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首页> 外文期刊>Stroke: A Journal of Cerebral Circulation >Lobar intracerebral hemorrhage model in pigs: rapid edema development in perihematomal white matter.
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Lobar intracerebral hemorrhage model in pigs: rapid edema development in perihematomal white matter.

机译:猪的大叶脑出血模型:血肿周围白质迅速浮肿。

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BACKGROUND AND PURPOSE: The mechanisms underlying brain injury from intracerebral hemorrhage (ICH) are complex and poorly understood. To comprehensively examine pathophysiological and pathochemical alterations after ICH and to examine the effects of hematoma removal on these processes, we developed a physiologically controlled, reproducible, large-animal model of ICH in pigs (weight, 6 to 8 kg). METHODS: We produced lobar hematomas by pressure- controlled infusions of 1.7 mL of autologous blood into the right frontal hemispheric white matter over 15 minutes. We froze brains in situ at 1, 3, 5, and 8 hours after hematoma induction and cut coronal sections of hematoma assessment, morphological brain examination, and immunohistochemical and water content determinations. RESULTS: At 1 hour after blood infusion, "translucent" white matter areas were present directly adjacent to the hematoma. These markedly edematous regions had a greater than 10% increase in water content (>85%) compared with the contralateral white matter (73%), and this increased water content persisted through 8 hours. In addition, these areas were strongly immunoreactive for serum proteins. Intravascular Evans blue dye failed to penetrate into the brain tissue at all time points, demonstrating that this serum protein accumulation and edema development were not due to increased blood-brain barrier permeability. CONCLUSIONS: Experimental lobar ICH in pigs models a prominent pathological feature of human ICH, ie, early perihematomal edema. Our findings suggest that serum proteins, originating from the hematoma, accumulate in adjacent white matter and result in rapid and prolonged edema after ICH. This interstitial edema likely corresponds to the low densities on CT scans and the hyperintensities on T2-weighted MR images that surround intracerebral hematomas acutely after human ICH.
机译:背景与目的:脑出血(ICH)导致脑损伤的机制很复杂,人们对此知之甚少。为了全面检查ICH后的病理生理和病理化学变化,并检查血肿清除对这些过程的影响,我们开发了猪的ICH(重6至8 kg)的生理控制,可重现的大动物模型。方法:我们在15分钟内通过压力控制地向右额半球白质中注入1.7 mL自体血,产生了大叶性血肿。我们在血肿诱发后的1、3、5和8小时就地冻结了大脑,并切下了血肿评估,形态学脑检查以及免疫组织化学和水含量测定的冠状切片。结果:输血后1小时,血肿附近直接出现“半透明”白质区域。与对侧白质(73%)相比,这些明显水肿的区域的水分含量增加了10%以上(> 85%),并且这种增加的水分持续了8小时。另外,这些区域对血清蛋白具有强烈的免疫反应性。血管内伊文思蓝染料在所有时间点都未能渗透到脑组织中,表明这种血清蛋白的积累和水肿的形成并不是由于血脑屏障通透性的提高。结论:猪的实验性大叶脑出血模拟了人类脑出血的突出病理特征,即早期血肿周围水肿。我们的发现表明,源自血肿的血清蛋白会在相邻的白质中积聚,并导致ICH后快速而长期的水肿。这种间质性水肿可能对应于CT扫描的低密度和人脑出血后急性围绕脑内血肿的T2加权MR图像上的高强度。

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