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Generation of integration-free human induced pluripotent stem cells from postnatal blood mononuclear cells by plasmid vector expression

机译:通过质粒载体表达从产后血液单核细胞中产生无整合的人诱导多能干细胞

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摘要

Several human postnatal somatic cell types have been successfully reprogrammed to induced pluripotent stem cells (iPSCs). Blood mononuclear cells (MNCs) offer several advantages compared with other cell types. They are easily isolated from umbilical cord blood (CB) or adult peripheral blood (PB), and can be used fresh or after freezing. A short culture allows for more efficient reprogramming, with iPSC colonies forming from blood MNCs in 14 d, compared with 28 d for age-matched fibroblastic cells. The advantages of briefly cultured blood MNCs may be due to favorable epigenetic profiles and gene expression patterns. Blood cells from adults, especially nonlymphoid cells that are replenished frequently from intermittently activated blood stem cells, are short-lived in vivo and may contain less somatic mutations than skin fibroblasts, which are more exposed to environmental mutagens over time. We describe here a detailed, validated protocol for effective generation of integration-free human iPSCs from blood MNCs by plasmid vectors.
机译:几种人类产后体细胞类型已成功地重编程为诱导性多能干细胞(iPSC)。与其他细胞类型相比,血液单核细胞(MNC)具有许多优势。它们很容易从脐带血(CB)或成人外周血(PB)中分离出来,可以新鲜使用或冷冻后使用。短期培养可实现更有效的重编程,与年龄匹配的成纤维细胞相比,在14天内由血液MNC形成iPSC集落,而在28天内形成。短暂培养的血液MNC的优势可能是由于有利的表观遗传学特征和基因表达模式。来自成人的血细胞,特别是从间歇性激活的血液干细胞中频繁补充的非淋巴细胞,在体内寿命短,并且可能比皮肤成纤维细胞包含的体细胞突变少,而随着时间的推移,皮肤成纤维细胞更容易暴露于环境诱变剂中。我们在这里描述了一种详细,有效的方案,可通过质粒载体从血液MNC有效生成无整合的人iPSC。

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