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首页> 外文期刊>Philosophical Transactions of the Royal Society of London, Series B. Biological Sciences >Using heterokaryons to understand pluripotency and reprogramming
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Using heterokaryons to understand pluripotency and reprogramming

机译:使用异核体了解多能性和重编程

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摘要

Reprogramming differentiated cells towards pluripotency can be achieved by different experimental strategies including the forced expression of specific ‘inducers’ and nuclear transfer. While these offer unparalleled opportunities to generate stem cells and advance disease modelling, the relatively low levels of successful reprogramming achieved (1–2%) makes a direct analysis of the molecular events associated with productive reprogramming very challenging. The generation of transient heterokaryons between human differentiated cells (such as lymphocytes or fibroblasts) and mouse pluripotent stem cell lines results in a much higher frequency of successful conversion (15% SSEA4 expressing cells) and provides an alternative approach to study early events during reprogramming. Under these conditions, differentiated nuclei undergo a series of remodelling events before initiating human pluripotent gene expression and silencing differentiation-associated genes. When combined with genetic or RNAi-based approaches and high-throughput screens, heterokaryon studies can provide important new insights into the factors and mechanisms required to reprogramme unipotent cells towards pluripotency.
机译:通过不同的实验策略,包括强迫表达特定的“诱导物”和核转移,可以实现分化细胞向多能性的重编程。尽管这些为生成干细胞和推进疾病建模提供了无与伦比的机会,但是成功实现相对较低的成功重编程水平(1-2%)使得直接分析与生产性重编程相关的分子事件非常具有挑战性。在人类分化细胞(例如淋巴细胞或成纤维细胞)和小鼠多能干细胞系之间产生瞬时异核体会导致成功转化的频率更高(15%SSEA4表达细胞),并提供了另一种方法来研究重编程期间的早期事件。在这些条件下,分化的核在开始人类多能基因表达和沉默分化相关基因之前经历了一系列重塑事件。当与基于遗传或RNAi的方法和高通量筛选相结合时,异核体研究可以为将单能细胞重新编程为多能性所需的因素和机制提供重要的新见解。

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