Department of Urology, Osaka City University Graduate School of Medicine, 1-4-3 Asahimachi, Abenoku, Osaka 545-8585, Japan.
Mol Oncol. 2012 Jun;6(3):267-75. doi: 10.1016/j.molonc.2012.01.003. Epub 2012 Jan 21.
Cancer cells can survive through the upregulation of cell cycle and the escape from apoptosis induced by numerous cellular stresses. In the normal cells, these biological cascades depend on scheduled proteolytic degradation of regulatory proteins via the ubiquitin-proteasome pathway. Therefore, interruption of regulated proteolytic pathways leads to abnormal cell-proliferation. Ubiquitin ligases called SCF complex (consisting of Skp-1, cullin, and F-box protein) or CRL (cullin-RING ubiquitin ligase) are predominant in a family of E3 ubiquitin ligases that control a final step in ubiquitination of diverse substrates. To a great extent, the ubiquitin ligase activity of the SCF complex requires the conjugation of NEDD8 to cullins, i.e. scaffold proteins. This review is anticipated to review the downregulation system of NEDD8 conjugation by several factors including a chemical compound such as MLN4924 and protein molecules (e.g. COP9 signalosome, inactive mutant of Ubc12, and NUB1/NUB1L). Since the downregulation of NEDD8 conjugation affects cell-cycle progression by inhibiting the ligase activity of SCF complexes, such knowledge in the NEDD8-conjugation pathway will contribute to the more magnificent therapies that selectively suppress tumorigenesis.
癌细胞可以通过细胞周期的上调和逃避许多细胞应激诱导的细胞凋亡而存活。在正常细胞中,这些生物级联反应依赖于通过泛素-蛋白酶体途径对调节蛋白进行预定的蛋白水解降解。因此,调节性蛋白水解途径的中断导致异常的细胞增殖。泛素连接酶称为 SCF 复合物(由 Skp1、cullin 和 F-box 蛋白组成)或 CRL(cullin-RING 泛素连接酶),是 E3 泛素连接酶家族中的主要成员,控制着各种底物泛素化的最后一步。在很大程度上,SCF 复合物的泛素连接酶活性需要将 NEDD8 连接到 cullins 上,即支架蛋白。本文预期将通过几种因素(包括 MLN4924 等化学化合物和 COP9 信号体、Ubc12 的无活性突变体以及 NUB1/NUB1L 等蛋白分子)综述 NEDD8 缀合的下调系统。由于 NEDD8 缀合的下调通过抑制 SCF 复合物的连接酶活性影响细胞周期进程,因此对 NEDD8 缀合途径的了解将有助于更具选择性地抑制肿瘤发生的更卓越的治疗方法。
