BCAS2 regulates oocyte meiotic prophase I by participating in mRNA alternative splicing

卵母细胞 生物 卵子发生 减数分裂 卵泡发生 男科 前期 细胞生物学 胚胎 遗传学 胚胎发生 基因 医学
作者
Xiaohong Yao,Chaofan Wang,Weiran Yu,Longjie Sun,Zheng Lv,Xiaomei Xie,Shuang Tian,Yan Lü,Lei Li,Jiali Liu
出处
期刊:The FASEB Journal [Wiley]
卷期号:38 (1): e23361-e23361 被引量:6
标识
DOI:10.1096/fj.202301234rr
摘要

Oocyte meiotic prophase I (MI) is an important event in female reproduction. Breast cancer amplified sequence 2 (BCAS2) is a component of the spliceosome. Previous reports have shown that BCAS2 is critical in male germ cell meiosis, oocyte development, and early embryo genome integrity. However, the role of BCAS2 in oocyte meiosis has not been reported. We used Stra8-GFPCre mice to knock out Bcas2 in oocytes during the pachytene phase. The results of fertility tests showed that Bcas2 conditional knockout (cKO) in oocytes results in infertility in female mice. Morphological analysis showed that the number of primordial follicles in the ovaries of 2-month-old (M) mice was significantly reduced and that follicle development was blocked. Further analysis showed that the number of primordial follicles decreased and that follicle development was slowed in 7-day postpartum (dpp) ovaries. Moreover, primordial follicles undergo apoptosis, and DNA damage cannot be repaired in primary follicle oocytes. Meiosis was abnormal; some oocytes could not reach the diplotene stage, and more oocytes could not develop to the dictyotene stage. Alternative splicing (AS) analysis revealed abnormal AS of deleted in azoospermia like (Dazl) and diaphanous related formin 2 (Diaph2) oogenesis-related genes in cKO mouse ovaries, and the process of AS was involved by CDC5L and PRP19.
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