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Diffusion tensor imaging detects chronic microstructural changes in white and gray matter after traumatic brain injury in rat

机译:扩散张量成像检测大鼠脑外伤后白和灰质的慢性微结构变化

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Traumatic brain injury (TBI) is a major cause of disability and death in people of all ages worldwide. An initial brain injury caused by external mechanical forces triggers a cascade of tissue changes that lead to a wide spectrum of symptoms and disabilities, such as cognitive deficits, mood or anxiety disorders, motor impairments, chronic pain, and epilepsy. We investigated the detectability of secondary injury at a chronic time-point using ex vivo diffusion tensor imaging (DTI) in a rat model of TBI, lateral fluid percussion (LFP) injury. Our analysis of ex vivo DTI data revealed persistent microstructural tissue changes in white matter tracts, such as the splenium of the corpus callosum, angular bundle, and internal capsule. Histologic examination revealed mainly loss of myelinated axons and/or iron accumulation. Gray matter areas in the thalamus exhibited an increase in fractional anisotropy associated with neurodegeneration, myelinated fiber loss, and/or calcifications at the chronic phase. In addition, we examined whether these changes could also be detected with in vivo settings at the same chronic time-point. Our results provide insight into DTI detection of microstructural changes in the chronic phase of TBI, and elucidate how these changes correlate with cellular level alterations.
机译:颅脑外伤(TBI)是导致世界各地所有年龄段的人致残和死亡的主要原因。由外部机械力引起的最初的脑损伤会触发一系列的组织变化,从而导致多种症状和残疾,例如认知缺陷,情绪或焦虑症,运动障碍,慢性疼痛和癫痫病。我们在TBI大鼠模型中,使用离体扩散张量成像(DTI),研究了在慢性时间点继发性损伤的可检测性,即侧面液体撞击(LFP)损伤。我们对离体DTI数据的分析揭示了白质束(例如call体的脾脏,角丛和内囊)中持续存在的微结构组织变化。组织学检查显示主要是髓鞘轴突丢失和/或铁积累。丘脑中的灰质区域在慢性期表现出与神经变性,髓鞘纤维丢失和/或钙化相关的分数各向异性的增加。此外,我们检查了在相同的慢性时间点体内设置是否也可以检测到这些变化。我们的结果提供了对TBI慢性期微结构变化的DTI检测的见解,并阐明了这些变化与细胞水平改变之间的关系。

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