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Slow-growing cells within isogenic populations have increased RNA polymerase error rates and DNA damage.

David van DijkRiddhiman DharAlsu M MissarovaLorena EspinarWilliam R BlevinsBen LehnerLucas B Carey
Published in: Nature communications (2015)
Isogenic cells show a large degree of variability in growth rate, even when cultured in the same environment. Such cell-to-cell variability in growth can alter sensitivity to antibiotics, chemotherapy and environmental stress. To characterize transcriptional differences associated with this variability, we have developed a method--FitFlow--that enables the sorting of subpopulations by growth rate. The slow-growing subpopulation shows a transcriptional stress response, but, more surprisingly, these cells have reduced RNA polymerase fidelity and exhibit a DNA damage response. As DNA damage is often caused by oxidative stress, we test the addition of an antioxidant, and find that it reduces the size of the slow-growing population. More generally, we find a significantly altered transcriptome in the slow-growing subpopulation that only partially resembles that of cells growing slowly due to environmental and culture conditions. Slow-growing cells upregulate transposons and express more chromosomal, viral and plasmid-borne transcripts, and thus explore a larger genotypic--and so phenotypic--space.
Keyphrases
  • induced apoptosis
  • oxidative stress
  • dna damage
  • cell cycle arrest
  • endoplasmic reticulum stress
  • gene expression
  • escherichia coli
  • stem cells
  • dna repair
  • cell death
  • cell proliferation
  • climate change
  • rna seq
  • genome wide