Similar frequency and signature of untargeted substitutions induced by abasic site analog under reduced human APE1 conditions

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  • Suzuki Tetsuya
    Graduate School of Biomedical and Health Sciences, Hiroshima University
  • Katayama Yuri
    Graduate School of Biomedical and Health Sciences, Hiroshima University
  • Komatsu Yasuo
    Biotechnology Research Institute for Drug Discovery, National Institute of Advanced Industrial Science and Technology (AIST)
  • Kamiya Hiroyuki
    Graduate School of Biomedical and Health Sciences, Hiroshima University

書誌事項

公開日
2021
資源種別
journal article
DOI
  • 10.2131/jts.46.283
公開者
一般社団法人 日本毒性学会

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説明

<p>Abasic sites are formed in cells by various factors including environmental mutagens and considered to be involved in cancer initiation, promotion, and progression. A chemically stable abasic site analog (tetrahydrofuran-type analog, THF) induces untargeted base substitutions as well as targeted substitution and large deletion mutations in human cells. The untargeted substitutions may be initiated by the cleavage of the DNA strand bearing THF by the human apurinic/apyrimidinic endonuclease 1 (APE1) protein, the major repair enzyme for THF and abasic sites. To examine the effects of lower APE1 levels, the protein was knocked down by siRNA in human U2OS cells. A plasmid containing a single THF modification outside the supF gene was introduced into the knockdown cells, and the untargeted substitution mutations in the reporter gene were analyzed. Unexpectedly, the knockdown had no evident impact on their frequency and spectrum. The G bases of 5′-GpA-3′ dinucleotides on the modified strand were quite frequently substituted, with and without the APE1 knockdown. These results suggested that the DNA strand cleavage by APE1 is not essential for the THF-induced untargeted base substitutions.</p>

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