4.7 Article

The lineage-specific transcription factor CDX2 navigates dynamic chromatin to control distinct stages of intestine development

Journal

DEVELOPMENT
Volume 146, Issue 5, Pages -

Publisher

COMPANY BIOLOGISTS LTD
DOI: 10.1242/dev.172189

Keywords

Lineage-specifying; Transcription factor; Development; Patterning; Intestine; Chromatin

Funding

  1. National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
  2. National Institute of Allergy and Infectious Diseases (NIAID) [U01 DK103141]
  3. National Institutes of Health [R01 CA190558, R01 DK082889]
  4. Human Genetics Institute of New Jersey
  5. Biospecimen Repository Service Shared Resource and Sequencing Facility of the Rutgers Cancer Institute of New Jersey [P30CA072720]
  6. University of Michigan Center for Gastrointestinal Research (UMCGR) [NIDDK 5P30DK034933]

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Lineage-restricted transcription factors, such as the intestine-specifying factor CDX2, often have dual requirements across developmental time. Embryonic loss of CDX2 triggers homeotic transformation of intestinal fate, whereas adult-onset loss compromises crucial physiological functions but preserves intestinal identity. It is unclear how such diverse requirements are executed across the developmental continuum. Using primary and engineered human tissues, mouse genetics, and a multi-omics approach, we demonstrate that divergent CDX2 loss-of-function phenotypes in embryonic versus adult intestines correspond to divergent CDX2 chromatin-binding profiles in embryonic versus adult stages. CDX2 binds and activates distinct target genes in developing versus adult mouse and human intestinal cells. We find that temporal shifts in chromatin accessibility correspond to these context-specific CDX2 activities. Thus, CDX2 is not sufficient to activate a mature intestinal program; rather, CDX2 responds to its environment, targeting stage-specific genes to contribute to either intestinal patterning or mature intestinal function. This study provides insights into the mechanisms through which lineage-specific regulatory factors achieve divergent functions over developmental time.

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