Department of Microbiology-Immunology, Lineberger Comprehensive Cancer Center, University of North Carolina, Chapel Hill, North Carolina 27599-7295, USA.
J Biol Chem. 2011 Feb 11;286(6):4098-106. doi: 10.1074/jbc.M110.147371. Epub 2010 Nov 19.
Heightened DJ-1 (Park7) expression is associated with a reduction in chemotherapeutic-induced cell death and poor prognosis in several cancers, whereas the loss of DJ-1 function is found in a subgroup of Parkinson disease associated with neuronal death. This study describes a novel pathway by which DJ-1 modulates cell survival. Mass spectrometry shows that DJ-1 interacts with BBS1, CLCF1, MTREF, and Cezanne/OTUD7B/Za20d1. Among these, Cezanne is a known deubiquitination enzyme that inhibits NF-κB activity. DJ-1/Cezanne interaction is confirmed by co-immunoprecipitation of overexpressed and endogenous proteins, maps to the amino-terminal 70 residues of DJ-1, and leads to the inhibition of the deubiquitinating activity of Cezanne. Microarray profiling of shRNA-transduced cells shows that DJ-1 and Cezanne regulate IL-8 and ICAM-1 expression in opposing directions. Similarly, DJ-1 enhances NF-κB nuclear translocation and cell survival, whereas Cezanne reduces these outcomes. Analysis of mouse Park7(-/-) primary cells confirms the regulation of ICAM-1 by DJ-1 and Cezanne. As NF-κB is important in cellular survival and transformation, IL-8 functions as an angiogenic factor and pro-survival signal, and ICAM-1 has been implicated in tumor progression, invasion, and metastasis; these data provide an additional modality by which DJ-1 controls cell survival and possibly tumor progression via interaction with Cezanne.
高度表达的 DJ-1(Park7)与几种癌症中化疗诱导的细胞死亡减少和预后不良有关,而 DJ-1 功能的丧失则存在于与神经元死亡相关的帕金森病亚组中。本研究描述了 DJ-1 调节细胞存活的新途径。质谱分析表明,DJ-1 与 BBS1、CLC-F1、MTREF 和 Cezanne/OTUD7B/Za20d1 相互作用。其中,Cezanne 是一种已知的去泛素化酶,可抑制 NF-κB 活性。DJ-1/Cezanne 相互作用通过过表达和内源性蛋白质的共免疫沉淀来证实,该相互作用定位于 DJ-1 的氨基端 70 个残基,并导致 Cezanne 的去泛素化活性受到抑制。shRNA 转导细胞的微阵列分析表明,DJ-1 和 Cezanne 以相反的方向调节 IL-8 和 ICAM-1 的表达。同样,DJ-1 增强 NF-κB 核易位和细胞存活,而 Cezanne 则降低这些结果。对 Park7(-/-)小鼠原代细胞的分析证实了 DJ-1 和 Cezanne 对 ICAM-1 的调控。由于 NF-κB 在细胞存活和转化中很重要,IL-8 作为一种血管生成因子和生存信号发挥作用,而 ICAM-1 已被牵涉到肿瘤进展、侵袭和转移中;这些数据提供了一种额外的模式,通过与 Cezanne 的相互作用,DJ-1 控制细胞存活并可能控制肿瘤进展。