Spinal Cord and Brain Injury Research Center, University of Kentucky Chandler Medical Center, Office B463, Biomedical and Biological Sciences Research Building, 741 S. Limestone St, Lexington, KY 40536-0509, USA.
Brain Struct Funct. 2012 Jan;217(1):49-61. doi: 10.1007/s00429-011-0323-z. Epub 2011 May 20.
Disruption and consequent reorganization of central nervous system circuits following traumatic brain injury may manifest as functional deficits and behavioral morbidities. We previously reported axotomy and neuronal atrophy in the ventral basal (VB) complex of the thalamus, without gross degeneration after experimental diffuse brain injury in adult rats. Pathology in VB coincided with the development of late-onset aberrant behavioral responses to whisker stimulation, which lead to the current hypothesis that neurodegeneration after experimental diffuse brain injury includes the primary somatosensory barrel cortex (S1BF), which receives projection of VB neurons and mediates whisker somatosensation. Over 28 days after midline fluid percussion brain injury, argyrophilic reaction product within superficial layers and layer IV barrels at 1 day progresses into the cortex to subcortical white matter by 7 days, and selective inter-barrel septa and subcortical white matter labeling at 28 days. Cellular consequences were determined by stereological estimates of neuronal nuclear volumes and number. In all cortical layers, neuronal nuclear volumes significantly atrophied by 42-49% at 7 days compared to sham, which marginally attenuated by 28 days. Concomitantly, the number of healthy neurons was reduced by 34-45% at 7 days compared to sham, returning to control levels by 28 days. Progressive neurodegeneration, including argyrophilic reaction product and neuronal nuclear atrophy, indicates injury-induced damage and reorganization of the reciprocal thalamocortical projections that mediate whisker somatosensation. The rodent whisker barrel circuit may serve as a discrete model to evaluate the causes and consequences of circuit reorganization after diffuse brain injury.
创伤性脑损伤后中枢神经系统回路的破坏和随之而来的重组可能表现为功能缺陷和行为障碍。我们之前报道过,在成年大鼠实验性弥漫性脑损伤后,腹侧基底(VB)复合体出现轴突切断和神经元萎缩,但无明显的退行性变。VB 的病理学与晚期出现的异常行为反应相一致,这种反应是对胡须刺激的反应,这导致了目前的假设,即实验性弥漫性脑损伤后的神经退行性变包括初级体感皮层(S1BF),它接收 VB 神经元的投射,并介导胡须体感。中线液冲击脑损伤后 28 天,1 天的浅层和 IV 层桶状核中的嗜银反应产物进展到 7 天的皮质下白质,28 天的选择性桶状核间隔和皮质下白质标记。细胞后果通过神经元核体积和数量的立体学估计来确定。在所有皮质层中,7 天时神经元核体积比假手术组显著萎缩了 42-49%,28 天时略有减轻。同时,7 天时健康神经元的数量比假手术组减少了 34-45%,28 天时恢复到对照水平。进行性神经退行性变,包括嗜银反应产物和神经元核萎缩,表明损伤诱导的损伤和介导胡须体感的丘脑皮质投射的逆行性重塑。啮齿动物胡须桶状回路可能作为一个离散的模型,用于评估弥漫性脑损伤后回路重塑的原因和后果。