31 / 2026-03-17 15:25:28
Nucleolar migration regulates meiotic sex chromosome inactivation during spermatogenesis
Nucleolus; Meiosis; Sex Chromosome Inactivation
摘要待审
振海 杜 / 中科院分子细胞科学卓越创新中心
During spermatogenesis, the unsynapsed XY chromosomes undergo meiotic sex chromosome inactivation (MSCI) and form a heterochromatic XY body. Defects in MSCI lead to meiotic arrest and male infertility. Although DNA damage response (DDR) factors are established as key initiators of MSCI, how transcriptional silencing is subsequently achieved remains elusive. Here, we identify the nucleolar components NPM1, SENP3, and rRNA as essential downstream effectors of DDR signaling in MSCI. During pachytene, these components migrate to and transiently cover the XY body during MSCI establishment, before becoming restricted to a corner of the XY body. Genetic deletion of Npm1 or Senp3, or inhibition of rRNA transcription severely impairs MSCI. Mechanistically, SENP3-mediated deSUMOylation of NPM1 promotes its interaction with rRNA, enabling liquid-liquid phase separation, via which they exclude Pol II from the XY body. Together, these data reveal a critical role of nucleolar components in the transcriptional regulation of MSCI in mammalian spermatogenesis
重要日期
  • 会议日期

    04月16日

    2026

    04月19日

    2026

  • 04月06日 2026

    初稿截稿日期

主办单位
西北农林科技大学
西安交通大学
浙江大学
华中农业大学
中国遗传学会三维基因组学专委会
承办单位
西北农林科技大学
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