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在卵母细胞中失活会损害卵母细胞的发育和成熟,导致小鼠卵巢储备减少。

Inactivation of in the oocyte impairs oocyte development and maturation, leading to a depletion of the ovarian reserve in mice.

机构信息

Univ Rennes, Inserm, EHESP, Irset (Institut de recherche en santé, environnement et travail) - UMR_S 1085, F-35000 Rennes, France.

Univ Rennes, CNRS, Inserm, Biosit UAR 3480 US 018, Protim core facility, F-35000 Rennes, France.

出版信息

Int J Biol Sci. 2023 Jan 31;19(4):1080-1093. doi: 10.7150/ijbs.72889. eCollection 2023.

Abstract

EXOSC10 is a catalytic subunit of the nuclear RNA exosome, and possesses a 3'-5' exoribonuclease activity. The enzyme processes and degrades different classes of RNAs. To delineate the role of EXOSC10 during oocyte growth, specific inactivation was performed in oocytes from the primordial follicle stage onward using the -iCre; mouse model ( ). female mice are infertile. The onset of puberty and the estrus cycle in mutants are initially normal and ovaries contain all follicle classes. By the age of eight weeks, vaginal smears reveal irregular estrus cycles and mutant ovaries are completely depleted of follicles. Mutant oocytes retrieved from the oviduct are degenerated, and occasionally show an enlarged polar body, which may reflect a defective first meiotic division. Under fertilization conditions, the mutant oocytes do not enter into an embryonic development process. Furthermore, we conducted a comparative proteome analysis of wild type and knockout mouse ovaries, and identified EXOSC10-dependent proteins involved in many biological processes, such as meiotic cell cycle progression and oocyte maturation. Our results unambiguously demonstrate an essential role for EXOSC10 in oogenesis and may serve as a model for primary ovarian insufficiency in humans. Data are available via ProteomeXchange with identifier PXD039417.

摘要

EXOSC10 是核 RNA 外切体的催化亚基,具有 3'-5'外切核酸酶活性。该酶处理和降解不同类别的 RNA。为了阐明 EXOSC10 在卵母细胞生长过程中的作用,使用 -iCre; 小鼠模型()在原始卵泡阶段以后的卵母细胞中特异性失活。 雌性小鼠不育。突变体的青春期和发情周期初始正常,并且卵巢包含所有卵泡类。到八周龄时,阴道涂片显示不规则的发情周期,并且突变体卵巢完全耗尽了卵泡。从输卵管中取出的突变体卵母细胞退化,偶尔会出现扩大的极体,这可能反映了第一次减数分裂的缺陷。在受精条件下,突变体卵母细胞不会进入胚胎发育过程。此外,我们对野生型和 敲除小鼠卵巢进行了比较蛋白质组分析,鉴定出 EXOSC10 依赖性蛋白参与许多生物学过程,如减数分裂细胞周期进程和卵母细胞成熟。我们的结果明确表明 EXOSC10 在卵发生中的重要作用,并可能作为人类原发性卵巢功能不全的模型。数据可通过 ProteomeXchange 以标识符 PXD039417 获得。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c2f1/10008699/ae5fa8bbb5ba/ijbsv19p1080g002.jpg

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