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首页> 外文期刊>Neoplasia: an international journal for oncology research >Telomeric Recombination Induced by DNA Damage Results in Telomere Extension and Length Heterogeneity
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Telomeric Recombination Induced by DNA Damage Results in Telomere Extension and Length Heterogeneity

机译:DNA损伤诱导的端粒重组导致端粒延伸和长度异质性

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摘要

About 15% of human cancers counteract telomere loss by alternative lengthening of telomeres (ALT), which is attributed to homologous recombination (HR)–mediated events. But how telomeric HR leads to length elongation is poorly understood. Here, we explore telomere clustering and telomeric HR induced by double-stranded breaks (DSBs). We show that telomere clustering could occur at G1 and S phase of cell cycle and that three types of telomeric HR occur based on the manner of telomeric DNA exchange: equivalent telomeric sister chromatin exchange (T-SCE), inequivalent T-SCE, and No-SCE. While inequivalent T-SCE increases telomere length heterogeneity with no net gain of telomere length, No-SCE, which is presumably induced by interchromatid HR and/or break-induced replication, results in telomere elongation. Accordingly, cells subjected to long-term telomeric DSBs display increased heterogeneity of length and longer telomeres. We also demonstrate that DSBs-induced telomere elongation is telomerase independent. Moreover, telomeric recombination induced by DSBs is associated with formation of ALT-associated PML body and C-circle. Thus, DNA damage triggers recombination mediated elongation, leading to the induction of multiple ALT phenotypes.
机译:约15%的人类癌症通过端粒的替代性延长(ALT)来抵消端粒的丧失,这是由于同源重组(HR)介导的事件。但是,端粒HR如何导致长度延长的认识很少。在这里,我们探讨由双链断裂(DSBs)诱导的端粒聚集和端粒HR。我们显示端粒聚类可能发生在细胞周期的G1和S期,并且基于端粒DNA交换的方式发生了三种类型的端粒HR:当量端粒姊妹染色质交换(T-SCE),不等价T-SCE和No -SCE。虽然不等价的T-SCE增加了端粒长度的异质性,而没有端粒长度的净增加,但是No-SCE可能是由染色质间HR和/或断裂诱导的复制诱导的,导致端粒伸长。因此,经受长期端粒DSB的细胞显示出增加的长度异质性和更长的端粒。我们还证明了DSBs诱导的端粒延长是端粒酶独立的。此外,DSBs诱导的端粒重组与ALT相关的PML体和C环的形成有关。因此,DNA损伤触发了重组介导的延伸,导致多种ALT表型的诱导。

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