论文
论文标题:Incorporation of a nucleoside analog maps genome repair sites in postmitotic human neurons
作者:Dylan A. Reid , Patrick J. Reed , Johannes C. M. Schlachetzki , Ioana I. Nitulescu , Grace Chou , Enoch C. Tsui , Jeffrey R. Jones , Sahaana Chandran , Ake T. Lu , Claire A. McClain , Jean H. Ooi , Tzu-Wen Wang , Addison J. Lana , Sara B. Linker , Anthony S. Ricciardulli , Shong Lau , Simon T. Schafer , Steve Horvath , Jesse R. Dixon , Nasun Hah , Christopher K. Glass , Fred H. Gage
期刊:Science
发表时间:2021/04/02
数字识别码:10.1126/science.abb9032
摘要:Neurons are the longest-lived cells in our bodies and lack DNA replication, which makes them reliant on a limited repertoire of DNA repair mechanisms to maintain genome fidelity. These repair mechanisms decline with age, but we have limited knowledge of how genome instability emerges and what strategies neurons and other long-lived cells may have evolved to protect their genomes over the human life span. A targeted sequencing approach in human embryonic stem cell–induced neurons shows that, in neurons, DNA repair is enriched at well-defined hotspots that protect essential genes. These hotspots are enriched with histone H2A isoforms and RNA binding proteins and are associated with evolutionarily conserved elements of the human genome. These findings provide a basis for understanding genome integrity as it relates to aging and disease in the nervous system.
