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DNA repair; chronological lifespan; oxidative DNA damage; reactive oxygen species; Schizosaccharomyces pombe
Defects of genome maintenance may causally contribute to aging. In general, base excision repair (BER) is involved in the repair of subtle base lesions and AP sites, and bulky helix-distorting lesions are restored by nucleotide excision repair (NER). Here, we measured the chronological lifespan (CLS) of BER- and NER-deficient mutants of the fission yeast Schizosaccharomyces pombe, and observed the aging process of cells. The CLS of the nth1 (gene for DNA glycosylase/AP lyase) mutant and the rad16 (a homolog of human XPF) mutant were slightly shorter than that of the wild type (WT) strain. However, survival of the nth1? rad16? double mutant was significantly reduced after entry into the stationary phase. Deletion of rad16 in an AP endonuclease mutant apn2? also accelerated chronological aging. These results indicate that BER and NER synergistically contribute to genome maintenance in non-dividing cells. Reactive oxygen species (ROS) accumulated in cells during the stationary phase, and nth1? rad16? cells produced more ROS than WT cells. High mutation frequencies and nuclear DNA fragmentation were observed in nth1? rad16? stationary-phase cells concurrent with apoptotic-like cell death. Calorie restriction significantly reduced the level of ROS in the stationary phase and extended the CLS of nth1? rad16? cells. Therefore, ROS production critically affects the survival of the DNA repair mutant during chronological aging.
Research papers (academic journals)
