Non-Canonical and Sexually Dimorphic X Dosage Compensation States in the Mouse and Human Germline

نویسندگان

  • Mahesh N. Sangrithi
  • Helene Royo
  • Shantha K. Mahadevaiah
  • Obah Ojarikre
  • Leena Bhaw
  • Abdul Sesay
  • Antoine H.F.M. Peters
  • Michael Stadler
  • James M.A. Turner
چکیده

Somatic X dosage compensation requires two mechanisms: X inactivation balances X gene output between males (XY) and females (XX), while X upregulation, hypothesized by Ohno and documented in vivo, balances X gene with autosomal gene output. Whether X dosage compensation occurs in germ cells is unclear. We show that mouse and human germ cells exhibit non-canonical X dosage states that differ from the soma and between the sexes. Prior to genome-wide reprogramming, X upregulation is present, consistent with Ohno's hypothesis. Subsequently, however, it is erased. In females, erasure follows loss of X inactivation, causing X dosage excess. Conversely, in males, erasure leads to permanent X dosage decompensation. Sex chromosomally abnormal models exhibit a "sex-reversed" X dosage state: XX males, like XX females, develop X dosage excess, while XO females, like XY males, develop X dosage decompensation. Thus, germline X dosage compensation states are determined by X chromosome number, not phenotypic sex. These unexpected differences in X dosage compensation states between germline and soma offer unique perspectives on sex chromosome infertility.

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عنوان ژورنال:

دوره 40  شماره 

صفحات  -

تاریخ انتشار 2017