变色
端粒
生物
基因组不稳定性
染色体不稳定性
核分裂突变
细胞生物学
双着丝粒染色体
遗传学
DNA损伤
基因
DNA
染色体
核型
作者
Kez Cleal,Duncan M. Baird
标识
DOI:10.1016/j.tig.2020.02.001
摘要
When cells progress to malignancy, they must overcome a final telomere-mediated proliferative lifespan barrier called replicative crisis. Crisis is characterized by extensive telomere fusion that drives widespread genomic instability, mitotic arrest, hyperactivation of autophagy, and cell death. Recently, it has become apparent that that the resolution of dicentric chromosomes, which arise from telomere fusions during crisis, can initiate a sequence of events that leads to chromothripsis, a form of extreme genomic catastrophe. Chromothripsis is characterized by localized genomic regions containing tens to thousands of rearrangements and it is becoming increasingly apparent that chromothripsis occurs widely across tumor types and has a clinical impact. Here we discuss how telomere dysfunction can initiate genomic complexity and the emerging mechanisms of chromothripsis.
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