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首页> 外文期刊>Journal of neurotrauma >Limited Colocalization of Microbleeds and Microstructural Changes after Severe Traumatic Brain Injury
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Limited Colocalization of Microbleeds and Microstructural Changes after Severe Traumatic Brain Injury

机译:微微脑损伤后微妙的微妙和微观结构变化有限

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Severe traumatic brain injury (TBI) produces shearing forces on long-range axons and brain vessels, causing axonal and vascular injury. To examine whether microbleeds and axonal injury colocalize after TBI, we performed whole-brain susceptibility-weighted imaging (SWI) and diffusion tensor imaging (DTI) in 14 patients during the subacute phase after severe TBI. SWI was used to determine the number and volumes of microbleeds in five brain regions: the frontotemporal lobe; parieto-occipital lobe; midsagittal region (cingular cortex, parasagittal white matter, and corpus callosum); deep nuclei (basal ganglia and thalamus); and brainstem. Averaged fractional anisotropy (FA) and mean diffusivity (MD) were measured to assess microstructural changes in the normal appearing white matter attributed to axonal injury in the same five regions. Regional expressions of microbleeds and microstructure were used in a partial least-squares model to predict the impairment of consciousness in the subacute stage after TBI as measured with the Coma Recovery Scale-Revised (CRS-R). Only in the midsagittal region, the expression of microbleeds was correlated with regional changes in microstructure as revealed by DTI. Microbleeds and microstructural DTI-based metrics of deep, but not superficial, brain regions were able to predict individual CRS-R. Our results suggest that microbleeds are not strictly related to axonal pathology in other than the midsagittal region. While each measure alone was predictive, the combination of both metrics scaled best with individual CRS-R. Structural alterations in deep brain structures are relevant in terms of determining the severity of impaired consciousness in the acute stage after TBI.
机译:严重的创伤性脑损伤(TBI)在远程轴突和脑血管上产生剪切力,导致轴突和血管损伤。为了检查TBI后的微孔和轴突损伤是否上均可,我们在严重TBI后,在亚急期性相期间在14名患者中进行了全脑敏感性加权成像(SWI)和扩散张量成像(DTI)。 SWI用于确定五个脑区中微斑秃的数量和体积:额颞叶;锥形枕叶;中间地区(Cingular cortex,Parasagittal白质和胼callosum);深核(基础神经节和丘脑);和脑干。测量平均分数各向异性(FA)和平均扩散性(MD)以评估归因于同一五个区域的正常出现的白质的微观结构变化。微杂种和微观结构的区域表达用于局部最小二乘模型,以预测TBI后亚急性阶段中的意识的损害,与COMA恢复规模修订(CRS-R)测量。仅在中间显着区域中,微杂种的表达与DTI透露的微观结构的区域变化相关。微妙的深层和微观结构DTI的深度,但不肤浅,脑区能够预测单独的CRS-R。我们的研究结果表明,除了仲裁地点外,微斑秃与轴突病理学不严格相关。虽然单独的每种措施都是预测的,但两个指标的组合都可以使用单独的CRS-R来缩放。深脑结构中的结构改变是根据在TBI急性阶段中的损伤意识的严重程度相关的。

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