Single-embryo transcriptomic atlas of oxygen response reveals the critical role of HIF-1α in prompting embryonic zygotic genome activation

母子转换 H3K4me3 胚泡 胚胎 转录组 胚胎干细胞 表观遗传学 细胞生物学 合子 生物 胚胎发生 组蛋白 遗传学 基因 基因表达 发起人
作者
Fusheng Yao,Meiqiang Chu,Guangyin Xi,Jiage Dai,Zhaochen Wang,Hao Jia,Qianying Yang,Wenjing Wang,Yawen Tang,Jingyu Zhang,Yuan Yue,Yue Wang,Yefen Xu,Wei Zhao,Lizhu Ma,Juan Liu,Zhenni Zhang,Jianhui Tian,Lei An
出处
期刊:Redox biology [Elsevier]
卷期号:72: 103147-103147 被引量:4
标识
DOI:10.1016/j.redox.2024.103147
摘要

Adaptive response to physiological oxygen levels (physO2; 5% O2) enables embryonic survival in a low-oxygen developmental environment. However, the mechanism underlying the role of physO2 in supporting preimplantation development, remains elusive. Here, we systematically studied oxygen responses of hallmark events in preimplantation development. Focusing on impeded transcriptional upregulation under atmospheric oxygen levels (atmosO2; 20% O2) during the 2-cell stage, we functionally identified a novel role of HIF-1α in promoting major zygotic genome activation by serving as an oxygen-sensitive transcription factor. Moreover, during blastocyst formation, atmosO2 impeded H3K4me3 and H3K27me3 deposition by deregulating histone-lysine methyltransferases, thus impairing X-chromosome inactivation in blastocysts. In addition, we found atmosO2 impedes metabolic shift to glycolysis before blastocyst formation, thus resulting a low-level histone lactylation deposition. Notably, we also reported an increased sex-dimorphic oxygen response of embryos upon preimplantation development. Together, focusing on genetic and epigenetic events that are essential for embryonic survival and development, the present study advances current knowledge of embryonic adaptive responses to physO2, and provides novel insight into mechanism underlying irreversibly impaired developmental potential due to a short-term atmosO2 exposure.
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