ENA

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ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/000/SRR9080430/SRR9080430.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/006/SRR9080426/SRR9080426.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/003/SRR9080413/SRR9080413.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/008/SRR9080428/SRR9080428.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/002/SRR9080432/SRR9080432.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/004/SRR9080424/SRR9080424.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/001/SRR9080421/SRR9080421.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/008/SRR9080418/SRR9080418.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/007/SRR9080417/SRR9080417.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/005/SRR9080415/SRR9080415.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/003/SRR9080423/SRR9080423.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/004/SRR9080434/SRR9080434.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/004/SRR9080414/SRR9080414.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/001/SRR9080431/SRR9080431.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/002/SRR9080412/SRR9080412.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/000/SRR9080420/SRR9080420.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/005/SRR9080425/SRR9080425.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/009/SRR9080429/SRR9080429.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/002/SRR9080422/SRR9080422.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/009/SRR9080419/SRR9080419.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/005/SRR9080435/SRR9080435.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/003/SRR9080433/SRR9080433.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/006/SRR9080416/SRR9080416.fastq.gzftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR908/007/SRR9080427/SRR9080427.fastq.gzprimaryOK200GenomicsLaurenti laboratory, Haematology, University of Cambridgehttps://www.ebi.ac.uk/ena/browser/view/PRJNA543492Homo sapiensIntegration of index sorting and single cell functional assays identified two functionally distinct subsets of phenotypic haematopoietic stem cells and multipotent progenitors (HSC/MPPs) in the peripheral blood (PB) from healthy individuals. CD71- HSC/MPPs from PB are multipotent and can repopulate the NSG xenograft model. CD71+ HSC/MPPs are a subset of phenotypic HSC/MPPs that is uniquely restricted to give rise to erythroid and megakaryocytic lineages, and expands in conditions with chronic stimulation of platelet production (e.g. frequent platelet donation, idiopathic thrombocytopenic purpura, essential thrombocythaemia). Here, we report the bulk transcriptomes of pools of 20 cells from CD71- HSC/MPPs (CD19- CD38- CD45RA- CD34lo CD71-) and CD71+ HSC/MPPs (CD19- CD38- CD45RA- CD34lo CD71+). Altogether the data shows the transcriptional similarities and differences between both subsets. It shows, that the unique erythroid/megakaryocytic lineage-priming of CD71+ HSC/MPPs is already initiated at transcriptional level, and that CD71+ HSC/MPPs differ from CD71- HSC/MPPs with regards to their protein synthesis/metabolic pathways. Overall design: Examination of the genome-wide transcriptome of bulk sorted (20 cells) CD71+ and CD71- HSC/MPPs from 4 different donors (donor1-4). Samples were sequenced as 3 technical replicates per subset and donor.ENAfalseTranscriptome of subsets of human haematopoietic stem cells from non-mobilised peripheral blood of healthy donorsTranscriptome of subsets of human haematopoietic stem cells from non-mobilised peripheral blood of healthy donors2025-09-242020-05-06PRJNA543492GSE1314099606