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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Clonal genetic and hematopoietic heterogeneity among human-induced pluripotent stem cell lines.
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Clonal genetic and hematopoietic heterogeneity among human-induced pluripotent stem cell lines.

机译:人类诱导的多能干细胞系之间的克隆遗传和造血异质性。

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摘要

Induced pluripotent stem cells (iPSCs) hold great promise for modeling human hematopoietic diseases. However, intrinsic variability in the capacities of different iPSC lines for hematopoietic development complicates comparative studies and is currently unexplained. We created and analyzed 3 separate iPSC clones from fibroblasts of 3 different normal individuals using a standardized approach that included excision of integrated reprogramming genes by Cre-Lox mediated recombination. Gene expression profiling and hematopoietic differentiation assays showed that independent lines from the same individual were generally more similar to one another than those from different individuals. However, one iPSC line (WT2.1) exhibited a distinctly different gene expression, proliferation rate, and hematopoietic developmental potential relative to all other iPSC lines. This "outlier" clone also acquired extensive copy number variations (CNVs) during reprogramming, which may be responsible for its divergent properties. Our data indicate how inherent and acquired genetic differences can influence iPSC properties, including hematopoietic potential.
机译:诱导多能干细胞(iPSC)在模拟人类造血疾病方面具有广阔的前景。然而,不同的iPSC系造血能力的内在变异性使比较研究变得复杂,目前尚无法解释。我们使用标准化方法从3个不同正常个体的成纤维细胞中创建并分析了3个独立的iPSC克隆,其中包括通过Cre-Lox介导的重组切除整合的重编程基因。基因表达谱分析和造血分化分析表明,来自同一个体的独立品系通常比来自不同个体的独立品系更为相似。然而,一个iPSC系(WT2.1)相对于所有其他iPSC系表现出明显不同的基因表达,增殖速率和造血发育潜能。该“异常”克隆在重编程期间还获得了广泛的拷贝数变异(CNV),这可能是其差异性的原因。我们的数据表明内在和后天遗传差异如何影响iPSC特性,包括造血潜能。

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