D'Ambrosio R, Maris D O, Grady M S, Winn H R, Janigro D
Department of Neurological Surgery, University of Washington, School of Medicine, Harborview Medical Center, Seattle, Washington 98104, USA.
J Neurosci. 1999 Sep 15;19(18):8152-62. doi: 10.1523/JNEUROSCI.19-18-08152.1999.
Traumatic brain injury (TBI) can be associated with memory impairment, cognitive deficits, or seizures, all of which can reflect altered hippocampal function. Whereas previous studies have focused on the involvement of neuronal loss in post-traumatic hippocampus, there has been relatively little understanding of changes in ionic homeostasis, failure of which can result in neuronal hyperexcitability and abnormal synchronization. Because glia play a crucial role in the homeostasis of the brain microenvironment, we investigated the effects of TBI on rat hippocampal glia. Using a fluid percussion injury (FPI) model and patch-clamp recordings from hippocampal slices, we have found impaired glial physiology 2 d after FPI. Electrophysiologically, we observed reduction in transient outward and inward K(+) currents. To assess the functional consequences of these glial changes, field potentials and extracellular K(+) activity were recorded in area CA3 during antidromic stimulation. An abnormal extracellular K(+) accumulation was observed in the post-traumatic hippocampal slices, accompanied by the appearance of CA3 afterdischarges. After pharmacological blockade of excitatory synapses and of K(+) inward currents, uninjured slices showed the same altered K(+) accumulation in the absence of abnormal neuronal activity. We suggest that TBI causes loss of K(+) conductance in hippocampal glia that results in the failure of glial K(+) homeostasis, which in turn promotes abnormal neuronal function. These findings provide a new potential mechanistic link between traumatic brain injury and subsequent development of disorders such as memory loss, cognitive decline, seizures, and epilepsy.
创伤性脑损伤(TBI)可能与记忆障碍、认知缺陷或癫痫发作有关,所有这些都可能反映出海马体功能的改变。尽管先前的研究集中在创伤后海马体中神经元损失的参与情况,但对离子稳态变化的了解相对较少,离子稳态的破坏会导致神经元过度兴奋和异常同步。由于神经胶质细胞在脑微环境的稳态中起着至关重要的作用,我们研究了TBI对大鼠海马神经胶质细胞的影响。使用液压冲击损伤(FPI)模型和海马切片的膜片钳记录,我们发现FPI后2天神经胶质细胞生理功能受损。在电生理学方面,我们观察到瞬时外向和内向K(+)电流减少。为了评估这些神经胶质细胞变化的功能后果,在逆向刺激期间记录了CA3区的场电位和细胞外K(+)活性。在创伤后的海马切片中观察到异常的细胞外K(+)积累,并伴有CA3区后放电的出现。在对兴奋性突触和K(+)内向电流进行药理学阻断后,未受伤的切片在没有异常神经元活动的情况下也显示出相同的K(+)积累改变。我们认为,TBI导致海马神经胶质细胞K(+)电导丧失,从而导致神经胶质细胞K(+)稳态失衡,进而促进神经元功能异常。这些发现为创伤性脑损伤与随后诸如记忆丧失、认知衰退、癫痫发作和癫痫等疾病的发展之间提供了一个新的潜在机制联系。