致癌性c-Myc诱导的淋巴瘤发生受到p19Arf-Mdm2-p53和RP-Mdm2-p53通路的非冗余抑制。
Oncogenic c-Myc-induced lymphomagenesis is inhibited non-redundantly by the p19Arf-Mdm2-p53 and RP-Mdm2-p53 pathways.
作者信息
Meng X, Carlson N R, Dong J, Zhang Y
机构信息
Department of Radiation Oncology, School of Medicine, The University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.
Lineberger Comprehensive Cancer Center, The University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.
出版信息
Oncogene. 2015 Nov 12;34(46):5709-17. doi: 10.1038/onc.2015.39. Epub 2015 Mar 30.
The multifaceted oncogene c-Myc plays important roles in the development and progression of human cancer. Recent in vitro and in vivo studies have shown that the p19Arf-Mdm2-p53 and the ribosomal protein (RP)-Mdm2-p53 pathways are both essential in preventing oncogenic c-Myc-induced tumorigenesis. Disruption of each pathway individually by p19Arf deletion or by Mdm2(C305F) mutation, which disrupts RP-Mdm2 binding, accelerates Eμ-myc transgene-induced pre-B/B-cell lymphoma in mice at seemingly similar paces with median survival around 10 and 11 weeks, respectively, compared to 20 weeks for Eμ-myc transgenic mice. Because p19Arf can inhibit ribosomal biogenesis through its interaction with nucleophosmin (NPM/B23), RNA helicase DDX5 and RNA polymerase I transcription termination factor (TTF-I), it has been speculated that the p19Arf-Mdm2-p53 and the RP-Mdm2-p53 pathways might be a single p19Arf-RP-Mdm2-p53 pathway, in which p19Arf activates p53 by inhibiting RP biosynthesis; thus, p19Arf deletion or Mdm2(C305F) mutation would result in similar consequences. Here, we generated mice with concurrent p19Arf deletion and Mdm2(C305F) mutation and investigated the compound mice for tumorigenesis in the absence and the presence of oncogenic c-Myc overexpression. In the absence of Eμ-myc transgene, the Mdm2(C305F) mutation did not elicit spontaneous tumors in mice, nor did it accelerate spontaneous tumors in mice with p19Arf deletion. In the presence of Eμ-myc transgene, however, Mdm2(C305F) mutation significantly accelerated p19Arf deletion-induced lymphomagenesis and promoted rapid metastasis. We found that when p19Arf-Mdm2-p53 and RP-Mdm2-p53 pathways are independently disrupted, oncogenic c-Myc-induced p53 stabilization and activation is only partially attenuated. When both pathways are concurrently disrupted, however, c-Myc-induced p53 stabilization and activation are essentially obliterated. Thus, the p19Arf-Mdm2-p53 and the RP-Mdm2-p53 are non-redundant pathways possessing similar capabilities to activate p53 upon c-Myc overexpression.
多面癌基因c-Myc在人类癌症的发生和发展中起着重要作用。最近的体外和体内研究表明,p19Arf-Mdm2-p53和核糖体蛋白(RP)-Mdm2-p53途径在预防致癌性c-Myc诱导的肿瘤发生中都至关重要。通过p19Arf缺失或Mdm2(C305F)突变分别破坏每条途径,其中Mdm2(C305F)突变会破坏RP-Mdm2结合,这会以看似相似的速度加速Eμ-myc转基因诱导的小鼠前B/B细胞淋巴瘤,中位生存期分别约为10周和11周,而Eμ-myc转基因小鼠的中位生存期为20周。由于p19Arf可以通过与核磷蛋白(NPM/B23)、RNA解旋酶DDX5和RNA聚合酶I转录终止因子(TTF-I)相互作用来抑制核糖体生物合成,因此有人推测p19Arf-Mdm2-p53和RP-Mdm2-p53途径可能是单一的p19Arf-RP-Mdm2-p53途径,其中p19Arf通过抑制RP生物合成来激活p53;因此,p19Arf缺失或Mdm2(C305F)突变会导致相似的结果。在这里,我们生成了同时缺失p19Arf和具有Mdm2(C305F)突变的小鼠,并研究了在不存在和存在致癌性c-Myc过表达的情况下复合小鼠的肿瘤发生情况。在没有Eμ-myc转基因的情况下,Mdm2(C305F)突变在小鼠中不会引发自发肿瘤,在p19Arf缺失的小鼠中也不会加速自发肿瘤的发生。然而,在存在Eμ-myc转基因的情况下,Mdm2(C305F)突变显著加速了p19Arf缺失诱导的淋巴瘤发生并促进了快速转移。我们发现,当p19Arf-Mdm2-p53和RP-Mdm2-p53途径被独立破坏时,致癌性c-Myc诱导的p53稳定和激活仅部分减弱。然而,当两条途径同时被破坏时,c-Myc诱导的p53稳定和激活基本上被消除。因此,p19Arf-Mdm2-p53和RP-Mdm2-p53是在c-Myc过表达时具有相似激活p53能力的非冗余途径。
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