实验性脑肿瘤和脑脓肿血脑屏障障碍的病理生理方面。

K A Hossmann, H W Bothe, W Bodsch, W Paschen
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引用次数: 18

摘要

实验肿瘤和脓肿分别由胚瘤胶质细胞克隆和金黄色葡萄球菌在半球内接种产生。两种模型均出现严重的血管源性脑水肿。通过全身应用Evans蓝或过氧化物酶来确定屏障病变的位置,并通过免疫自显像定位渗出的血清蛋白来确定水肿的扩散。在两种实验条件下,血清蛋白弥漫性地积聚在同侧半球的白质中,尽管屏障病变严格局限于病理病灶。肿瘤和脓肿附近水肿白质含水量分别由69.1和80.6 ml/100g w.w.增加到82.3 ml/100g w.w.。这种增加与流量的体积依赖性减少、钠的平行增加和外渗血清蛋白的增加有关。后者由一种新开发的免疫化学方法确定,并对血清总蛋白含量的血管内部分进行适当的校正。肿瘤和脓肿水肿液中钠的计算浓度分别为132和129 ueq/ml。血清蛋白浓度分别为8.7和6.4 mg/ml。因此,水肿液的蛋白质含量低于血清的10%。这表明血管源性水肿中的液体积聚不能仅仅用外渗蛋白的致瘤性来解释。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pathophysiological aspects of blood-brain barrier disturbances in experimental brain tumors and brain abscesses.

Experimental tumors and abscesses were produced by intrahemispheric inoculation of a blastomatous glial cell clone and of staphylococcus aureus, respectively. In both models severe vasogenic brain edema developed. The site of the barrier lesion was identified by systemic application of Evans blue or peroxidase, and the spread of edema by immunoautoradiographic localisation of extravasated serum proteins. In both experimental conditions, serum proteins accumulated diffusely in the white matter of the ipsilateral hemisphere, although the barrier lesion was strictly confined to the pathological focus. Water content of the edematous white matter in the vicinity of tumors and abscesses increased from 69.1 to 80.6 and 82.3 ml/100g w.w., respectively. This increase was associated with a volume-dependent decrease of flow, a parallel increase of sodium and an increase of extravasated serum proteins. The latter was determined by a newly developed immunochemical approach with appropriate corrections for the intravascular fraction of total serum protein content. The calculated concentration of sodium in edema fluid of tumors and abscesses amounted to 132 and 129 ueq/ml, respectively. The concentration of serum proteins was 8.7 and 6.4 mg/ml, respectively. Protein content of edema fluid, in consequence was less than 10% of blood serum. This suggests that fluid accumulation in vasogenic edema cannot be explained by the oncotic properties of extravasated proteins alone.

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