首页> 美国卫生研究院文献>Journal of Neurotrauma >Imaging of White Matter Injury Correlates with Plasma and Tissue Biomarkers in Pediatric Porcine Model of Traumatic Brain Injury
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Imaging of White Matter Injury Correlates with Plasma and Tissue Biomarkers in Pediatric Porcine Model of Traumatic Brain Injury

机译:白质损伤的成像与创伤性脑损伤儿科猪模型中的血浆和组织生物标志物相关

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摘要

Traumatic brain injury (TBI) causes significant white matter injury, which has been characterized by various rodent and human clinical studies. The exact time course of imaging changes in a pediatric brain after TBI and its relation to biomarkers of injury and cellular function, however, is unknown. To study the changes in major white matter structures using a valid model of TBI that is comparable to a human pediatric brain in terms of size and anatomical features, we utilized a four-week-old pediatric porcine model of injury with controlled cortical impact (CCI). Using diffusion tensor imaging differential tractography, we show progressive anisotropy changes at major white matter tracts such as the corona radiata and inferior fronto-occipital fasciculus between day 1 and day 30 after injury. Moreover, correlational tractography shows a large part of bilateral corona radiata having positive correlation with the markers of cellular respiration. In contrast, bilateral corona radiata has a negative correlation with the plasma biomarkers of injury such as neurofilament light or glial fibrillary acidic protein. These are expected correlational findings given that higher integrity of white matter would be expected to correlate with lower injury biomarkers. We then studied the magnetic resonance spectroscopy findings and report decrease in a N-acetylaspartate/creatinine (NAA/Cr) ratio at the pericontusional cortex, subcortical white matter, corona radiata, thalamus, genu, and splenium of corpus callosum at 30 days indicating injury. There was also an increase in choline/creatinine ratio in these regions indicating rapid membrane turnover. Given the need for a pediatric TBI model that is comparable to human pediatric TBI, these data support the use of a pediatric pig model with CCI in future investigations of therapeutic agents. This model will allow future TBI researchers to rapidly translate our pre-clinical study findings into clinical trials for pediatric TBI.
机译:创伤性脑损伤 (TBI) 会导致严重的白质损伤,各种啮齿动物和人类临床研究都以这种损伤为特征。然而,TBI 后儿科大脑成像变化的确切时间进程及其与损伤生物标志物和细胞功能的关系尚不清楚。为了使用在大小和解剖特征方面与人类儿科大脑相当的有效 TBI 模型研究主要白质结构的变化,我们使用了一个 4 周龄的儿科猪损伤模型,具有受控皮层影响 (CCI)。使用弥散张量成像差异束造影,我们显示了受伤后第 1 天和第 30 天之间主要白质束(如放射冠和额枕下束)的进行性各向异性变化。此外,相关束造影显示大部分双侧放射冠状动脉与细胞呼吸标志物呈正相关。相比之下,双侧放射冠状动脉与损伤的血浆生物标志物(如神经丝光或神经胶质纤维酸性蛋白)呈负相关。鉴于白质的较高完整性预计与较低的损伤生物标志物相关,这些是预期的相关结果。然后,我们研究了磁共振波谱检查结果,并报告了 30 天时挫伤周围皮层、皮质下白质、放射冠、丘脑、膝和胼胝体脾的 N-乙酰天冬氨酸/肌酐 (NAA/Cr) 比率降低,表明受伤。这些区域的胆碱/肌酐比值也有所增加,表明膜更新迅速。鉴于需要与人类儿科 TBI 相当的儿科 TBI 模型,这些数据支持在未来治疗药物的研究中使用带有 CCI 的儿科猪模型。该模型将使未来的 TBI 研究人员能够快速将我们的临床前研究结果转化为儿科 TBI 的临床试验。

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