Project description:RNA-seq data of founder mice pancreatic islets

Project description:Abundant and equipotent founder cells establish and maintain acute lymphoblastic leukaemia

Project description:ATAC-seq data of founder mice pancreatic islets

Project description:Founder mice islet RNA profiling

Project description:To identify the metabolic transcriptome landscape within leukaemic cells we performed scRNA-Seq on the sorted leukaemia cells (GFP+) cells from MLL-AF9 mice.

Project description:We present a computational tool, FounderTracker, for discovering founder mutations in cancer, based on the detection of significantly conserved haplotypes in tumor SNP profiles. We demonstrate the relevance of the approach by identifying founder mutations in two different cancers, and we show with simulated data that FounderTracker can detect rare founder mutations with high power and negligible false discovery rate. FounderTracker is a powerful tool for discovering novel founder mutations that may explain part of the "missing" heritability in cancer. This SuperSeries is composed of the SubSeries listed below.

Project description:Leukaemia is caused by the clonal evolution of a cell that accumulates mutations/genomic rearrangements, allowing unrestrained cell growth. However, recent identification of leukaemic mutations in the blood cells of healthy individuals revealed that additional events are required to expand the mutated clones for overt leukaemia. Here, we assessed the functional consequences of deleting the Fanconi anaemia A (Fanca) gene, which encodes a DNA damage response protein, in Spi1 transgenic mice that develop preleukaemic syndrome. Loss of FANCA increases SPI1-associated disease penetrance and favours leukaemic progression without increasing the global mutation load of leukaemic clones. However, leukaemic FANCA-deleted cells display heterozygote activating mutations in known oncogenes, such as Kit or Nras, that are identified at low frequency in WT mice with preleukaemic syndrome, indicating that FANCA loss-of-function supports the emergence of oncogene mutated leukaemic cells. We show that a unique transcriptional deregulation is associated with the leukaemic status of cells devoid of FANCA activity, including MDM4, NOTCH and Wnt/-catenin pathways. Our observations provide evidence that FANCA-deficient preleukaemic cells carrying oncogenic Kit or Ras mutations require a favourable intracellular environment to allow the emergence of leukaemic clones. The loss of FANCA may provide this mandatory cellular setup by allowing the simultaneous activation of several proliferative pathways.

Project description:The goal of this project was to identify strain-dependent expression of miRNAs in lung tissue from Collaborative Cross founder strains that were sensitized and challenged with house dust mite allergen (Der p 1). We analyzed whole lung RNAs from the eight Collaborative Cross founder strains (n=4/strain, all males) using Affymetrix miRNA 2.0 arrays

Project description:RNA-Seq was performed on all 8 mouse founder strains of the Collaborative Cross to obtain a comprehensive splicing landscape of each strain.

Project description:Escherichia coli MG1655 founder resequencing genome sequencing