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体外模拟淋巴细胞向脑内的迁移:受淋巴细胞活化、细胞因子和抗原的调控

Lymphocyte migration into brain modelled in vitro: control by lymphocyte activation, cytokines, and antigen.

作者信息

Male D, Pyrce G, Hughes C, Lantos P

机构信息

Department of Neuropathology, Institute of Psychiatry, Denmark Hill, London, United Kingdom.

出版信息

Cell Immunol. 1990 Apr 15;127(1):1-11. doi: 10.1016/0008-8749(90)90109-5.

Abstract

Factors controlling lymphocyte adhesion to brain endothelium were investigated in vitro. Mitogen activation of lymphocytes causes increased adhesion to endothelium, which is maximal at 7-24 hr, declines to normal levels after the cells divide, and requires protein synthesis. Rat brain endothelium can be stimulated with IFN-gamma to increase its adhesion to either normal or activated lymphocytes. The endothelium is sensitive to low levels of cytokine: adhesion develops rapidly after stimulation and requires new protein synthesis. Antigen-specific line cells also adhere more effectively to endothelium than normal lymph node cells. This is enhanced by IFN-gamma treatment of the endothelium and is further increased marginally in the presence of the cognate antigen. The results suggest that either local stimulation of endothelium with cytokines or lymphocyte activation in the periphery will modulate lymphocyte traffic into brain.

摘要

在体外研究了控制淋巴细胞与脑内皮细胞黏附的因素。淋巴细胞的丝裂原激活导致其与内皮细胞的黏附增加,在7 - 24小时达到最大值,细胞分裂后降至正常水平,且这一过程需要蛋白质合成。大鼠脑内皮细胞可用γ干扰素刺激,以增加其与正常或活化淋巴细胞的黏附。内皮细胞对低水平细胞因子敏感:刺激后黏附迅速形成,且需要新的蛋白质合成。抗原特异性系细胞也比正常淋巴结细胞更有效地黏附于内皮细胞。内皮细胞经γ干扰素处理可增强这种黏附,在存在同源抗原的情况下黏附进一步略有增加。结果表明,细胞因子对内皮细胞的局部刺激或外周淋巴细胞的激活都会调节淋巴细胞向脑内的迁移。

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