Nucleolar Localization and Dynamic Roles of Flap Endonuclease 1 in Ribosomal DNA Replication and Damage Repair

Author:

Guo Zhigang1,Qian Limin1,Liu Ren1,Dai Huifang1,Zhou Mian1,Zheng Li1,Shen Binghui1

Affiliation:

1. Department of Radiation Biology, City of Hope National Medical Center and Beckman Research Institute, Duarte, California 91010

Abstract

ABSTRACT Despite the wealth of information available on the biochemical functions and our recent findings of its roles in genome stability and cancer avoidance of the structure-specific flap endonuclease 1 (FEN1), its cellular compartmentalization and dynamics corresponding to its involvement in various DNA metabolic pathways are not yet elucidated. Several years ago, we demonstrated that FEN1 migrates into the nucleus in response to DNA damage and under certain cell cycle conditions. In the current paper, we found that FEN1 is superaccumulated in the nucleolus and plays a role in the resolution of stalled DNA replication forks formed at the sites of natural replication fork barriers. In response to UV irradiation and upon phosphorylation, FEN1 migrates to nuclear plasma to participate in the resolution of UV cross-links on DNA, most likely employing its concerted action of exonuclease and gap-dependent endonuclease activities. Based on yeast complementation experiments, the mutation of Ser 187 Asp, mimicking constant phosphorylation, excludes FEN1 from nucleolar accumulation. The replacement of Ser 187 by Ala, eliminating the only phosphorylation site, retains FEN1 in nucleoli. Both of the mutations cause UV sensitivity, impair cellular UV damage repair capacity, and decline overall cellular survivorship.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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