The Processing of Holliday Junctions by BLM and WRN Helicases Is Regulated by p53

BLM, WRN, and p53 are involved in the homologous DNA recombination pathway. The DNA structure-specific helicases, BLM and WRN, unwind Holliday junctions (HJ), an activity that could suppress inappropriate homologous recombination during DNA replication. Here, we show that purified, recombinant p53 b...

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Veröffentlicht in:The Journal of biological chemistry 2002-08, Vol.277 (35), p.31980-31987
Hauptverfasser: Yang, Qin, Zhang, Ran, Wang, Xin Wei, Spillare, Elisa A, Linke, Steven P, Subramanian, Deepa, Griffith, Jack D, Li, Ji Liang, Hickson, Ian D, Shen, Jiang Cheng, Loeb, Lawrence A, Mazur, Sharlyn J, Appella, Ettore, Brosh, Jr, Robert M, Karmakar, Parimal, Bohr, Vilhelm A, Harris, Curtis C
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Sprache:eng
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Zusammenfassung:BLM, WRN, and p53 are involved in the homologous DNA recombination pathway. The DNA structure-specific helicases, BLM and WRN, unwind Holliday junctions (HJ), an activity that could suppress inappropriate homologous recombination during DNA replication. Here, we show that purified, recombinant p53 binds to BLM and WRN helicases and attenuates their ability to unwind synthetic HJ in vitro . The p53 248W mutant reduces abilities of both to bind HJ and inhibit helicase activities, whereas the p53 273H mutant loses these abilities. Moreover, full-length p53 and a C-terminal polypeptide (residues 373–383) inhibit the BLM and WRN helicase activities, but phosphorylation at Ser 376 or Ser 378 completely abolishes this inhibition. Following blockage of DNA replication, Ser 15 phospho-p53, BLM, and RAD51 colocalize in nuclear foci at sites likely to contain DNA replication intermediates in cells. Our results are consistent with a novel mechanism for p53-mediated regulation of DNA recombinational repair that involves p53 post-translational modifications and functional protein-protein interactions with BLM and WRN DNA helicases.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.M204111200