4.7 Article

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

期刊

FASEB JOURNAL
卷 33, 期 2, 页码 2301-2313

出版社

FEDERATION AMER SOC EXP BIOL
DOI: 10.1096/fj.201801379R

关键词

DNA damage; PML nuclear bodies; superresolution microscopy

资金

  1. Polish Ministry of Science and Higher Education
  2. Polish National Science Centre (NCN) [2013/09/N/NZ3/00203, 2013/11/B/NZ3/00189, 2017/27/B/NZ3/01065]
  3. Jagiellonian University
  4. U.S. National Institutes of Health, National Institute on Drug Abuse [U01 DA-040588]
  5. National Science Centre [DEC-2015/16/T/NZ3/00157]

向作者/读者索取更多资源

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 a peripheral layer, and XRCC1 in the center. They also contain other factors, including PML, poly(ADP-ribose) polymerase 1 (PARP1), ligase III, and origin recognition complex subunit 5. The breast cancer 1 and -2 C terminus domains of XRCC1 are essential for formation of these repair foci. These results reveal that XRCC1-contaning foci constitute newly recognized PML-like nuclear bodies that accrete and locally deliver essential factors for repair of single-strand DNA breaks in replication regions.Kordon, M. M., Szczurek, A., Berniak, K., Szelest, O., Solarczyk, K., Tworzydo, M., Wachsmann-Hogiu, S., Vaahtokari, A., Cremer, C., Pederson, T., Dobrucki, J. W. PML-like subnuclear bodies, containing XRCC1, juxtaposed to DNA replication-based single-strand breaks.

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