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卵母细胞动力蛋白相关蛋白 1 的耗竭导致胚胎发育中的母体效应异常。

Depletion of oocyte dynamin-related protein 1 shows maternal-effect abnormalities in embryonic development.

机构信息

Development and Stem Cell Program and Department of Anatomy and Developmental Biology, Monash Biomedicine Discovery Institute, Monash University, Melbourne, Victoria 3800, Australia.

Applied Embryology Department, High Institute for Infertility Diagnosis and Assisted Reproductive Technologies, Al-Nahrain University, Baghdad, Iraq.

出版信息

Sci Adv. 2022 Jun 17;8(24):eabl8070. doi: 10.1126/sciadv.abl8070. Epub 2022 Jun 15.

Abstract

Eggs contain about 200,000 mitochondria that generate adenosine triphosphate and metabolites essential for oocyte development. Mitochondria also integrate metabolism and transcription via metabolites that regulate epigenetic modifiers, but there is no direct evidence linking oocyte mitochondrial function to the maternal epigenome and subsequent embryo development. Here, we have disrupted oocyte mitochondrial function via deletion of the mitochondrial fission factor Drp1. Fission-deficient oocytes exhibit a high frequency of failure in peri- and postimplantation development. This is associated with altered mitochondrial function, changes in the oocyte transcriptome and proteome, altered subcortical maternal complex, and a decrease in oocyte DNA methylation and H3K27me3. Transplanting pronuclei of fertilized Drp1 knockout oocytes to normal ooplasm fails to rescue embryonic lethality. We conclude that mitochondrial function plays a role in establishing the maternal epigenome, with serious consequences for embryo development.

摘要

卵子含有约 20 万个线粒体,这些线粒体产生三磷酸腺苷和代谢物,对卵母细胞的发育至关重要。线粒体还通过调节表观遗传修饰物的代谢物来整合代谢和转录,但没有直接证据将卵母细胞线粒体功能与母体表观基因组和随后的胚胎发育联系起来。在这里,我们通过删除线粒体分裂因子 Drp1 来破坏卵母细胞的线粒体功能。分裂缺陷的卵母细胞在植入前和植入后发育过程中失败的频率很高。这与线粒体功能改变、卵母细胞转录组和蛋白质组改变、亚皮质母体复合物改变以及卵母细胞 DNA 甲基化和 H3K27me3 减少有关。将受精的 Drp1 敲除卵母细胞的原核移植到正常卵质中不能挽救胚胎致死性。我们得出结论,线粒体功能在建立母体表观基因组中发挥作用,对胚胎发育有严重影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c6c1/9200162/64541df7abfd/sciadv.abl8070-f1.jpg

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