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Cancer-mutated ribosome protein L22 (RPL22/eL22) suppresses cancer cell survival by blocking p53-MDM2 circuit  期刊论文  

  • 编号:
    67820138-0f6a-4db6-86b9-50c5e7410cea
  • 作者:
    Cao, Bo[1];Fang, Ziling[1,2];Liao, Peng[1];Zhou, Xiang(周祥)[1,3,4]Xiong, Jianping[2];Zeng, Shelya[1];Lu, Hua[1];
  • 语种:
    English
  • 期刊:
    ONCOTARGET ISSN:1949-2553 2017 年 8 卷 53 期 (90651 - 90661) ; OCT 31
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  • 摘要:

    Several ribosomal proteins (RPs) in response to various ribosomal stressors have been shown to play a critical role in p53-dependent regulation of cell cycle arrest, apoptosis and tumor suppression. Here, we report ribosomal protein L22 (RPL22/eL22) as a novel p53 activator highly mutated (mostly deletion mutation) in various types of human cancers, but not essential for ribosomal biogenesis in normal cells. Ectopic expression of RPL22/eL22 suppressed the colony formation of cancer cells in a p53-dependent manner, whereas knockdown of RPL22/eL22 significantly compromised p53 activation by Actinomycin D, rescuing p53-induced G1/G0 cell cycle arrest. Interestingly, human tumors with RPL22/eL22 deletion appeared to sustain wild type p53. Mechanistically, RPL22/eL22 bound to MDM2 acidic domain and inhibited MDM2-mediated p53 ubiquitination and degradation, hence extending the half-life of p53. Ribosome-profiling analysis revealed that induction of ribosomal stress by Actinomycin D leads to the increase of ribosome-free RPL22/eL22 pool. Also, RPL22/eL22 formed a complex with MDM2/RPL5/uL18/RPL11/uL5 and synergized with RPL11/uL5 to activate p53. Furthermore, the N terminus of RPL22/eL22 bound to MDM2, while the C terminus interacted with RPL5/uL18/RPL11/uL5; both of these two fragments activated p53 by inhibiting MDM2. Our study indicates that RPL22/eL22 highly mutated in human cancers plays an anti-cancer role likely through regulation of the MDM2-p53 feedback loop, and also suggests that targeting the RPL22/eL22MDM2- p53 pathway could be a potential strategy for future development of anticancer therapy.

  • 推荐引用方式
    GB/T 7714:
    Cao Bo,Fang Ziling,Liao Peng, et al. Cancer-mutated ribosome protein L22 (RPL22/eL22) suppresses cancer cell survival by blocking p53-MDM2 circuit [J].ONCOTARGET,2017,8(53):90651-90661.
  • APA:
    Cao Bo,Fang Ziling,Liao Peng,Zhou Xiang,&Lu Hua.(2017).Cancer-mutated ribosome protein L22 (RPL22/eL22) suppresses cancer cell survival by blocking p53-MDM2 circuit .ONCOTARGET,8(53):90651-90661.
  • MLA:
    Cao Bo, et al. "Cancer-mutated ribosome protein L22 (RPL22/eL22) suppresses cancer cell survival by blocking p53-MDM2 circuit" .ONCOTARGET 8,53(2017):90651-90661.
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