4.7 Article

The Defects of Epigenetic Reprogramming in Dox-Dependent Porcine-iPSCs

期刊

出版社

MDPI
DOI: 10.3390/ijms231911941

关键词

porcine-iPSCs; epigenetic modification; ATAC-seq; DNA methylation; differential allelic expression gene

资金

  1. JBGS project of Seed Industry Revitalization in Jiangsu province [JBGS[2021]026]
  2. National Natural Science Foundation of China [31972571, 31630072]

向作者/读者索取更多资源

This study investigates the aberrant epigenetic reprogramming during the formation of piPSCs in pigs. It reveals that incomplete chromatin remodeling and DNA demethylation hinder pluripotent activation, resulting in low expression of endogenous pluripotency genes. The study also highlights the abnormal expression of potential imprinted genes in piPSCs, providing insight into porcine-iPSC reprogramming and genome imprinting.
Porcine-induced pluripotent stem cells (piPSCs) are of great significance to animal breeding and human medicine; however, an important problem is that the maintenance of piPSCs mainly depends on exogenous expression of pluripotent transcription factors (TFs), and germline transmission-competent piPSCs have not yet been successfully established. In this study, we explore the defect of epigenetic reprogramming during piPSCs formation, including chromatin accessibility, DNA methylation, and imprinted gene expression, with high-throughput sequencing (ATAC-seq, WGBS, RNA-seq, and Re-seq) methods. We found the somatic features were successfully silenced by connecting closed chromatin loci with downregulated genes, while DNA methylation has limited effects on somatic silence. However, the incomplete chromatin remodeling and DNA demethylation in pluripotency genes hinder pluripotent activation, resulting in the low expression of endogenous pluripotency genes. In addition, the expression of potential imprinted genes was abnormal, and many allelic-biased expressed genes in porcine embryonic fibroblasts (PEFs) were erased, accompanied by establishment of new allelic-biased expressed genes in piPSCs. This study reveals the aberrant epigenetic reprogramming during dox-dependent piPSCs formation, which lays the foundation for research of porcine-iPSC reprogramming and genome imprinting.

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