Scientific Reports (Jun 2017)

Dosage compensation in the process of inactivation/reactivation during both germ cell development and early embryogenesis in mouse

  • Xiaoyong Li,
  • Zhiqiang Hu,
  • Xuelin Yu,
  • Chen Zhang,
  • Binbin Ma,
  • Lin He,
  • Chaochun Wei,
  • Ji Wu

DOI
https://doi.org/10.1038/s41598-017-03829-z
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 13

Abstract

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Abstract Ohno proposed that dosage compensation in mammals evolved as a two-step mechanism involving X-inactivation and X-upregulation. While X-inactivation is well characterized, it remains to further analysis whether upregulation of the single activated X chromosome in mammals occurs. We obtained RNA-seq data, including single-cell RNA-seq data, from cells undergoing inactivation/reactivation in both germ cell development and early embryogenesis stages in mouse and calculated the X: A ratio from the gene expression. Our results showed that the X: A ratio is always 1, regardless of the number of X chromosomes being transcribed for expressed genes. Furthermore, the single-cell RNA-seq data across individual cells of mouse preimplantation embryos of mixed backgrounds indicated that strain-specific SNPs could be used to distinguish transcription from maternal and paternal chromosomes and further showed that when the paternal was inactivated, the average gene dosage of the active maternal X chromosome was increased to restore the balance between the X chromosome and autosomes. In conclusion, our analysis of RNA-seq data (particularly single-cell RNA-seq) from cells undergoing the process of inactivation/reactivation provides direct evidence that the average gene dosage of the single active X chromosome is upregulated to achieve a similar level to that of two active X chromosomes and autosomes present in two copies.