| Literature DB >> 33113355 |
Luca Gerosa1, Christopher Chidley1, Fabian Fröhlich1, Gabriela Sanchez1, Sang Kyun Lim1, Jeremy Muhlich1, Jia-Yun Chen1, Sreeram Vallabhaneni1, Gregory J Baker1, Denis Schapiro2, Mariya I Atanasova1, Lily A Chylek1, Tujin Shi3, Lian Yi3, Carrie D Nicora3, Allison Claas4, Thomas S C Ng5, Rainer H Kohler5, Douglas A Lauffenburger4, Ralph Weissleder5, Miles A Miller5, Wei-Jun Qian3, H Steven Wiley6, Peter K Sorger7.
Abstract
Targeted inhibition of oncogenic pathways can be highly effective in halting the rapid growth of tumors but often leads to the emergence of slowly dividing persister cells, which constitute a reservoir for the selection of drug-resistant clones. In BRAFV600E melanomas, RAF and MEK inhibitors efficiently block oncogenic signaling, but persister cells emerge. Here, we show that persister cells escape drug-induced cell-cycle arrest via brief, sporadic ERK pulses generated by transmembrane receptors and growth factors operating in an autocrine/paracrine manner. Quantitative proteomics and computational modeling show that ERK pulsing is enabled by rewiring of mitogen-activated protein kinase (MAPK) signaling: from an oncogenic BRAFV600E monomer-driven configuration that is drug sensitive to a receptor-driven configuration that involves Ras-GTP and RAF dimers and is highly resistant to RAF and MEK inhibitors. Altogether, this work shows that pulsatile MAPK activation by factors in the microenvironment generates a persistent population of melanoma cells that rewires MAPK signaling to sustain non-genetic drug resistance.Entities:
Keywords: BRAF(V600E) melanoma; MAPK pathway; cancer persistence; kinase inhibitors; kinetic modeling; non-genetic drug resistance; signaling plasticity; systems pharmacology; targeted therapy
Year: 2020 PMID: 33113355 PMCID: PMC8009031 DOI: 10.1016/j.cels.2020.10.002
Source DB: PubMed Journal: Cell Syst ISSN: 2405-4712 Impact factor: 10.304