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PML-like subnuclear bodies, containing XRCC1, juxtaposed to DNA replication-based single-strand breaks.

FASEB J.. 2018-09; 
KordonMagdalena M,SzczurekAleksander,BerniakKrzysztof,SzelestOskar,SolarczykKamil,TworzydłoMagdalena,Wachsmann-HogiuSebastian,VaahtokariAnne,CremerChristoph,PedersonThoru,DobruckiJur
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Gene Synthesis … Other vectors used in the major experiments contained the correct gene encoding XRCC1; it was ordered and synthe- sized by GenScript (Piscataway, NJ, USA) and subcloned into empty vectors pEGFP-C2 (Clontech Laboratories, Mountain View, CA, USA), and pmRFP-C1 … Get A Quote

摘要

DNA lesions induce recruitment and accumulation of various repair factors, resulting in formation of discrete nuclear foci. Using superresolution fluorescence microscopy as well as live cell and quantitative imaging, we demonstrate that X-ray repair cross-complementing protein 1 (XRCC1), a key factor in single-strand break and base excision repair, is recruited into nuclear bodies formed in response to replication-related single-strand breaks. Intriguingly, these bodies are assembled immediately in the vicinity of these breaks and never fully colocalize with replication foci. They are structurally organized, containing canonical promyelocytic leukemia (PML) nuclear body protein SP100 concentrated in... More

关键词

DNA damage,PML nuclear bodies,superresolution micros