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用于追踪人类细胞命运的合成记忆电路。

Synthetic memory circuits for tracking human cell fate.

机构信息

Department of Systems Biology, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

Genes Dev. 2012 Jul 1;26(13):1486-97. doi: 10.1101/gad.189035.112.

Abstract

A variety of biological phenomena, from disease progression to stem cell differentiation, are typified by a prolonged cellular response to a transient environmental cue. While biologically relevant, heterogeneity in these long-term responses is difficult to assess at the population level, necessitating the development of biological tools to track cell fate within subpopulations. Here we present a novel synthetic biology approach for identifying and tracking mammalian cell subpopulations. We constructed three genomically integrated circuits that use bistable autoregulatory transcriptional feedback to retain memory of exposure to brief stimuli. These "memory devices" are used to isolate and track the progeny of cells that responded differentially to doxycycline, hypoxia, or DNA-damaging agents. Following hypoxic or ultraviolet radiation exposure, strongly responding cells activate the memory device and exhibit changes in gene expression, growth rates, and viability for multiple generations after the initial stimulus. Taken together, these results indicate that a heritable memory of hypoxia and DNA damage exists in subpopulations that differ in long-term cell behavior.

摘要

多种生物现象,从疾病进展到干细胞分化,其特征是细胞对短暂环境线索的长时间反应。虽然具有生物学意义,但这些长期反应的异质性在群体水平上很难评估,因此需要开发生物工具来跟踪亚群中的细胞命运。在这里,我们提出了一种用于识别和跟踪哺乳动物细胞亚群的新合成生物学方法。我们构建了三个基因组整合的电路,这些电路使用双稳态自调节转录反馈来保留对短暂刺激暴露的记忆。这些“记忆装置”用于分离和跟踪对强力霉素、缺氧或 DNA 损伤剂有不同反应的细胞的后代。在缺氧或紫外线辐射暴露后,强烈反应的细胞激活记忆装置,并在初始刺激后多个代中表现出基因表达、生长速率和活力的变化。总之,这些结果表明,在长期细胞行为不同的亚群中存在缺氧和 DNA 损伤的可遗传记忆。

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