Meiosis I arrest abnormalities lead to severe oligozoospermia in meiosis 1 arresting protein (M1ap)-deficient mice

  • Nelson Alexander Arango
  • , Li Li
  • , Deepa Dabir
  • , Fotini Nicolau
  • , Rafael Pieretti-Vanmarcke
  • , Carla Koehler
  • , John R. McCarrey
  • , Naifang Lu
  • , Patricia K. Donahoe

Research output: Contribution to journalArticlepeer-review

28 Scopus citations

Abstract

Meiosis1 arresting protein (M1ap) is a novel vertebrate gene expressed exclusively in germ cells of the embryonic ovary and the adult testis. In male mice, M1ap expression, which is present from spermatogonia to secondary spermatocytes, is evolutionarily conserved and has a specific spatial and temporal pattern suggestive of a role during germ cell development. To test its function, mice deficient in M1ap were created. Whereas females had histologically normal ovaries, males exhibited reduced testicular size and a myriad of tubular defects, which led to severe oligozoospermia and infertility. Although some germ cells arrested at the zygotene/pachytene stages, most cells advanced to metaphase I before arresting and entering apoptosis. Cells that reached metaphase I were unable to properly align their chromosomes at the metaphase plate due to abnormal chromosome synapses and failure to form crossover foci. Depending on the state of tubular degeneration, all germ cells, with the exemption of spermatogonia, disappeared; with further deterioration, tubules displaying only Sertoli cells reminiscent of Sertoli cell-only syndrome in humans were observed. Our results uncovered an essential role for M1ap as a novel germ cell gene not previously implicated in male germ cell development and suggest that mutations in M1AP could account for some cases of nonobstructive oligozoospermia in men.

Original languageEnglish (US)
Article number76
JournalBiology of reproduction
Volume88
Issue number3
DOIs
StatePublished - Mar 2013
Externally publishedYes

Keywords

  • Infertility
  • Meiosis
  • Meiotic arrest
  • Oligozoospermia
  • Spermatogenesis
  • Testis
  • Vertebrates

ASJC Scopus subject areas

  • Reproductive Medicine

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