PLoS ONE (Jan 2011)

Imprinted genes that regulate early mammalian growth are coexpressed in somatic stem cells.

  • Jonathan S Berg,
  • Kuanyin K Lin,
  • Corinne Sonnet,
  • Nathan C Boles,
  • David C Weksberg,
  • Hoang Nguyen,
  • Lowenna J Holt,
  • Danny Rickwood,
  • Roger J Daly,
  • Margaret A Goodell

DOI
https://doi.org/10.1371/journal.pone.0026410
Journal volume & issue
Vol. 6, no. 10
p. e26410

Abstract

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Lifelong, many somatic tissues are replenished by specialized adult stem cells. These stem cells are generally rare, infrequently dividing, occupy a unique niche, and can rapidly respond to injury to maintain a steady tissue size. Despite these commonalities, few shared regulatory mechanisms have been identified. Here, we scrutinized data comparing genes expressed in murine long-term hematopoietic stem cells with their differentiated counterparts and observed that a disproportionate number were members of the developmentally-important, monoallelically expressed imprinted genes. Studying a subset, which are members of a purported imprinted gene network (IGN), we found their expression in HSCs rapidly altered upon hematopoietic perturbations. These imprinted genes were also predominantly expressed in stem/progenitor cells of the adult epidermis and skeletal muscle in mice, relative to their differentiated counterparts. The parallel down-regulation of these genes postnatally in response to proliferation and differentiation suggests that the IGN could play a mechanistic role in both cell growth and tissue homeostasis.