Regulation of CTCF loop formation during pancreatic cell differentiation

Transcription reprogramming during cell differentiation involves targeting enhancers to genes responsible for establishment of cell fates. To understand the contribution of CTCF-mediated chromatin organization to cell lineage commitment, we analyzed 3D chromatin architecture during the differentiati...

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Published inNature communications Vol. 14; no. 1; p. 6314
Main Authors Lyu, Xiaowen, Rowley, M Jordan, Kulik, Michael J, Dalton, Stephen, Corces, Victor G
Format Journal Article
LanguageEnglish
Published England Nature Publishing Group 09.10.2023
Nature Publishing Group UK
Nature Portfolio
Subjects
CCCTC-Binding Factor - genetics
CCCTC-Binding Factor - metabolism
Cell Cycle Proteins - genetics
Cell Cycle Proteins - metabolism
Cell differentiation
Cell Differentiation - genetics
Cell lineage
Chromatin
Cohesin
Demethylation
Deoxyribonucleic acid
Differentiation (biology)
DNA
DNA - metabolism
DNA methylation
Embryo cells
Enhancers
Gene expression
Genes
Genomes
Histones
Humans
Nucleosomes
Organoids
Pancreas
Protein Binding
Stem cells
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Summary:Transcription reprogramming during cell differentiation involves targeting enhancers to genes responsible for establishment of cell fates. To understand the contribution of CTCF-mediated chromatin organization to cell lineage commitment, we analyzed 3D chromatin architecture during the differentiation of human embryonic stem cells into pancreatic islet organoids. We find that CTCF loops are formed and disassembled at different stages of the differentiation process by either recruitment of CTCF to new anchor sites or use of pre-existing sites not previously involved in loop formation. Recruitment of CTCF to new sites in the genome involves demethylation of H3K9me3 to H3K9me2, demethylation of DNA, recruitment of pioneer factors, and positioning of nucleosomes flanking the new CTCF sites. Existing CTCF sites not involved in loop formation become functional loop anchors via the establishment of new cohesin loading sites containing NIPBL and YY1 at sites between the new anchors. In both cases, formation of new CTCF loops leads to strengthening of enhancer promoter interactions and increased transcription of genes adjacent to loop anchors. These results suggest an important role for CTCF and cohesin in controlling gene expression during cell differentiation.
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ISSN:2041-1723
2041-1723
DOI:10.1038/s41467-023-41964-6