Publication | Closed Access
Gene expression in human neural stem cells: effects of leukemia inhibitory factor
166
Citations
66
References
2003
Year
Adult Stem CellCell ProliferationCell SpecializationImportant Growth FactorStem CellsHuman Ltnscctx CulturesHealth SciencesLif WithdrawalLeukemia Inhibitory FactorGene ExpressionCell BiologyLineage PlasticityDevelopmental BiologyStem Cell ResearchCellular SenescenceStem-cell TherapySystems BiologyMedicineNeural Stem CellEmbryonic Stem Cell
Human neural precursor cells grown in culture provide a source of tissue for drug screening, developmental studies and cell therapy. However, mechanisms underlying their growth and differentiation are poorly understood. We show that epidermal growth factor (EGF) responsive precursors derived from the developing human cortex undergo senescence after 30-40 population doublings. Leukemia inhibitory factor (LIF) increased overall expansion rates, prevented senescence and allowed the growth of a long-term self renewing neural stem cell (ltNSCctx) for up to 110 population doublings. We established basal gene expression in ltNSCctx using Affymetrix oligonucleotide microarrays that delineated specific members of important growth factor and signaling families consistently expressed across three separate lines. Following LIF withdrawal, 200 genes showed significant decreases. Protein analysis confirmed LIF-regulated expression of glial fibrillary acidic protein, CD44, and major histocompatibility complex I. This study provides the first molecular profile of human ltNSCctx cultures capable of long-term self renewal, and reveals specific sets of genes that are directly or indirectly regulated by LIF.
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