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CD30 连接可诱导人 T 细胞系中的核因子-κB 激活。

CD30 ligation induces nuclear factor-kappa B activation in human T cell lines.

作者信息

McDonald P P, Cassatella M A, Bald A, Maggi E, Romagnani S, Gruss H J, Pizzolo G

机构信息

Department of General Pathology, University of Verona, Italy.

出版信息

Eur J Immunol. 1995 Oct;25(10):2870-6. doi: 10.1002/eji.1830251024.

Abstract

CD30 is a recently described member of the tumor necrosis factor/nerve growth factor receptor superfamily. In this report, we show that following incubation of L540 cells (Hodgkin's disease-derived, T cell-like, CD30+ cells) with the agonistic anti-CD30 monoclonal antibodies (mAb) M44 and M67, two nuclear factor (NF)-kappa B DNA binding activities were induced in nuclear extracts, as determined in gel retardation assays. The effect of the mAb towards NF-kappa B activation was rapid, as it occurred within 20 min, and was sustained for up to 6 h. By comparison, an isotype-matched antibody had no effect on NF-kappa B activation. Moreover, in human T helper (Th) clones functionally characterized as being of the type 0, type 1 and type 2 (28%, < 1% und 93% CD30+, respectively), the extent of CD30-mediated NF-kappa B activation correlated with the proportion of CD30+ cells. In all cell lines investigated, the NF-kappa B complexes induced following CD30 engagement were shown to contain p50 NF-kappa B1, p65 RelA, and possibly other transcription factors. Collectively, our results demonstrate that nuclear translocation and activation of NF-kappa B rank among the short-term cellular responses elicited following CD30 ligation.

摘要

CD30是肿瘤坏死因子/神经生长因子受体超家族中最近被描述的成员。在本报告中,我们显示,在用激动性抗CD30单克隆抗体(mAb)M44和M67孵育L540细胞(源自霍奇金病的T细胞样CD30+细胞)后,凝胶阻滞试验测定核提取物中诱导出两种核因子(NF)-κB DNA结合活性。mAb对NF-κB激活的作用迅速,在20分钟内即可发生,并持续长达6小时。相比之下,同型匹配抗体对NF-κB激活无影响。此外,在功能上被鉴定为0型、1型和2型(分别为28%、<1%和93% CD30+)的人T辅助(Th)克隆中,CD30介导的NF-κB激活程度与CD30+细胞比例相关。在所有研究的细胞系中,CD30参与后诱导的NF-κB复合物显示含有p50 NF-κB1、p65 RelA以及可能的其他转录因子。总体而言,我们的结果表明,NF-κB的核转位和激活是CD30连接后引发的短期细胞反应之一。

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