A modified fluctuation-test framework characterizes the population dynamics and mutation rate of colorectal cancer persister cells

Mariangela Russo(Candiolo Cancer Institute), Simone Pompei(IFOM), Alberto Sogari(Candiolo Cancer Institute), Mattia Corigliano(University of Milan), Giovanni Crisafulli(Candiolo Cancer Institute), Alberto Puliafito(Candiolo Cancer Institute), Simona Lamba(Candiolo Cancer Institute), Jessica Erriquez(Candiolo Cancer Institute), Andrea Bertotti(Candiolo Cancer Institute), Marco Gherardi(University of Milan), Federica Di Nicolantonio(Candiolo Cancer Institute), Alberto Bardelli(Candiolo Cancer Institute), Marco Cosentino Lagomarsino(University of Milan)
Nature Genetics
July 1, 2022
Cited by 68Open Access
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Abstract

Compelling evidence shows that cancer persister cells represent a major limit to the long-term efficacy of targeted therapies. However, the phenotype and population dynamics of cancer persister cells remain unclear. We developed a quantitative framework to study persisters by combining experimental characterization and mathematical modeling. We found that, in colorectal cancer, a fraction of persisters slowly replicates. Clinically approved targeted therapies induce a switch to drug-tolerant persisters and a temporary 7- to 50-fold increase of their mutation rate, thus increasing the number of persister-derived resistant cells. These findings reveal that treatment may influence persistence and mutability in cancer cells and pinpoint inhibition of error-prone DNA polymerases as a strategy to restrict tumor recurrence.


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