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人类B淋巴细胞上MHC II类介导信号传导后的早期生化事件。

Early biochemical events after MHC class II-mediated signaling on human B lymphocytes.

作者信息

Mooney N A, Grillot-Courvalin C, Hivroz C, Ju L Y, Charron D

机构信息

Laboratoire d'Immunogénétique Moléculaire, Institut Biomédical des Cordeliers, Paris, France.

出版信息

J Immunol. 1990 Oct 1;145(7):2070-6.

PMID:2398273
Abstract

These studies examined the role of the MHC class II Ag in signal transduction using human B lymphocytes. Early events in signal transduction were considered including the intracellular calcium [Ca2+)i) flux, the activation of phospholipase C, and induction of protein phosphorylation. The (Ca2+)i was enhanced after incubation of B lymphocytes with several mAb anti-HLA class II and cross-linking with rabbit anti-mouse-F(ab')2. We have also demonstrated an enhancement of the (Ca2+)i in response to a suboptimal concentration of a monoclonal anti-IgM either in the presence of or after preincubation with a mAb anti-HLA class II. The activation of phospholipase C was assessed by measuring the generation of inositol phosphates in permeabilized B lymphocytes. mAb anti-HLA-class II of two different epitopes were used to demonstrate both the (Ca2+)i flux and the generation of inositol phosphates. Two-dimensional gel electrophoresis was used to investigate the phosphorylation pattern of resting B lymphocytes and the changes in the pattern after stimulation with soluble mAb anti-HLA-DR, immobilized mAb anti-HLA-DR, and PMA. In addition to the augmentation of phosphorylation observed with regard to phosphoproteins already present in resting B lymphocytes, new phosphorylations were observed after stimulation by any one of the reagents. Furthermore, stimulation by PMA did not result in an identical pattern to that observed after stimulation by mAb anti-HLA class II. An inhibition of the proliferative response to PMA was demonstrated after prestimulation of cells with immobilized mAb anti-HLA-DR, supporting the notion of a shared pathway of activation. In summary, these data demonstrate signal transduction via MHC class II Ag as assessed by three different measures of early events in human B lymphocyte activation and suggest that a protein kinase C pathway is at least partly involved.

摘要

这些研究利用人B淋巴细胞检验了MHCⅡ类抗原在信号转导中的作用。研究考虑了信号转导的早期事件,包括细胞内钙([Ca2+]i)通量、磷脂酶C的激活以及蛋白质磷酸化的诱导。用几种抗HLAⅡ类单克隆抗体(mAb)孵育人B淋巴细胞并与兔抗小鼠F(ab')2交联后,[Ca2+]i增强。我们还证明,在存在抗HLAⅡ类mAb或用其预孵育后,对次优浓度的抗IgM单克隆抗体反应时,[Ca2+]i也会增强。通过测量通透化B淋巴细胞中肌醇磷酸的生成来评估磷脂酶C的激活。使用两种不同表位的抗HLAⅡ类mAb来证明[Ca2+]i通量和肌醇磷酸的生成。二维凝胶电泳用于研究静息B淋巴细胞的磷酸化模式以及用可溶性抗HLA-DR mAb、固定化抗HLA-DR mAb和佛波酯(PMA)刺激后模式的变化。除了观察到静息B淋巴细胞中已存在的磷蛋白磷酸化增加外,在用任何一种试剂刺激后还观察到了新的磷酸化。此外,PMA刺激产生的模式与抗HLAⅡ类mAb刺激后观察到的模式不同。在用固定化抗HLA-DR mAb预刺激细胞后,证明对PMA的增殖反应受到抑制,这支持了存在共同激活途径的观点。总之,这些数据通过人B淋巴细胞激活早期事件的三种不同测量方法证明了经由MHCⅡ类抗原的信号转导,并表明蛋白激酶C途径至少部分参与其中。

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