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血液及血液制品对蛛网膜细胞的影响。

The effects of blood and blood products on the arachnoid cell.

作者信息

Hansen Eric A, Romanova Liudmila, Janson Christopher, Lam Cornelius H

机构信息

Department of Research, Minneapolis VA Medical Center, 1 Veterans Drive, Research Service 151, Minneapolis, MN, 55417, USA.

Department of Neurology and Rehabilitation, University of Illinois, Chicago, IL, USA.

出版信息

Exp Brain Res. 2017 Jun;235(6):1749-1758. doi: 10.1007/s00221-017-4927-2. Epub 2017 Mar 11.

Abstract

After traumatic brain injury (TBI), large amounts of red blood cells and hemolytic products are deposited intracranially creating debris in the cerebrospinal fluid (CSF). This debris, which includes heme and bilirubin, is cleared via the arachnoid granulations and lymphatic systems. However, the mechanisms by which erythrocytes and their breakdown products interfere with normal CSF dynamics remain poorly defined. The purpose of this study was to model in vitro how blood breakdown products affect arachnoid cells at the CSF-blood barrier, and the extent to which the resorption of CSF into the venous drainage system is mechanically impaired following TBI. Arachnoid cells were grown to confluency on permeable membranes. Rates of growth and apoptosis were measured in the presence of blood and lysed blood, changes in transepithelial electrical resistance (TEER) was measured in the presence of blood and hemoglobin, and small molecule permeability was determined in the presence of blood, lysed blood, bilirubin, and biliverdin. These results were directly compared with an established rat brain endothelial cell line (RBEC4) co-cultured with rat brain astrocytes. We found that arachnoid cells grown in the presence of whole or lysed erythrocytes had significantly slower growth rates than controls. Bilirubin and biliverdin, despite their low solubilities, altered the paracellular transport of arachnoid cells more than the acute blood breakdown components of whole and lysed blood. Mannitol permeability was up to four times higher in biliverdin treatments than controls, and arachnoid membranes demonstrated significantly decreased small molecule permeabilities in the presence of whole and lysed blood. We conclude that short-term (<24 h) arachnoid cell transport and long-term (>5 days) arachnoid cell viability are affected by blood and blood breakdown products, with important consequences for CSF flow and blood clearance after TBI.

摘要

创伤性脑损伤(TBI)后,大量红细胞和溶血产物沉积在颅内,在脑脊液(CSF)中产生碎屑。这些碎屑包括血红素和胆红素,通过蛛网膜颗粒和淋巴系统清除。然而,红细胞及其分解产物干扰正常脑脊液动力学的机制仍不清楚。本研究的目的是在体外模拟血液分解产物如何影响脑脊液-血液屏障处的蛛网膜细胞,以及TBI后脑脊液回吸收进入静脉引流系统在机械方面受损的程度。蛛网膜细胞在可渗透膜上生长至汇合。在有血液和溶血血液存在的情况下测量生长和凋亡率,在有血液和血红蛋白存在的情况下测量跨上皮电阻(TEER)的变化,并在有血液、溶血血液、胆红素和胆绿素存在的情况下测定小分子通透性。将这些结果与与大鼠脑星形胶质细胞共培养的已建立的大鼠脑内皮细胞系(RBEC4)直接进行比较。我们发现,在全血或溶血红细胞存在下生长的蛛网膜细胞的生长速度明显低于对照组。胆红素和胆绿素尽管溶解度低,但对蛛网膜细胞旁细胞转运的改变比全血和溶血血液的急性血液分解成分更大。在胆绿素处理组中甘露醇通透性比对照组高四倍,并且在全血和溶血血液存在下蛛网膜膜的小分子通透性显著降低。我们得出结论,短期(<24小时)蛛网膜细胞转运和长期(>5天)蛛网膜细胞活力受血液和血液分解产物影响,这对TBI后脑脊液流动和血液清除具有重要影响。

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