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Human Induced Pluripotent Stem Cell-Derived B Lymphocytes Express sIgM and Can Be Generated via a Hemogenic Endothelium Intermediate

机译:人类诱导的多能干细胞衍生的B淋巴细胞表达sIgM,并可以通过生血内皮中间体产生

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摘要

The differentiation of human pluripotent stem cells to the B-cell lymphoid lineage has important clinical applications that include in vitro modeling of developmental lymphogenesis in health and disease. Here, we first demonstrate the capacity of human induced pluripotent stem cells (hiPSCs) to differentiate into CD144(+)CD73(-)CD43/CD235a(-) cells, characterized as hemogenic endothelium, and show that this population is capable of differentiating to CD10(+)CD19(+) B lymphocytes. We also demonstrate that B lymphocytes generated from hiPSCs are able to undergo full VDJ rearrangement and express surface IgM (sIgM(+)), thus representing an immature B-cell subset. Efficiency of sIgM expression on the hiPSC-derived B lymphocytes (similar to 5% of CD19(+) cells) was comparable with B lymphocytes generated from human umbilical cord blood (UCB) hematopoietic progenitor cells. Importantly, when assessed by global transcriptional profiling, hiPSC-derived B-cells show a very high level of similarity when compared with their UCB-derived counterparts, such that from more than 47,000 different transcripts, only 45 were significantly different (with a criteria adjusted P value P<0.05, log FC >1.5 or 2.8-fold). This represents a unique in vitro model to delineate critical events during lymphogeneisis in development and lymphoid diseases such as acute lymphocytic leukemia.
机译:人多能干细胞向B细胞淋巴样谱系的分化具有重要的临床应用,包括在健康和疾病中对发育性淋巴生成进行体外建模。在这里,我们首先证明了人类诱导的多能干细胞(hiPSC)分化为CD144(+)CD73(-)CD43 / CD235a(-)细胞的能力,该细胞具有造血性内皮细胞的特性,并表明该人群能够分化为CD10(+)CD19(+)B淋巴细胞。我们还证明了从hiPSC产生的B淋巴细胞能够经历完整的VDJ重排并表达表面IgM(sIgM(+)),从而代表了一个不成熟的B细胞亚群。 hiSPC来源的B淋巴细胞(约5%CD19(+)细胞)上sIgM表达的效率与人脐带血(UCB)造血祖细胞产生的B淋巴细胞相当。重要的是,通过全局转录谱评估时,hiPSC衍生的B细胞与UCB衍生的B细胞相比显示出非常高的相似性,因此在47,000多种不同的转录本中,只有45种显着不同(调整了标准P值P <0.05,log FC> 1.5或2.8倍)。这代表了独特的体外模型,用于描述发育中的淋巴细胞生成过程和淋巴样疾病(例如急性淋巴细胞白血病)中的关键事件。

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