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The frequency of heterologous synapsis increases with aging in Robertsonian heterozygous male mice

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2012-02
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Vasco, Chiara
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The frequency of heterologous synapsis increases with aging in Robertsonian heterozygous male mice
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Author
  • Vasco, Chiara;
  • Manterola, Marcia;
  • Page, Jesús;
  • Zuccotti, Maurizio;
  • Fuente, Roberto de la;
  • Redi, Carlo Alberto;
  • Fernández Donoso, Raúl;
  • Garagna, Silvia;
Abstract
The house mouse is characterised by highly variable chromosome number due to the presence of Robertsonian (Rb) chromosomes. During meiosis in Rb heterozygotes, intricated chromosomal figures are produced, and many unsynapsed regions are present during the first prophase, triggering a meiotic silencing of unsynapsed chromatin (MSUC) in a similar mode to the sex chromosome inactivation. The presence of unsynapsed chromosome regions is associated with impaired spermatogenesis. Interestingly, in male mice carrying multiple Rb trivalents, the frequency of germ cell death, defective tubules, and altered sperm morphology decreases during aging. Here, we studied whether synapsis of trivalent chromosomes and MSUC are involved in this improvement. By immunocytochemistry, we analysed the frequency of unsynapsed chromosomes and of those positive to gamma H2AX (a marker of MSUC) labelling in spermatocytes of 3-, 5- and 7-month-old Rb heterozygotes. With aging, we observed a decrease of the frequency of unsynapsed chromosomes, of spermatocytes bearing them and of trivalents carrying gamma H2AX-negative unsynapsed regions. Our quantitative results show that both synapsis and MSUC processes are better accomplished during male aging, partially accounting for the improvement of spermatogenesis.
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Regione Lombardia (Fondo per la promozione di accordi istituzionali) Alma Mater Ticinensis (Promuovere la ricerca d'eccellenza, University of Pavia), Italy Ministerio de Ciencia e Innovacion (Spain) BFU2099/10987 CONICYT (Chile) Fondecyt (Chile) 1080090
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URI: https://repositorio.uchile.cl/handle/2250/129000
DOI: DOI 10.1007/s10577-011-9272-x
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Chromosome Res (2012) 20:269–278
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