Towne Jennifer E, Garka Kirsten E, Renshaw Blair R, Virca G Duke, Sims John E
Amgen Corporation, Seattle, Washington 98101, USA.
J Biol Chem. 2004 Apr 2;279(14):13677-88. doi: 10.1074/jbc.M400117200. Epub 2004 Jan 20.
Interleukin 1 (IL-1) plays a prominent role in immune and inflammatory reactions. Our understanding of the IL-1 family has recently expanded to include six novel members named IL-1F5 to IL-1F10. Recently, it was reported that IL-1F9 activated NF-kappaB through the orphan receptor IL-1 receptor (IL-1R)-related protein 2 (IL-1Rrp2) in Jurkat cells (Debets, R., Timans, J. C., Homey, B., Zurawski, S., Sana, T. R., Lo, S., Wagner, J., Edwards, G., Clifford, T., Menon, S., Bazan, J. F., and Kastelein, R. A. (2001) J. Immunol. 167, 1440-1446). In this study, we demonstrate that IL-1F6 and IL-1F8, in addition to IL-1F9, activate the pathway leading to NF-kappaB in an IL-1Rrp2-dependent manner in Jurkat cells as well as in multiple other human and mouse cell lines. Activation of the pathway leading to NF-kappaB by IL-1F6 and IL-1F8 follows a similar time course to activation by IL-1beta, suggesting that signaling by the novel family members occurs through a direct mechanism. In a mammary epithelial cell line, NCI/ADR-RES, which naturally expresses IL-1Rrp2, all three cytokines signal without further receptor transfection. IL-1Rrp2 antibodies block activation of the pathway leading to NF-kappaB by IL-1F6, IL-1F8, and IL-1F9 in both Jurkat and NCI/ADR-RES cells. In NCI/ADR-RES cells, the three IL-1 homologs activated the MAPKs, JNK and ERK1/2, and activated downstream targets as well, including an IL-8 promoter reporter and the secretion of IL-6. We also provide evidence that IL-1RAcP, in addition to IL-1Rrp2, is required for signaling by all three cytokines. Antibodies directed against IL-1RAcP and transfection of cytoplasmically deleted IL-1RAcP both blocked activation of the pathway leading to NF-kappaB by the three cytokines. We conclude that IL-1F6, IL-1F8, and IL-1F9 signal through IL-1Rrp2 and IL-1RAcP.
白细胞介素1(IL-1)在免疫和炎症反应中起重要作用。我们对IL-1家族的认识最近有所扩展,包括六个新成员,命名为IL-1F5至IL-1F10。最近有报道称,在Jurkat细胞中,IL-1F9通过孤儿受体白细胞介素1受体(IL-1R)相关蛋白2(IL-1Rrp2)激活核因子κB(Debets, R., Timans, J. C., Homey, B., Zurawski, S., Sana, T. R., Lo, S., Wagner, J., Edwards, G., Clifford, T., Menon, S., Bazan, J. F., and Kastelein, R. A. (2001) J. Immunol. 167, 1440 - 1446)。在本研究中,我们证明,除了IL-1F9之外,IL-1F6和IL-1F8在Jurkat细胞以及多种其他人和小鼠细胞系中,以依赖IL-1Rrp2的方式激活导致核因子κB的信号通路。IL-1F6和IL-1F8对导致核因子κB信号通路的激活与IL-1β激活的时间进程相似,这表明新家族成员的信号传导是通过直接机制发生的。在天然表达IL-1Rrp2的乳腺上皮细胞系NCI/ADR-RES中,所有三种细胞因子无需进一步转染受体即可发出信号。IL-1Rrp2抗体可阻断Jurkat细胞和NCI/ADR-RES细胞中IL-1F6、IL-1F8和IL-1F9对导致核因子κB信号通路的激活。在NCI/ADR-RES细胞中,这三种IL-1同源物激活了丝裂原活化蛋白激酶JNK和ERK1/2,并激活了下游靶点,包括IL-8启动子报告基因和IL-6的分泌。我们还提供证据表明,除了IL-1Rrp2之外,IL-1受体辅助蛋白(IL-1RAcP)也是这三种细胞因子信号传导所必需的。针对IL-1RAcP的抗体以及细胞质缺失的IL-1RAcP的转染均阻断了这三种细胞因子对导致核因子κB信号通路的激活。我们得出结论,IL-1F6、IL-1F8和IL-1F9通过IL-1Rrp2和IL-1RAcP发出信号。
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