4.6 Article

Regulatory domains controlling high intestinal vitamin D receptor gene expression are conserved in mouse and human

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 298, Issue 3, Pages -

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ELSEVIER
DOI: 10.1016/j.jbc.2022.101616

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Funding

  1. National Institutes of Diabetes and Digestive and Kidney Diseases [R01 DK112365]

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This study identified the regulatory sites controlling intestine-specific Vdr gene expression using ATAC-Seq technology. The results showed that these sites vary during intestinal development and are associated with intestinal transcription factors. Comparison with DNAse-Seq data from other tissues revealed that these regulatory sites are highly conserved in humans as well.
Vitamin D receptor (VDR) levels are highest in the intestine where it mediates 1,25 dihydroxyvitamin D-induced gene expression. However, the mechanisms controlling high intestinal VDR gene expression are unknown. Here, we used Assay for Transposase-Accessible Chromatin using Sequencing (ATAC-Seq) to identify the regulatory sites controlling intestine-specific Vdr gene expression in the small intestine (villi and crypts) and colon of developing, adult, and aged mice. We identified 17 ATAC peaks in a 125 kb region from intron 3 to -55.8 kb from exon 1 of the Vdr gene. Interestingly, many of these peaks were missing/reduced in the developing intestine. peaks for intestinal transcription factors (TFs) were present within the ATAC peaks and at HiChIP looping attachments that connected the ATAC/TF ChIP peaks to the transcription start site and CCCTF-binding factor sites at the borders of the Vdr gene regulatory domain. Intestine-specific regulatory sites were identified by comparing ATAC peaks to DNAse-Seq data from other tissues that revealed tissue-specific, evolutionary conserved, and species-specific peaks. Bioinformatics analysis of human DNAse-Seq peaks revealed polymorphisms that disrupt TF-binding sites. Our analysis shows that mouse intestinal Vdr gene regulation requires a complex interaction of multiple distal regulatory regions and is controlled by a combination of intestinal TFs. These intestinal regulatory sites are well conserved in humans suggesting that they may be key components of VDR regulation in both mouse and human intestines.

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