Meiotic Kinetochores Fragment into Multiple Lobes upon Cohesin Loss in Aging Eggs

动细胞 生物 着丝粒 粘蛋白 细胞生物学 染色体分离 减数分裂 主轴杆体 中期 主轴装置 遗传学 染色体 细胞分裂 基因 细胞
作者
Agata P. Zielinska,Eirini Bellou,Ninadini Sharma,Ann-Sophie Frombach,K. Bianka Seres,Jennifer R. Gruhn,Martyn Blayney,H. Eckel,Rüdiger Moltrecht,Kay Elder,Eva R. Hoffmann,Melina Schuh
出处
期刊:Current Biology [Elsevier]
卷期号:29 (22): 3749-3765.e7 被引量:74
标识
DOI:10.1016/j.cub.2019.09.006
摘要

Chromosome segregation errors during female meiosis are a leading cause of pregnancy loss and human infertility. The segregation of chromosomes is driven by interactions between spindle microtubules and kinetochores. Kinetochores in mammalian oocytes are subjected to special challenges: they need to withstand microtubule pulling forces over multiple hours and are built on centromeric chromatin that in humans is decades old. In meiosis I, sister kinetochores are paired and oriented toward the same spindle pole. It is well established that they progressively separate from each other with advancing female age. However, whether aging also affects the internal architecture of centromeres and kinetochores is currently unclear. Here, we used super-resolution microscopy to study meiotic centromere and kinetochore organization in metaphase-II-arrested eggs from three mammalian species, including humans. We found that centromeric chromatin decompacts with advancing maternal age. Kinetochores built on decompacted centromeres frequently lost their integrity and fragmented into multiple lobes. Fragmentation extended across inner and outer kinetochore regions and affected over 30% of metaphase-II-arrested (MII) kinetochores in aged women and mice, making the lobular architecture a prominent feature of the female meiotic kinetochore. We demonstrate that a partial cohesin loss, as is known to occur in oocytes with advancing maternal age, is sufficient to trigger centromere decompaction and kinetochore fragmentation. Microtubule pulling forces further enhanced the fragmentation and shaped the arrangement of kinetochore lobes. Fragmented kinetochores were frequently abnormally attached to spindle microtubules, suggesting that kinetochore fragmentation could contribute to the maternal age effect in mammalian eggs.

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