PLoS Biology (Nov 2019)

Hypothalamic miR-30 regulates puberty onset via repression of the puberty-suppressing factor, Mkrn3.

  • Violeta Heras,
  • Susana Sangiao-Alvarellos,
  • Maria Manfredi-Lozano,
  • María J Sanchez-Tapia,
  • Francisco Ruiz-Pino,
  • Juan Roa,
  • Maribel Lara-Chica,
  • Rosario Morrugares-Carmona,
  • Nathalie Jouy,
  • Ana P Abreu,
  • Vincent Prevot,
  • Denise Belsham,
  • Maria J Vazquez,
  • Marco A Calzado,
  • Leonor Pinilla,
  • Francisco Gaytan,
  • Ana C Latronico,
  • Ursula B Kaiser,
  • Juan M Castellano,
  • Manuel Tena-Sempere

DOI
https://doi.org/10.1371/journal.pbio.3000532
Journal volume & issue
Vol. 17, no. 11
p. e3000532

Abstract

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Mkrn3, the maternally imprinted gene encoding the makorin RING-finger protein-3, has recently emerged as putative pubertal repressor, as evidenced by central precocity caused by MKRN3 mutations in humans; yet, the molecular underpinnings of this key regulatory action remain largely unexplored. We report herein that the microRNA, miR-30, with three binding sites in a highly conserved region of its 3' UTR, operates as repressor of Mkrn3 to control pubertal onset. Hypothalamic miR-30b expression increased, while Mkrn3 mRNA and protein content decreased, during rat postnatal maturation. Neonatal estrogen exposure, causing pubertal alterations, enhanced hypothalamic Mkrn3 and suppressed miR-30b expression in female rats. Functional in vitro analyses demonstrated a strong repressive action of miR-30b on Mkrn3 3' UTR. Moreover, central infusion during the juvenile period of target site blockers, tailored to prevent miR-30 binding to Mkrn3 3' UTR, reversed the prepubertal down-regulation of hypothalamic Mkrn3 protein and delayed female puberty. Collectively, our data unveil a novel hypothalamic miRNA pathway, involving miR-30, with a prominent role in the control of puberty via Mkrn3 repression. These findings expand our current understanding of the molecular basis of puberty and its disease states.