Project description:The goal of this study is to study the chromatin accessibility signature of embronic hindgut epithelia

Project description:ATAC-seq of Intestine Epithelia (Ileum and Colon) from Satb2-deficient and WT mice

Project description:Transcriptional profiling of Bmi1 mutant dental epithelia including the stem cell compartment to determine which genes are upregulated in response to loss of Bmi1. Two condition experiment: dental epithelia homozygous null for Bmi1 and WT dental epithelia. 4 replicates each

Project description:Farmed salmon individuals from AquaGen AS was sampled and hindgut tissue was taken for RNAseq

Project description:scRNA-Seq of Intestine Epithelia (Ileum and Colon) from Satb2-deficient and WT mice

Project description:Bulk RNA-seq of Early Time Course Colonic Epithelia from Satb2-deficient and WT mice

Project description:To study the epigenetic regulation of intestinal epithelium we focus on the role of chromatin modulators. Lysine-specific histone demethylase 1a (KDM1A, LSD1) is one of the enzymes that can erase the H3K4me1/2 mark. To assess the role of LSD1 in intestinal epithelium we studied wild type (WT) (Villin-Cre -; Lsd1f/f) and intestinal-epithelial-specific knock-out (KO) (Villin-Cre+; Lsd1f/f) mice. We found that KO mice completely lack Paneth cells, and have altered stem cell characteristics compared to WT littermates. To assess genome-wide ATAC levels in WT and KO small intestines, we isolated intestinal epithelium tissue from wild type mice and LSD1 KO mice. This tissue was digested to single cells and performed ATAC seq as described in the protocols.

Project description:Tregs deltaDC mice vs. wt mice

Project description:Transcriptional profiling of Bmi1 mutant dental epithelia including the stem cell compartment to determine which genes are upregulated in response to loss of Bmi1.

Project description:Bulk RNA-seq of Intestine Epithelia (Jejunum, Ileum, Cecum and Colon) from Satb2-deficient and WT mice