Aneuploidy in mammalian oocytes and the impact of maternal ageing

被引:76
|
作者
Charalambous, Chloe [1 ]
Webster, Alexandre [1 ]
Schuh, Melina [1 ]
机构
[1] Max Planck Inst Multidisciplinary Sci, Dept Meiosis, Gottingen, Germany
关键词
SPINDLE ASSEMBLY CHECKPOINT; STEROID-HORMONE PRODUCTION; BISPHENOL-A; CHROMOSOME SEGREGATION; MOUSE OOCYTES; ERROR-PRONE; IN-VITRO; MEIOSIS-I; OXIDATIVE STRESS; DNA-DAMAGE;
D O I
10.1038/s41580-022-00517-3
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Fidelity of meiosis in human oocytes can be compromised, leading to egg aneuploidy and impaired embryo development, which increase with advanced maternal age. Recent studies have shed light on the molecular mechanisms underlying aberrant chromosome segregation during oocyte meiosis and the impact of ageing on this process. During fertilization, the egg and the sperm are supposed to contribute precisely one copy of each chromosome to the embryo. However, human eggs frequently contain an incorrect number of chromosomes - a condition termed aneuploidy, which is much more prevalent in eggs than in either sperm or in most somatic cells. In turn, aneuploidy in eggs is a leading cause of infertility, miscarriage and congenital syndromes. Aneuploidy arises as a consequence of aberrant meiosis during egg development from its progenitor cell, the oocyte. In human oocytes, chromosomes often segregate incorrectly. Chromosome segregation errors increase in women from their mid-thirties, leading to even higher levels of aneuploidy in eggs from women of advanced maternal age, ultimately causing age-related infertility. Here, we cover the two main areas that contribute to aneuploidy: (1) factors that influence the fidelity of chromosome segregation in eggs of women from all ages and (2) factors that change in response to reproductive ageing. Recent discoveries reveal new error-causing pathways and present a framework for therapeutic strategies to extend the span of female fertility.
引用
收藏
页码:27 / 44
页数:18
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