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Inhibition of p53 and/or AKT as a new therapeutic approach specifically targeting ALT cancers
Yuanlong Ge, Shu Wu, Zepeng Zhang, Xiaocui Li, Feng Li, Siyu Yan, Haiying Liu, Junjiu Huang, Yong Zhao
Protein Cell. 2019, 10 (11): 808-824.
https://doi.org/10.1007/s13238-019-0634-z
While the majority of all human cancers counteract telomere shortening by expressing telomerase,∼15% of all cancers maintain telomere length by a telomeraseindependent mechanism known as alternative lengthening of telomeres (ALT). Here, we show that high load of intrinsic DNA damage is present in ALT cancer cells, leading to apoptosis stress by activating p53-independent, but JNK/c-Myc-dependent apoptotic pathway. Notably, ALT cells expressing wild-type p53 show much lower apoptosis than p53-deficient ALT cells. Mechanistically, we find that intrinsic DNA damage in ALT cells induces low level of p53 that is insufficient to initiate the transcription of apoptosis-related genes, but is sufficient to stimulate the expression of key components of mTORC2 (mTOR and Rictor), which in turn leads to phosphorylation of AKT. Activated AKT (p-AKT) thereby stimulates downstream anti-apoptotic events. Therefore, p53 and AKT are the key factors that suppress spontaneous apoptosis in ALT cells. Indeed, inhibition of p53 or AKT selectively induces rapid death of ALT cells in vitro, and p53 inhibitor severely suppresses the growth of ALT-cell xenograft tumors in mice. These findings reveal a previously unrecognized function of p53 in antiapoptosis and identify that the inhibition of p53 or AKT has a potential as therapeutics for specifically targeting ALT cancers.
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Multiple sgRNAs facilitate base editingmediated i-stop to induce complete and precise gene disruption
Kun Jia, Zongyang Lu, Fei Zhou, Zhiqi Xiong, Rui Zhang, Zhiwei Liu, Yu’e Ma, Lei He, Cong Li, Zhen Zhu, Dejing Pan, Zhengxing Lian
Protein Cell. 2019, 10 (11): 832-839.
https://doi.org/10.1007/s13238-019-0611-6
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Analysis of VISTA expression and function in renal cell carcinoma highlights VISTA as a potential target for immunotherapy
Shanjuan Hong, Qing Yuan, Haizhui Xia, Genzhen Zhu, Yu Feng, Qiang Wang, Zhiyin Zhang, Wei He, Jian Lu, Chen Dong, Ling Ni
Protein Cell. 2019, 10 (11): 840-845.
https://doi.org/10.1007/s13238-019-0642-z
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DJ-1 is dispensable for human stem cell homeostasis
Fang Cheng, Si Wang, Moshi Song, Zunpeng Liu, Ping Liu, Lei Wang, Yanjiang Wang, Qian Zhao, Kaowen Yan, Piu Chan, Weiqi Zhang, Jing Qu, Guang-Hui Liu
Protein Cell. 2019, 10 (11): 846-853.
https://doi.org/10.1007/s13238-019-00659-9
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9 articles
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