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小鼠雌性减数分裂I中姐妹染色单体过早分离的频率受遗传背景影响。

The frequency of precocious segregation of sister chromatids in mouse female meiosis I is affected by genetic background.

作者信息

Danylevska Anna, Kovacovicova Kristina, Awadova Thuraya, Anger Martin

机构信息

Veterinary Research Institute, Hudcova 70, 621 00, Brno, Czech Republic.

出版信息

Chromosome Res. 2014 Sep;22(3):365-73. doi: 10.1007/s10577-014-9428-6. Epub 2014 Jun 17.

Abstract

Mammalian female gametes frequently suffer from numerical chromosomal aberrations, the main cause of miscarriages and severe developmental defects. The underlying mechanisms responsible for the development of aneuploidy in oocytes are still not completely understood and remain a subject of extensive research. From studies focused on prevalence of aneuploidy in mouse oocytes, it has become obvious that reported rates of aneuploidy are strongly dependent on the method used for chromosome counting. In addition, it seems likely that differences between mouse strains could influence the frequency of aneuploidy as well; however, up till now, such a comparison has not been available. Therefore, in our study, we measured the levels of aneuploidy which has resulted from missegregation in meiosis I, in oocytes of three commonly used mouse strains-CD-1, C3H/HeJ, and C57BL/6. Our results revealed that, although the overall chromosomal numerical aberration rates were similar in all three strains, a different number of oocytes in each strain contained prematurely segregated sister chromatids (PSSC). This indicates that a predisposition for this type of chromosome segregation error in oocyte meiosis I is dependent on genetic background.

摘要

哺乳动物的雌性配子经常出现染色体数目异常,这是流产和严重发育缺陷的主要原因。卵母细胞中出现非整倍体的潜在机制仍未完全了解,仍是广泛研究的课题。从专注于小鼠卵母细胞中非整倍体发生率的研究中可以明显看出,报道的非整倍体率在很大程度上取决于用于染色体计数的方法。此外,小鼠品系之间的差异似乎也可能影响非整倍体的频率;然而,到目前为止,尚未有这样的比较。因此,在我们的研究中,我们测量了三种常用小鼠品系(CD-1、C3H/HeJ和C57BL/6)的卵母细胞中,由于减数分裂I中染色体错分而导致的非整倍体水平。我们的结果表明,尽管所有三个品系的总体染色体数目畸变率相似,但每个品系中含有过早分离的姐妹染色单体(PSSC)的卵母细胞数量不同。这表明卵母细胞减数分裂I中这种类型的染色体分离错误的易感性取决于遗传背景。

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