The Journal of Reproduction and Development (Apr 2024)

DNA repair is efficient in irradiated M phase zygotes

  • Yuan WANG,
  • Dai TSUKIOKA,
  • Shoji ODA,
  • Hiroshi MITANI,
  • Fugaku AOKI

DOI
https://doi.org/10.1262/jrd.2024-018
Journal volume & issue
Vol. 70, no. 3
pp. 197 – 201

Abstract

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In somatic cells, DNA repair is attenuated during mitosis to prevent the formation of anaphase bridges and facilitate the proper segregation of sister chromatids. Irradiation-induced γH2AX foci persist for hours in M phase somatic cells. However, we observed that anaphase bridges formed in a significant fraction of mouse zygotes irradiated during mitosis. Additionally, γH2AX signals in M phase zygotes peaked 30 min after irradiation and subsequently reduced with a half-life within 1–2 h. These results suggest that the DNA repair system may operate efficiently in M phase zygotes following irradiation, leading to the frequent formation of anaphase bridges. The absence of H2AX promoted the successful segregation of sister chromatids and enhanced the development of embryos to the blastocyst stage. The DNA repair system may be differentially regulated during the M phase of the first cell cycle to ensure the immediate elimination of damaged zygotes, thereby efficiently preventing transmission of mutations to subsequent generations.

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