胶质细胞增生和离子紊乱。在这里,我们展示了一种研究TBI诱导的海马功能障碍的组合方法。我们的方法将多种离体生理技术与动物行为和生化分析相结合,以分析TBI后海马的变化。我们首先采用实验性损伤范式并结合行为分析来评估TBI后的认知障碍。接下来,我们重点介绍三种不同的离体记录技术:细胞外场电位记录、可视化全细胞膜片钳记录和电压敏感染料记录。最后,我们展示了一种对海马亚区域进行区域解剖的方法,这对于详细分析TBI后的神经化学和代谢改变可能是有用的。这些方法已被用于检查TBI后海马回路的改变,并探究海马齿状回和CA1亚区域网络回路功能发生的相反变化(见图1)。分析每个亚区域TBI后变化的能力对于理解导致TBI诱导的行为和认知缺陷的潜在机制至关重要。这里概述的多方面系统使研究人员能够超越对疾病状态(在这种情况下是TBI)诱导的现象学的表征,并确定与TBI相关的观察到的病理学的负责机制。