Regamey Alexandre, Hohl Daniel, Liu Jia Wei, Roger Thierry, Kogerman Priit, Toftgard Rune, Huber Marcel
Department of Dermatology, CHUV, Lausanne, Switzerland.
J Exp Med. 2003 Dec 15;198(12):1959-64. doi: 10.1084/jem.20031187.
Cylindromas are benign adnexal skin tumors caused by germline mutations in the CYLD gene. In most cases the second wild-type allele is lost in tumor tissue, suggesting that CYLD functions as tumor suppressor. CYLD is a protein of 956 amino acids harboring a functional deubiquitinating domain at the COOH-terminal end. To shed more light on the function of CYLD, we have performed a yeast two hybrid screen using an HaCaT cDNA library that identified the RING finger protein TRIP (TRAF-interacting protein) as interactor with full-length CYLD. Mapping of the interacting domains revealed that the central domain of CYLD binds to the COOH-terminal end of TRIP. Far Western analysis and coimmunoprecipitations in mammalian cells confirmed that full-length CYLD binds to the COOH-terminal domain of TRIP. Because TRIP is an inhibitor of nuclear factor (NF)-kappaB activation by tumor necrosis factor (TNF), the effect of CYLD on NF-kappaB activation was investigated in HeLa cells. The results established that CYLD down-regulates NF-kappaB activation by TNF-alpha. The inhibition by CYLD depends on the presence of the central domain interacting with TRIP and its deubiquitinating activity. These findings indicate that cylindromas arise through constitutive NF-kappaB activation leading to hyperproliferation and tumor growth.
圆柱瘤是由CYLD基因种系突变引起的良性附属器皮肤肿瘤。在大多数情况下,肿瘤组织中第二个野生型等位基因缺失,这表明CYLD起着肿瘤抑制作用。CYLD是一种含有956个氨基酸的蛋白质,在COOH末端具有功能性去泛素化结构域。为了更深入了解CYLD的功能,我们使用HaCaT cDNA文库进行了酵母双杂交筛选,该筛选鉴定出环状结构域蛋白TRIP(TRAF相互作用蛋白)为全长CYLD的相互作用蛋白。相互作用结构域的定位显示CYLD的中央结构域与TRIP的COOH末端结合。哺乳动物细胞中的Far Western分析和免疫共沉淀证实全长CYLD与TRIP的COOH末端结构域结合。由于TRIP是肿瘤坏死因子(TNF)激活核因子(NF)-κB的抑制剂,因此在HeLa细胞中研究了CYLD对NF-κB激活的影响。结果表明CYLD下调TNF-α介导的NF-κB激活。CYLD的抑制作用取决于与TRIP相互作用的中央结构域的存在及其去泛素化活性。这些发现表明圆柱瘤是通过组成性NF-κB激活导致细胞过度增殖和肿瘤生长而产生的。
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