WDR62 regulates mouse oocyte meiotic maturation related to p-JNK and H3K9 trimethylation

细胞生物学 减数分裂 主轴杆体 动细胞 减数分裂II 生物 卵母细胞 主轴检查点 染色体分离 有丝分裂 中心体 多极纺锤 主轴装置 胞质分裂 遗传学 细胞周期 细胞分裂 染色体 细胞 胚胎 基因
作者
Yong‐Sheng Wang,Chao Chen,Muhammad Jamil Ahmad,Fan Chen,Zhi‐Ming Ding,Sheng-Ji Yang,Yang‐Wu Chen,Ze‐Qun Duan,Ming Liu,Aixin Liang,Changjiu He,Guohua Hua,Li–Jun Huo
出处
期刊:The International Journal of Biochemistry & Cell Biology [Elsevier BV]
卷期号:144: 106169-106169 被引量:9
标识
DOI:10.1016/j.biocel.2022.106169
摘要

WDR62 (WD40-repeat protein 62) participates in diverse biological process, especially mitotic spindle organization via regulating centriole biogenesis and the function of centriole-associated protein. However, the role of WDR62 exerts in spindle assembly and meiotic progression control in oocytes lacking typical centrosomes remains obscure. In a previous study, we reported that WDR62 is involved in spindle migration and asymmetric cytokinesis in mouse oocyte meiosis. In the current study, another novel function of WDR62 regulating cell cycle progression through meiotic spindle formation during oocyte meiotic maturation was found. Knockdown of WDR62 through siRNA microinjection disrupted the meiotic cell cycle and induced metaphase-I (MI) arrest coupled with severe spindle abnormality, chromosome misalignment, and aneuploid generation. Moreover, WDR62 depletion induced defective kinetochore-microtubule attachments (K-MT) and activated spindle assembly checkpoint (SAC), which could trigger the arrest of meiotic progression. Further study demonstrated that depletion of WDR62 was associated with an aberrant location of p-JNK and reduced its expression level; concomitantly, status of H3K9 trimethylation was also altered. In addition, phenotypes similar to WDR62 depletion were observed during the function-loss analysis of p-JNK using a specific inhibitor (SP600125), which signifies that WDR62 is important for spindle organization and meiotic progression, and this function might be via its regulation of p-JNK. In conclusion, this study revealed that WDR62 functions in multiple ways during oocyte meiotic maturation, which could be related to p-JNK and H3K9 trimethylation.
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