Boone David L, Turer Emre E, Lee Eric G, Ahmad Regina-Celeste, Wheeler Matthew T, Tsui Colleen, Hurley Paula, Chien Marcia, Chai Sophia, Hitotsumatsu Osamu, McNally Elizabeth, Pickart Cecile, Ma Averil
Department of Medicine, University of California at San Francisco, San Francisco, California 94143-0451, USA.
Nat Immunol. 2004 Oct;5(10):1052-60. doi: 10.1038/ni1110. Epub 2004 Aug 29.
A20 is a cytoplasmic protein required for the termination of tumor necrosis factor (TNF)-induced signals. We show here that mice doubly deficient in either A20 and TNF or A20 and TNF receptor 1 developed spontaneous inflammation, indicating that A20 is also critical for the regulation of TNF-independent signals in vivo. A20 was required for the termination of Toll-like receptor-induced activity of the transcription factor NF-kappaB and proinflammatory gene expression in macrophages, and this function protected mice from endotoxic shock. A20 accomplished this biochemically by directly removing ubiquitin moieties from the signaling molecule TRAF6. The critical function of this deubiquitinating enzyme in the restriction of TLR signals emphasizes the importance of the regulation of ubiquitin conjugation in innate immune cells.
A20是一种细胞质蛋白,是肿瘤坏死因子(TNF)诱导信号终止所必需的。我们在此表明,A20和TNF双缺陷或A20和肿瘤坏死因子受体1双缺陷的小鼠会发生自发性炎症,这表明A20对于体内TNF非依赖性信号的调节也至关重要。A20是巨噬细胞中Toll样受体诱导的转录因子NF-κB活性终止和促炎基因表达所必需的,该功能可保护小鼠免受内毒素休克。A20通过直接从信号分子TRAF6上去除泛素部分来实现这一生物化学过程。这种去泛素化酶在限制TLR信号中的关键功能强调了先天免疫细胞中泛素缀合调节的重要性。
Zotero 插件