Transient naive reprogramming corrects hiPS cells functionally and epigenetically

重编程 生物 表观遗传学 诱导多能干细胞 DNA甲基化 胚胎干细胞 细胞生物学 染色质 干细胞 表观基因组 细胞分化 体细胞 遗传学 细胞 基因表达 基因
作者
Sam Buckberry,Xiaodong Liu,Daniel Poppe,Jia Ping Tan,Guizhi Sun,Joseph Chen,Trung Viet Nguyen,Alex de Mendoza,Jahnvi Pflueger,Thomas Frazer,Dulce B Vargas-Landin,Jacob M. Paynter,Nathan Smits,Ning Liu,John F. Ouyang,Fernando Rossello,Hun S. Chy,Owen J. L. Rackham,Andrew L. Laslett,James Breen,Geoffrey J. Faulkner,Christian M. Nefzger,José M. Polo,Ryan Lister
出处
期刊:Nature [Springer Nature]
卷期号:620 (7975): 863-872 被引量:13
标识
DOI:10.1038/s41586-023-06424-7
摘要

Cells undergo a major epigenome reconfiguration when reprogrammed to human induced pluripotent stem cells (hiPS cells). However, the epigenomes of hiPS cells and human embryonic stem (hES) cells differ significantly, which affects hiPS cell function1-8. These differences include epigenetic memory and aberrations that emerge during reprogramming, for which the mechanisms remain unknown. Here we characterized the persistence and emergence of these epigenetic differences by performing genome-wide DNA methylation profiling throughout primed and naive reprogramming of human somatic cells to hiPS cells. We found that reprogramming-induced epigenetic aberrations emerge midway through primed reprogramming, whereas DNA demethylation begins early in naive reprogramming. Using this knowledge, we developed a transient-naive-treatment (TNT) reprogramming strategy that emulates the embryonic epigenetic reset. We show that the epigenetic memory in hiPS cells is concentrated in cell of origin-dependent repressive chromatin marked by H3K9me3, lamin-B1 and aberrant CpH methylation. TNT reprogramming reconfigures these domains to a hES cell-like state and does not disrupt genomic imprinting. Using an isogenic system, we demonstrate that TNT reprogramming can correct the transposable element overexpression and differential gene expression seen in conventional hiPS cells, and that TNT-reprogrammed hiPS and hES cells show similar differentiation efficiencies. Moreover, TNT reprogramming enhances the differentiation of hiPS cells derived from multiple cell types. Thus, TNT reprogramming corrects epigenetic memory and aberrations, producing hiPS cells that are molecularly and functionally more similar to hES cells than conventional hiPS cells. We foresee TNT reprogramming becoming a new standard for biomedical and therapeutic applications and providing a novel system for studying epigenetic memory.
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