Leukemia reconstitution in vivo is driven by cells in early cell cycle and low metabolic state. Homo sapiens
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https://www.ncbi.nlm.nih.gov/bioproject/PRJNA292298
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To characterize LICs in ALL irrespective of surface markers expression, we investigated leukemia initiating activities of cellular subfractions of patient-derived xenograft BCP-ALL cells sorted according to different cell cycle phases (i.e. G0/G1 and G2/M) followed by transplantation onto NOD/SCID mice. All cell fractions led to leukemia engraftment indicating LIC activity irrespective of cell cycle stage. Most importantly, cells isolated from G0/G1 cell cycle phases led to early leukemia engraftment in contrast to cells from late cell cycle (G2/M). To further characterize cells with different engraftment potential in vivo, we analyzed the gene expression profiles of early (G1b early) and late (G2/M) engrafting cells. Overall design: Gene expression was measured using Affymetrix platform in 8 BCP-ALL patient derived xenograft samples sorted according to cell cycle annotations
创建时间:
2015-08-07



