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Bub1突变的杂合性会导致小鼠雌性特异性生殖细胞非整倍体。

Heterozygosity for a Bub1 mutation causes female-specific germ cell aneuploidy in mice.

作者信息

Leland Shawn, Nagarajan Prabakaran, Polyzos Aris, Thomas Sharon, Samaan George, Donnell Robert, Marchetti Francesco, Venkatachalam Sundaresan

机构信息

Department of Biochemistry and Cellular and Molecular Biology, University of Tennessee, Knoxville, TN 37996, USA.

出版信息

Proc Natl Acad Sci U S A. 2009 Aug 4;106(31):12776-81. doi: 10.1073/pnas.0903075106. Epub 2009 Jul 17.

Abstract

Aneuploidy, the most common chromosomal abnormality at birth and the main ascertained cause of pregnancy loss in humans, originates primarily from chromosome segregation errors during oogenesis. Here, we report that heterozygosity for a mutation in the mitotic checkpoint kinase gene, Bub1, induces aneuploidy in female germ cells of mice and that the effect increases with advancing maternal age. Analysis of Bub1 heterozygous oocytes showed that aneuploidy occurred primarily during the first meiotic division and involved premature sister chromatid separation. Furthermore, aneuploidy was inherited in zygotes and resulted in the loss of embryos after implantation. The incidence of aneuploidy in zygotes was sufficient to explain the reduced litter size in matings with Bub1 heterozygous females. No effects were seen in germ cells from heterozygous males. These findings show that Bub1 dysfunction is linked to inherited aneuploidy in female germ cells and may contribute to the maternal age-related increase in aneuploidy and pregnancy loss.

摘要

非整倍体是出生时最常见的染色体异常,也是人类已知的妊娠丢失的主要原因,主要源于卵子发生过程中的染色体分离错误。在此,我们报告有丝分裂检查点激酶基因Bub1的突变杂合性在小鼠雌性生殖细胞中诱导非整倍体,并且这种效应随着母龄增长而增强。对Bub1杂合卵母细胞的分析表明,非整倍体主要发生在第一次减数分裂期间,并且涉及姐妹染色单体过早分离。此外,非整倍体在合子中遗传,并导致植入后胚胎丢失。合子中非整倍体的发生率足以解释与Bub1杂合雌性交配时产仔数减少的现象。在杂合雄性的生殖细胞中未观察到任何影响。这些发现表明,Bub1功能障碍与雌性生殖细胞中的遗传性非整倍体有关,并且可能导致与母龄相关的非整倍体增加和妊娠丢失。

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