首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Human lymphoblastoid B-cell lines reprogrammed to EBV-free induced pluripotent stem cells.
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Human lymphoblastoid B-cell lines reprogrammed to EBV-free induced pluripotent stem cells.

机译:人淋巴母细胞B细胞系重新编程为无EBV诱导的多能干细胞。

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摘要

Generation of patient-specific induced pluripotent cells (iPSCs) holds great promise for regenerative medicine. Epstein-Barr virus immortalized lymphoblastoid B-cell lines (LCLs) can be generated from a minimal amount of blood and are banked worldwide as cellular reference material for immunologic or genetic analysis of pedigreed study populations. We report the generation of iPSCs from 2 LCLs (LCL-iPSCs) via a feeder-free episomal method using a cocktail of transcription factors and small molecules. LCL-derived iPSCs exhibited normal karyotype, expressed pluripotency markers, lost oriP/EBNA-1 episomal vectors, generated teratomas, retained donor identity, and differentiated in vitro into hematopoietic, cardiac, neural, and hepatocyte-like lineages. Significantly, although the parental LCLs express viral EBNA-1 and other Epstein-Barr virus latency-related elements for their survival, their presence was not detectable in LCL-iPSCs. Thus, reprogramming LCLs could offer an unlimited source for patient-specific iPSCs.
机译:患者特异性诱导多能细胞(iPSC)的产生对于再生医学具有广阔的前景。爱泼斯坦-巴尔病毒永生化的淋巴母细胞B细胞系(LCL)可以从少量血液中产生,并在世界范围内被作为细胞参考材料用于有研究的人群的免疫学或遗传学分析。我们报告通过使用编码因子和小分子混合物的无饲养线游离方法从2个LCL(LCL-iPSC)生成iPSC。 LCL衍生的iPSC表现出正常的核型,表达多能性标记,丢失oriP / EBNA-1游离型载体,产生畸胎瘤,保留供体身份,并在体外分化为造血,心脏,神经和肝细胞样谱系。重要的是,尽管亲本LCL为生存而表达病毒EBNA-1和其他与爱泼斯坦-巴尔病毒潜伏期有关的元件,但在LCL-iPSC中无法检测到它们的存在。因此,重新编程LCL可以为患者特定的iPSC提供无限的来源。

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