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Male-driven de novo mutations in haploid germ cells

  • Marie Chantal Gregoire
  • , Julien Massonneau
  • , Olivier Simard
  • , Anne Gouraud
  • , Marc Andre Brazeau
  • , Melina Arguin
  • , Frederic Leduc
  • , Guylain Boissonneault
  • University of Sherbrooke

Résultats de recherche: Contribution à un journalArticleRevue par des pairs

Résumé

At the sequence level, genetic diversity is provided by de novo transmittable mutations that may act as a substrate for natural selection. The gametogenesis process itself is considered more likely to induce endogenous mutations and a clear male bias has been demonstrated from recent next-generation sequencing analyses. As new experimental evidence accumulates, the post-meiotic events of the male gametogenesis (spermiogenesis) appear as an ideal context to induce de novo genetic polymorphism transmittable to the next generation. It may prove to be a major component of the observed male mutation bias. As spermatids undergo chromatin remodeling, transient endogenous DNA double-stranded breaks are produced and trigger a DNA damage response. In these haploid cells, one would expect that the non-templated, DNA end-joining repair processes may generate a repertoire of sequence alterations in every sperm cell potentially transmittable to the next generation. This may therefore represent a novel physiological mechanism contributing to genetic diversity and evolution.

langue originaleAnglais
Pages (de - à)495-499
Nombre de pages5
journalMolecular Human Reproduction
Volume19
Numéro de publication8
Les DOIs
étatPublié - 1 août 2013
Modification externeOui

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