Sidrit Uruci, Nicole M Hoitsma, Maria E. Soler-Oliva, Aleix Bayona-Feliu, Vincent Gaggioli, Maria L. Garcia Rubio, Calvin S.Y. Lo, Collin Bakker, Jessica Marinello, Eleni Maria Manolika, Giovanni Capranico, Martijn S. Luijsterburg, Karolin Luger, Andres Aguilera, Nitika Taneja
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引用次数: 0
摘要
DNA 复制经常会遇到转录机制停滞和 R 环等障碍。核糖核酸酶和DNA-RNA螺旋酶可以解决这些结构,但染色质重塑者的作用仍未得到充分研究。通过一系列体外和体内实验,我们发现染色质重塑器 SMARCAD1 与活跃的复制叉相关联,对于解决附近的 R 环以维持复制叉的稳定性至关重要。SMARCAD1通过其ATPase结构域直接结合R环,并通过其N端区域与复制体结合。这两种相互作用对于解决细胞内的 R 环至关重要。全基因组检测显示,表达突变体 SMARCAD1 的细胞比野生型细胞积累了更多的 R-环,尤其是在与已知叉阻断易发位点不同的区域。在种系肿瘤中,SMARCAD1突变体中的这些R环富集区也表现出更多的突变,表明它们是癌症突变的热点。因此,SMARCAD1 在积极进展的分叉中充当 R 环传感器和解旋酶,维持基因组稳定并防止肿瘤发生。
SMARCAD1 Regulates R-Loops at Active Replication Forks Linked to Cancer Mutation Hotspots
DNA replication often encounters obstacles like the stalled transcription machinery and R-loops. While ribonucleases and DNA-RNA helicases can resolve these structures, the role of chromatin remodelers remains understudied. Through a series of in vitro and in vivo experiments, we show that the chromatin remodeler SMARCAD1, which associates with active replication forks, is crucial for resolving nearby R-loops to maintain fork stability. SMARCAD1 directly binds R-loops via its ATPase domain and associates with the replisome through its N-terminus region. Both interactions are critical for resolving R-loops within cells. Genome-wide assays reveal that cells expressing mutant SMARCAD1 accumulate significantly more R-loops than wild-type cells, particularly in regions distinct from known fork blockage-prone sites. These R-loop-enriched regions in SMARCAD1 mutants also exhibit increased mutagenesis in germline tumors, suggesting they are mutation hotspots in cancer. Therefore, SMARCAD1 acts as an R-loop sensor and resolvase at actively progressing forks, maintaining genome stability and preventing tumorigenesis.