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Loss of Centromere Cohesion in Aneuploid Human Oocytes Correlates with Decreased Kinetochore Localization of the Sac Proteins Bub1 and Bubr1
被引:0
|作者:
Julie Lagirand-Cantaloube
Cendrine Ciabrini
Sophie Charrasse
Alice Ferrieres
Anna Castro
Tal Anahory
Thierry Lorca
机构:
[1] Université de Montpellier,Département de Gynécologie Obstétrique
[2] Centre de Recherche de Biologie Cellulaire de Montpellier,undefined
[3] Unité de Cytogénétique DPI,undefined
[4] CHU Arnaud de Villeneuve,undefined
[5] Unité d’AMP DPI,undefined
[6] CHU Arnaud de Villeneuve,undefined
[7] Equipe Médecine de la Reproduction,undefined
[8] CHU Arnaud de Villeneuve,undefined
来源:
Scientific Reports
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7卷
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摘要:
In human eggs, aneuploidy increases with age and can result in infertility and genetic diseases. Studies in mouse oocytes suggest that reduced centromere cohesion and spindle assembly checkpoint (SAC) activity could be at the origin of chromosome missegregation. Little is known about these two features in humans. Here, we show that in human eggs, inter-kinetochore distances of bivalent chromosomes strongly increase with age. This results in the formation of univalent chromosomes during metaphase I (MI) and of single chromatids in metaphase II (MII). We also investigated SAC activity by checking the localization of BUB1 and BUBR1. We found that they localize at the kinetochore with a similar temporal timing than in mitotic cells and in a MPS1-dependent manner, suggesting that the SAC signalling pathway is active in human oocytes. Moreover, our data also suggest that this checkpoint is inactivated when centromere cohesion is lost in MI and consequently cannot inhibit premature sister chromatid separation. Finally, we show that the kinetochore localization of BUB1 and BUBR1 decreases with the age of the oocyte donors. This could contribute to oocyte aneuploidy.
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