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Dazl is a target RNA suppressed by mammalian NANOS2 in sexually differentiating male germ cells

Author

Listed:
  • Yuzuru Kato

    (Genetic Strains Research Center, National Institute of Genetics
    SOKENDAI)

  • Takeo Katsuki

    (Kavli Institute for Brain and Mind, University of California)

  • Hiroki Kokubo

    (Genetic Strains Research Center, National Institute of Genetics
    Present address: Department of Cardiovascular Physiology and Medicine, Graduate School of Biomedical and Health Sciences, Hiroshima University, Kasumi 1-2-3, Minami-ku, Hiroshima 734-8551, Japan)

  • Aki Masuda

    (Genetic Strains Research Center, National Institute of Genetics)

  • Yumiko Saga

    (Genetic Strains Research Center, National Institute of Genetics
    SOKENDAI
    Graduate School of Science, The University of Tokyo)

Abstract

Evolutionally conserved Nanos RNA-binding proteins play crucial roles in germ cell development. While a mammalian Nanos family protein, NANOS2, is required for sexual differentiation of male (XY) germ cells in mice, the underlying mechanisms and the identities of its target RNAs in vivo remain elusive. Using comprehensive microarray analysis and a bacterial artificial chromosome transgenic system, here we identify Dazl, a germ cell-specific gene encoding an RNA-binding protein implicated in translation, as a crucial target of NANOS2. Importantly, removal of the Dazl 3′-untranslated region in XY germ cells stabilizes the Dazl mRNA, resulting in elevated meiotic gene expression, abnormal resumption of the cell cycle and impaired processing-body formation, reminiscent of Nanos2-knockout phenotypes. Furthermore, our data suggest that NANOS2 acts as an antagonist of the DAZL protein. We propose a dual system of NANOS2-mediated suppression of Dazl expression as a pivotal molecular mechanism promoting sexual differentiation of XY germ cells.

Suggested Citation

  • Yuzuru Kato & Takeo Katsuki & Hiroki Kokubo & Aki Masuda & Yumiko Saga, 2016. "Dazl is a target RNA suppressed by mammalian NANOS2 in sexually differentiating male germ cells," Nature Communications, Nature, vol. 7(1), pages 1-11, September.
  • Handle: RePEc:nat:natcom:v:7:y:2016:i:1:d:10.1038_ncomms11272
    DOI: 10.1038/ncomms11272
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