4.7 Article

Synthetic memory circuits for tracking human cell fate

Journal

GENES & DEVELOPMENT
Volume 26, Issue 13, Pages 1486-1497

Publisher

COLD SPRING HARBOR LAB PRESS, PUBLICATIONS DEPT
DOI: 10.1101/gad.189035.112

Keywords

synthetic circuit; memory; bistability; human cell fate; DNA damage; hypoxia

Funding

  1. National Science Foundation (NSF) Synthetic Biology Engineering Research Center (SynBERC)
  2. Natural Sciences and Engineering Research Council of Canada
  3. Harvard University Center for the Environment
  4. NSF SynBERC
  5. National Institutes of Health
  6. Wyss Institute for Biologically Inspired Engineering
  7. Defense Advanced Research Projects Agency

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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.

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