Deschênes-Simard Xavier, Lessard Frédéric, Gaumont-Leclerc Marie-France, Bardeesy Nabeel, Ferbeyre Gerardo
Department of Biochemistry and Molecular Medicine; Université de Montréal; Montréal, Québec, Canada.
Massachusetts General Hospital Cancer Center; Harvard Medical School; Boston, MA USA.
Cell Cycle. 2014;13(12):1840-58. doi: 10.4161/cc.29335. Epub 2014 May 27.
Autophagy and the ubiquitin-proteasome pathway (UPP) are the major protein degradation systems in eukaryotic cells. Whereas the former mediate a bulk nonspecific degradation, the UPP allows a rapid degradation of specific proteins. Both systems have been shown to play a role in tumorigenesis, and the interest in developing therapeutic agents inhibiting protein degradation is steadily growing. However, emerging data point to a critical role for autophagy in cellular senescence, an established tumor suppressor mechanism. Recently, a selective protein degradation process mediated by the UPP was also shown to contribute to the senescence phenotype. This process is tightly regulated by E3 ubiquitin ligases, deubiquitinases, and several post-translational modifications of target proteins. Illustrating the complexity of UPP, more than 600 human genes have been shown to encode E3 ubiquitin ligases, a number which exceeds that of the protein kinases. Nevertheless, our knowledge of proteasome-dependent protein degradation as a regulated process in cellular contexts such as cancer and senescence remains very limited. Here we discuss the implications of protein degradation in senescence and attempt to relate this function to the protein degradation pattern observed in cancer cells.
自噬和泛素 - 蛋白酶体途径(UPP)是真核细胞中的主要蛋白质降解系统。前者介导大量非特异性降解,而UPP则允许特定蛋白质的快速降解。这两个系统均已被证明在肿瘤发生中起作用,并且开发抑制蛋白质降解的治疗剂的兴趣正在稳步增长。然而,新出现的数据表明自噬在细胞衰老(一种既定的肿瘤抑制机制)中起关键作用。最近,由UPP介导的选择性蛋白质降解过程也被证明有助于衰老表型。这个过程受到E3泛素连接酶、去泛素化酶和靶蛋白的几种翻译后修饰的严格调控。说明了UPP的复杂性,已证明超过600个人类基因编码E3泛素连接酶,这一数量超过了蛋白激酶的数量。然而,我们对蛋白酶体依赖性蛋白质降解作为癌症和衰老等细胞环境中的一种受调控过程的了解仍然非常有限。在这里,我们讨论蛋白质降解在衰老中的意义,并试图将这种功能与在癌细胞中观察到的蛋白质降解模式联系起来。
