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. 2024 Sep 24;43(9):114700.
doi: 10.1016/j.celrep.2024.114700. Epub 2024 Sep 4.

Parent-of-origin-specific DNA replication timing is confined to large imprinted regions

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Free article

Parent-of-origin-specific DNA replication timing is confined to large imprinted regions

Matthew M Edwards et al. Cell Rep. .
Free article

Abstract

Genomic imprinting involves differential DNA methylation and gene expression between homologous paternal and maternal loci. It remains unclear, however, whether DNA replication also shows parent-of-origin-specific patterns at imprinted or other genomic regions. Here, we investigate genome-wide asynchronous DNA replication utilizing uniparental human embryonic stem cells containing either maternal-only (parthenogenetic) or paternal-only (androgenetic) DNA. Four clusters of imprinted genes exhibited differential replication timing based on parent of origin, while the remainder of the genome, 99.82%, showed no significant replication asynchrony between parental origins. Active alleles in imprinted gene clusters replicated earlier than their inactive counterparts. At the Prader-Willi syndrome locus, replication asynchrony spanned virtually the entirety of S phase. Replication asynchrony was carried through differentiation to neuronal precursor cells in a manner consistent with gene expression. This study establishes asynchronous DNA replication as a hallmark of large imprinted gene clusters.

Keywords: CP: Genomics; CP: Molecular biology; DNA replication timing; Prader-Willi syndrome; epigenetics; genomic imprinting; human embryonic stem cells.

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Conflict of interest statement

Declaration of interests N.B. is the CSO of NewStem Ltd.

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