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Aneuploidy and early human embryo development

机译:非整倍体与人类早期胚胎发育

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摘要

Human embryo development occurs through a process that encompasses reprogramming, sequential cleavage divisions and mitotic chromosome segregation and embryonic genome activation. Chromosomal abnormalities may arise during germ cell and/or pre-implantation embryo development, and are a major cause of spontaneous miscarriage or birth defects. Nonetheless, model systems suitable for the study of human germ cell and embryo development have been limited until recently. We suggest that human embryonic stem cells may provide a valuable human cell-based model for genetic studies of human pre-implantation pluripotent cells. Here, we review the current literature on diagnosing chromosomal abnormalities in the pre-implantation embryo, and the importance of provisions from the human oocyte in establishing and maintaining the human embryonic genome during the first 3 days post-conception. We focus on trans-criptional analysis of human oocytes and embryos and the unique cell cycle and checkpoint requirements in theearly embryo. Taken together, data suggest that the unique programs of the early human embryo, including management of aneuploid cells, may paradoxically promote embryo development but contribute to the high rate of spontaneous miscarriages in human pregnancies.
机译:人类胚胎发育通过包括重编程,顺序切割分裂,有丝分裂染色体分离和胚胎基因组激活的过程发生。染色体异常可能在生殖细胞和/或植入前胚胎发育过程中出现,并且是自然流产或先天缺陷的主要原因。但是,直到最近,适用于人类生殖细胞和胚胎发育研究的模型系统仍受到限制。我们建议人类胚胎干细胞可能为人类植入前多能细胞的遗传研究提供有价值的基于人类细胞的模型。在这里,我们回顾了有关在植入前胚胎中诊断染色体异常的现有文献,以及在受孕后的前三天中从人类卵母细胞中提供蛋白质对建立和维持人类胚胎基因组的重要性。我们专注于人类卵母细胞和胚胎的转录分析,以及早期胚胎中独特的细胞周期和检查点要求。综上所述,数据表明,早期人类胚胎的独特程序,包括对非整倍体细胞的管理,可能自相矛盾地促进了胚胎的发育,但是却助长了人类怀孕中的自然流产。

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