Division of Tumor Biology and Immunology, The Netherlands Cancer Institute, Amsterdam, The Netherlands.
Department of Clinical Genetics, VU University Medical Center, Amsterdam, The Netherlands.
Elife. 2018 Oct 16;7:e37868. doi: 10.7554/eLife.37868.
In cancer cells, loss of G1/S control is often accompanied by p53 pathway inactivation, the latter usually rationalized as a necessity for suppressing cell cycle arrest and apoptosis. However, we found an unanticipated effect of p53 loss in mouse and human G1-checkpoint-deficient cells: reduction of DNA damage. We show that abrogation of the G1/S-checkpoint allowed cells to enter S-phase under growth-restricting conditions at the expense of severe replication stress manifesting as decelerated DNA replication, reduced origin firing and accumulation of DNA double-strand breaks. In this system, loss of p53 allowed mitogen-independent proliferation, not by suppressing apoptosis, but rather by restoring origin firing and reducing DNA breakage. Loss of G1/S control also caused DNA damage and activation of p53 in an retinoblastoma model. Moreover, in a teratoma model, loss of p53 reduced DNA breakage. Thus, loss of p53 may promote growth of incipient cancer cells by reducing replication-stress-induced DNA damage.
在癌细胞中,G1/S 控制的丧失通常伴随着 p53 通路失活,后者通常被合理化为抑制细胞周期阻滞和细胞凋亡的必要性。然而,我们在小鼠和人 G1 检查点缺陷细胞中发现了 p53 缺失的一个意外影响:降低了 DNA 损伤。我们表明,G1/S 检查点的消除允许细胞在生长受限的条件下进入 S 期,代价是严重的复制应激,表现为 DNA 复制减速、起始点减少和 DNA 双链断裂的积累。在这个系统中,p53 的缺失允许有丝分裂原非依赖性增殖,不是通过抑制细胞凋亡,而是通过恢复起始点并减少 DNA 断裂。G1/S 控制的丧失也会导致视网膜母细胞瘤模型中的 DNA 损伤和 p53 的激活。此外,在畸胎瘤模型中,p53 的缺失减少了 DNA 断裂。因此,p53 的缺失可能通过减少复制应激诱导的 DNA 损伤来促进初期癌细胞的生长。
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