Rapidly induced drug adaptation mediates escape from BRAF inhibition in single melanoma cells Journal Article uri icon

Overview

abstract

  • AbstractDespite increasing numbers of effective anti-cancer therapies, successful treatment is limited by the development of drug resistance. While the contribution of genetic factors to drug resistance is undeniable, little is known about how drug-sensitive cells first evade drug action to proliferate in drug. Here we track the response of thousands of single melanoma cells to BRAF inhibitors and show that a subset escapes drug within the first 3 days of treatment. Cell-cycle re-entry occurs via a non-genetic mechanism involving activation of mTORC1 and ATF4, validated in cultures of patient biopsies. These escapees cycle periodically in drug, incur significant DNA damage, and out-proliferate non-escapees over extended treatment. Our work reveals a mutagenesis-prone, expanding subpopulation of early drug escapees that may seed development of permanent drug resistance.

publication date

  • March 17, 2020

has restriction

  • green

Date in CU Experts

  • November 17, 2020 10:37 AM

Full Author List

  • Yang C; Tian C; Hoffman TE; Jacobsen NK; Spencer SL

author count

  • 5

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