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淋巴细胞“体外”运动:生长激活剂和趋化因子的作用

Lymphocyte locomotion "in vitro": the role of growth activators and chemoattractants.

作者信息

Wilkinson P C

机构信息

Bacteriology and Immunology Department, University of Glasgow (Western Infirmary), U.K.

出版信息

Biomed Pharmacother. 1987;41(6):329-36.

PMID:3328629
Abstract

Studies of lymphocyte locomotion in vitro are reviewed. This locomotion is important (a) for recirculation and the traversing of high endothelial venules in lymphoid tissue; (b) for recruitment of lymphocytes into inflammatory sites. In the latter situation, activated lymphocytes migrate more actively than resting lymphocytes. Our studies indicate that lymphocyte activators such as PHA, anti-CD3 antibodies, or the Cowan staphylococcus confer locomotor capacity on populations of human blood lymphocytes which, in the resting state, are immotile. Locomotor capacity is acquired in the G1 phase of growth and requires protein and RNA synthesis but not DNA synthesis. Anti-CD3-driven locomotor activation is inhibited by cyclosporin A, suggesting that new gene expression is required. The mitogens do not act directly as locomotor stimulants, i.e. they are not themselves chemotactic or chemokinetic factors. Rather they activate the potential for motility of lymphocytes and also cause release of lymphokines which are the direct stimulants for locomotion. One of these lymphokines (lymphocyte chemotactic factor: LCF) has been partially characterized.

摘要

本文综述了淋巴细胞体外运动的研究。这种运动具有重要意义:(a) 对于淋巴细胞在淋巴组织中的再循环以及穿越高内皮微静脉而言;(b) 对于淋巴细胞募集至炎症部位而言。在后一种情况下,活化的淋巴细胞比静息淋巴细胞迁移更为活跃。我们的研究表明,淋巴细胞激活剂,如植物血凝素(PHA)、抗CD3抗体或考恩葡萄球菌,可赋予人血淋巴细胞群体运动能力,而这些淋巴细胞在静息状态下是不运动的。运动能力在生长的G1期获得,且需要蛋白质和RNA合成,但不需要DNA合成。抗CD3驱动的运动激活受到环孢素A的抑制,这表明需要新的基因表达。这些促有丝分裂原并非直接作为运动刺激剂起作用,即它们本身不是趋化因子或化学动力因子。相反,它们激活淋巴细胞的运动潜能,并导致淋巴因子释放,而淋巴因子是运动的直接刺激物。其中一种淋巴因子(淋巴细胞趋化因子:LCF)已得到部分表征。

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