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DNA 损伤诱导的卵母细胞细胞死亡。

DNA Damaged Induced Cell Death in Oocytes.

机构信息

Institute of Biophysical Chemistry and Center for Biomolecular Magnetic Resonance, Goethe University, 60438 Frankfurt, Germany.

Department for Gynecological Endocrinology and Reproductive Medicine, University Hospital of Bonn, Venusberg-Campus 1, 53217 Bonn, Germany.

出版信息

Molecules. 2020 Dec 3;25(23):5714. doi: 10.3390/molecules25235714.

Abstract

The production of haploid gametes through meiosis is central to the principle of sexual reproduction. The genetic diversity is further enhanced by exchange of genetic material between homologous chromosomes by the crossover mechanism. This mechanism not only requires correct pairing of homologous chromosomes but also efficient repair of the induced DNA double-strand breaks. Oocytes have evolved a unique quality control system that eliminates cells if chromosomes do not correctly align or if DNA repair is not possible. Central to this monitoring system that is conserved from nematodes and fruit fly to humans is the p53 protein family, and in vertebrates in particular p63. In mammals, oocytes are stored for a long time in the prophase of meiosis I which, in humans, can last more than 50 years. During the entire time of this arrest phase, the DNA damage checkpoint remains active. The treatment of female cancer patients with DNA damaging irradiation or chemotherapeutics activates this checkpoint and results in elimination of the oocyte pool causing premature menopause and infertility. Here, we review the molecular mechanisms of this quality control system and discuss potential therapeutic intervention for the preservation of the oocyte pool during chemotherapy.

摘要

通过减数分裂产生单倍体配子是有性生殖的核心原则。通过交叉机制同源染色体之间遗传物质的交换进一步增强了遗传多样性。该机制不仅需要同源染色体的正确配对,还需要诱导的 DNA 双链断裂的有效修复。卵母细胞已经进化出一种独特的质量控制系统,如果染色体不能正确排列或如果无法进行 DNA 修复,该系统就会消除细胞。该监控系统的核心是从线虫和果蝇到人类都保守的 p53 蛋白家族,特别是在脊椎动物中是 p63。在哺乳动物中,卵母细胞在减数分裂 I 的前期被长时间储存,在人类中,这个过程可以持续超过 50 年。在整个阻滞阶段,DNA 损伤检查点保持活跃。女性癌症患者接受 DNA 损伤辐射或化疗药物的治疗会激活这个检查点,导致卵母细胞库被消除,从而导致过早绝经和不孕。在这里,我们综述了这个质量控制系统的分子机制,并讨论了在化疗期间保存卵母细胞库的潜在治疗干预措施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/115f/7730327/adddaf6ba498/molecules-25-05714-g001.jpg

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