首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Human-induced pluripotent stem cells from blood cells of healthy donors and patients with acquired blood disorders
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Human-induced pluripotent stem cells from blood cells of healthy donors and patients with acquired blood disorders

机译:人类诱导的多能干细胞,来自健康供体和获得性血液疾病患者的血细胞

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Human induced pluripotent stem (iPS) cells derived from somatic cells hold promise to develop novel patient-specific cell therapies and research models for inherited and acquired diseases. We and others previously reprogrammed human adherent cells, such as postnatal fibroblasts to iPS cells, which resemble adherent embryonic stem cells. Here we report derivation of iPS cells from postnatal human blood cells and the potential of these pluripotent cells for disease modeling. MultiplehumaniPS cell lines were generated from previously frozen cord blood or adult CD34+ cells of healthy donors, and could be redirected to hematopoietic differentiation. Multiple iPS cell lines were also generated from peripheral blood CD34+ cells of 2 patients with myeloproliferative disorders (MPDs) who acquired the JAK2-V617F somatic mutation in their blood cells. The MPD-derived iPS cells containing the mutation appeared normal in phenotypes, karyotype, and pluripotency. After directed hematopoietic differentiation, the MPD-iPS cell-derived hematopoietic progenitor (CD34+CD45+) cells showed the increased erythropoiesis and gene expression of specific genes, recapitulating features of the primary CD34+ cells of the corresponding patient from whom the iPS cells were derived. These iPS cells provide a renewable cell source and a prospective hematopoiesis model for investigating MPD pathogenesis.
机译:源自体细胞的人诱导多能干(iPS)细胞有望为新型的患者特异性细胞疗法和遗传性和后天性疾病研究模型的开发。我们和其他人先前将人类贴壁细胞(如产后成纤维细胞)重编程为iPS细胞,类似于贴壁胚胎干细胞。在这里,我们报道了从产后人类血细胞衍生的iPS细胞以及这些多能细胞在疾病建模中的潜力。多人类iPS细胞系是从先前冷冻的脐带血或健康供体的成年CD34 +细胞中产生的,可以重定向至造血分化。还从2名患有骨髓增生性疾病(MPD)的患者的外周血CD34 +细胞中产生了多个iPS细胞系,这些患者的血细胞中获得了JAK2-V617F体细胞突变。含有突变的MPD衍生的iPS细胞在表型,核型和多能性方面表现正常。在定向造血分化后,源自MPD-iPS细胞的造血祖细胞(CD34 + CD45 +)细胞显示出增加的红细胞生成和特定基因的基因表达,从而再现了iPS细胞来源的相应患者的原代CD34 +细胞的特征。这些iPS细胞为研究MPD发病机理提供了可再生的细胞来源和预期的造血模型。

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