Center for Neurotrauma, Neurodegeneration and Restoration, Corporal Michael J. Crescenz Veterans Affairs Medical Center, Philadelphia, Pennsylvania, USA.
Department of Neurosurgery, University of Pennsylvania, Philadelphia, Pennsylvania, USA.
J Neurotrauma. 2020 Sep 1;37(17):1918-1932. doi: 10.1089/neu.2019.6738. Epub 2020 May 5.
Oculomotor deficits, such as insufficiencies in accommodation, convergence, and saccades, are common following traumatic brain injury (TBI). Previous studies in patients with mild TBI attributed these deficits to insufficient activation of subcortical oculomotor nuclei, although the exact mechanism is unknown. A possible cause for neuronal dysfunction in these regions is biomechanically induced plasma membrane permeability. We used our established porcine model of head rotational TBI to investigate whether cell permeability changes occurred in subcortical oculomotor areas following single or repetitive TBI, with repetitive injuries separated by 15 min, 3 days, or 7 days. Swine were subjected to sham conditions or head rotational acceleration in the sagittal plane using a HYGE pneumatic actuator. Two hours prior to the final injury, the cell-impermeant dye Lucifer Yellow was injected into the ventricles to diffuse throughout the interstitial space to assess plasmalemmal permeability. Animals were sacrificed 15 min after the final injury for immunohistological analysis. Brain regions examined for cell membrane permeability included caudate, substantia nigra pars reticulata, superior colliculus, and cranial nerve oculomotor nuclei. We found that the distribution of permeabilized neurons varied depending on the number and spacing of injuries. Repetitive injuries separated by 15 min or 3 days resulted in the most permeability. Many permeabilized cells lost neuron-specific nuclear protein reactivity, although no neuronal loss occurred acutely after injury. Microglia contacted and appeared to begin phagocytosing permeabilized neurons in repetitively injured animals. These pathologies within oculomotor areas may mediate transient dysfunction and/or degeneration that may contribute to oculomotor deficits following diffuse TBI.
眼动缺陷,如调节不足、集合不足和扫视不足,在创伤性脑损伤 (TBI) 后很常见。以前对轻度 TBI 患者的研究将这些缺陷归因于皮质下眼动核的激活不足,尽管确切机制尚不清楚。这些区域神经元功能障碍的一个可能原因是生物力学引起的质膜通透性增加。我们使用已建立的猪头部旋转 TBI 模型来研究皮质下眼动区是否在单次或重复 TBI 后发生细胞通透性变化,重复损伤间隔 15 分钟、3 天或 7 天。猪通过 HYGE 气动执行器在矢状面接受假条件或头部旋转加速。在最后一次损伤前 2 小时,将不透细胞的染料 Lucifer Yellow 注射到脑室中,使其扩散到整个间质空间,以评估质膜通透性。最后一次损伤后 15 分钟处死动物,进行免疫组织化学分析。检查细胞膜通透性的脑区包括尾状核、黑质网状部、上丘和颅神经动眼神经核。我们发现,通透性神经元的分布取决于损伤的数量和间隔。间隔 15 分钟或 3 天的重复损伤导致最多的通透性。许多通透性细胞失去神经元特异性核蛋白反应性,尽管损伤后急性无神经元丢失。在重复损伤的动物中,小胶质细胞接触并似乎开始吞噬通透性神经元。动眼区的这些病理学可能介导短暂的功能障碍和/或退化,这可能导致弥漫性 TBI 后的眼动缺陷。