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不同类型的滞后染色体是导致小鼠年龄相关卵母细胞非整倍体的基础。

Distinct classes of lagging chromosome underpin age-related oocyte aneuploidy in mouse.

机构信息

Centre de Recherche CHUM, 900 Rue St Denis, Montreal, QC H2X0A9, Canada.

Centre de Recherche CHUM, 900 Rue St Denis, Montreal, QC H2X0A9, Canada; Department of Obstetrics and Gynaecology, University of Montreal, 2900 Boul Edouard Montpetit, Montreal, QC H3T 1J4, Canada.

出版信息

Dev Cell. 2021 Aug 23;56(16):2273-2283.e3. doi: 10.1016/j.devcel.2021.07.022.

Abstract

Chromosome segregation errors that cause oocyte aneuploidy increase in frequency with maternal age and are considered a major contributing factor of age-related fertility decline in females. Lagging anaphase chromosomes are a common age-associated phenomenon in oocytes, but whether anaphase laggards actually missegregate and cause aneuploidy is unclear. Here, we show that lagging chromosomes in mouse oocytes comprise two mechanistically distinct classes of chromosome motion that we refer to as "class-I" and "class-II" laggards. We use imaging approaches and mechanistic interventions to dissociate the two classes and find that whereas class-II laggards are largely benign, class-I laggards frequently directly lead to aneuploidy. Most notably, a controlled prolongation of meiosis I specifically lessens class-I lagging to prevent aneuploidy. Our data thus reveal lagging chromosomes to be a cause of age-related aneuploidy in mouse oocytes and suggest that manipulating the cell cycle could increase the yield of useful oocytes in some contexts.

摘要

染色体分离错误导致卵母细胞非整倍体的频率随母体年龄的增加而增加,被认为是女性与年龄相关的生育能力下降的一个主要因素。后期滞后染色体是卵母细胞中常见的与年龄相关的现象,但后期滞后的染色体是否实际上发生了错误分离并导致非整倍体还不清楚。在这里,我们表明,小鼠卵母细胞中的滞后染色体包括两种机制上不同的染色体运动类别,我们称之为“I 类”和“II 类”滞后染色体。我们使用成像方法和机制干预来分离这两种类别,并发现虽然 II 类滞后染色体在很大程度上是良性的,但 I 类滞后染色体经常直接导致非整倍体。最值得注意的是,对减数分裂 I 的时间进行精确的延长可以显著减少 I 类滞后,从而防止非整倍体的发生。因此,我们的数据表明,滞后染色体是导致小鼠卵母细胞与年龄相关的非整倍体的原因,并表明在某些情况下,操纵细胞周期可以增加有用卵母细胞的产量。

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