FADD是受体Fas下游的多个信号事件所必需的。

P Juo, M S Woo, C J Kuo, P Signorelli, H P Biemann, Y A Hannun, J Blenis
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引用次数: 0

摘要

为了确定fas诱导的凋亡信号通路的重要组成部分,研究人员对Jurkat T淋巴细胞进行了化学诱变,并选择了对fas诱导的凋亡具有抗性的克隆。我们获得了5个在接头FADD中含有突变的细胞系。免疫印迹分析显示,这5种细胞系均未表达FADD,对fas诱导的死亡具有完全抗性。FADD突变细胞系与野生型FADD互补可恢复fas介导的细胞凋亡。Fas对caspase-2、caspase-3、caspase-7和caspase-8的激活以及底物如BID、蛋白激酶Cdelta和聚(adp核糖)聚合酶的蛋白水解裂解在FADD突变细胞系中完全缺陷。此外,Fas对应激激酶p38和c-Jun NH2激酶的激活以及Fas连接反应中神经酰胺的产生在FADD突变细胞系中被阻断。这些数据表明FADD对Fas下游的多个信号事件至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
FADD is required for multiple signaling events downstream of the receptor Fas.

To identify essential components of the Fas-induced apoptotic signaling pathway, Jurkat T lymphocytes were chemically mutagenized and selected for clones that were resistant to Fas-induced apoptosis. We obtained five cell lines that contain mutations in the adaptor FADD. All five cell lines did not express FADD by immunoblot analysis and were completely resistant to Fas-induced death. Complementation of the FADD mutant cell lines with wild-type FADD restored Fas-mediated apoptosis. Fas activation of caspase-2, caspase-3, caspase-7, and caspase-8 and the proteolytic cleavage of substrates such as BID, protein kinase Cdelta, and poly(ADP-ribose) polymerase were completely defective in the FADD mutant cell lines. In addition, Fas activation of the stress kinases p38 and c-Jun NH2 kinase and the generation of ceramide in response to Fas ligation were blocked in the FADD mutant cell lines. These data indicate that FADD is essential for multiple signaling events downstream of Fas.

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