Pak2的减少导致小鼠早期胚胎发育失败。

Reproductive biology and endocrinology : RB&E Pub Date : 2021-12-09 DOI:10.1186/s12958-021-00865-3

Juan Zeng, Nengqing Liu, Yinghong Yang, Yi Cheng, Yuanshuai Li, Xiaoxia Guo, Qian Luo, Lifen Zhu, Hongmei Guan, Bing Song, Xiaofang Sun

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引用次数: 3

摘要

背景:早期胚胎的质量对胚胎发育和着床至关重要。作为一种高度保守的丝氨酸/苏氨酸激酶，p21活化激酶2 (Pak2)参与多种生物过程，尤其是细胞骨架重塑和细胞凋亡。在小鼠中，Pak2基因敲除和内皮细胞的缺失显示出胚胎致死性。然而，Pak2在着床前胚胎中的作用尚不清楚。方法:在本研究中，利用一种特定的小干扰RNA在小鼠早期胚胎中减少Pak2，验证了Pak2在小鼠早期胚胎发育过程中纺锤体组装和DNA修复中的独特作用。我们还采用免疫印迹、免疫染色、体外受精(IVF)和图像定量分析来检测Pak2基因敲低对胚胎发育进程、纺锤体组装、染色体排列、氧化应激、DNA损伤和囊胚细胞凋亡的影响。通过免疫荧光显微镜检测染色质中含有γ - h2ax的区域，并将其作为DNA损伤的生物标志物。结果:我们发现Pak2敲低可显著减少早期胚胎的囊胚形成。此外，Pak2的减少导致胚胎中纺锤体组装异常和染色体畸变的急剧增加。我们注意到在Pak2敲低的胚胎中活性氧(ROS)的过量产生。在DNA双链断裂(dsb)的响应中，组蛋白H2AX在丝氨酸139处特异性磷酸化，产生γH2AX，用于定量dsb。在本研究中，Pak2敲低也导致磷酸化的γ - h2ax积累，表明胚胎DNA损伤增加。与此相对应的是，与对照相比，Pak2-KD胚胎中囊胚细胞凋亡率显著增加。结论:总的来说，我们的数据表明Pak2可能是纺锤体组装和DNA修复的重要调节因子，从而参与了早期小鼠胚胎的发育。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Pak2 reduction induces a failure of early embryonic development in mice.

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Pak2 reduction induces a failure of early embryonic development in mice.

Background: The quality of the early embryo is vital to embryonic development and implantation. As a highly conserved serine/threonine kinase, p21-activated kinase 2 (Pak2) participates in diverse biologic processes, especially in cytoskeleton remodeling and cell apoptosis. In mice, Pak2 knock out and endothelial depletion of Pak2 showed embryonic lethality. However, the role of Pak2 in preimplantation embryos remains unelucidated.

Methods: In the present work, Pak2 was reduced using a specific small interfering RNA in early mouse embryos, validating the unique roles of Pak2 in spindle assembly and DNA repair during mice early embryonic development. We also employed immunoblotting, immunostaining, in vitro fertilization (IVF) and image quantification analyses to test the Pak2 knockdown on the embryonic development progression, spindle assembly, chromosome alignment, oxidative stress, DNA lesions and blastocyst cell apoptosis. Areas in chromatin with γH2AX were detected by immunofluorescence microscopy and serve as a biomarker of DNA damages.

Results: We found that Pak2 knockdown significantly reduced blastocyst formation of early embryos. In addition, Pak2 reduction led to dramatically increased abnormal spindle assembly and chromosomal aberrations in the embryos. We noted the overproduction of reactive oxygen species (ROS) with Pak2 knockdown in embryos. In response to DNA double strand breaks (DSBs), the histone protein H2AX is specifically phosphorylated at serine139 to generate γH2AX, which is used to quantitative DSBs. In this research, Pak2 knockdown also resulted in the accumulation of phosphorylated γH2AX, indicative of increased embryonic DNA damage. Commensurate with this, a significantly augmented rate of blastocyst cell apoptosis was detected in Pak2-KD embryos compared to their controls.

Conclusions: Collectively, our data suggest that Pak2 may serve as an important regulator of spindle assembly and DNA repair, and thus participate in the development of early mouse embryos.

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Reproductive biology and endocrinology : RB&E

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