| Literature DB >> 33099406 |
Mickael Meyer1, Agnès Paquet2, Marie-Jeanne Arguel2, Ludovic Peyre1, Luis C Gomes-Pereira3, Kevin Lebrigand2, Baharia Mograbi1, Patrick Brest1, Rainer Waldmann2, Pascal Barbry2, Paul Hofman1, Jérémie Roux4.
Abstract
Non-genetic heterogeneity observed in clonal cell populations is an immediate cause of drug resistance that remains challenging to profile because of its transient nature. Here, we coupled three single-cell technologies to link the predicted drug response of a cell to its own genome-wide transcriptomic profile. As a proof of principle, we analyzed the response to tumor-necrosis-factor-related apoptosis-inducing ligand (TRAIL) in HeLa cells to demonstrate that cell dynamics can discriminate the transient transcriptional states at the origin of cell decisions such as sensitivity and resistance. Our same-cell approach, named fate-seq, can reveal the molecular factors regulating the efficacy of a drug in clonal cells, providing therapeutic targets of non-genetic drug resistance otherwise confounded in gene expression noise. A record of this paper's transparent peer review process is included in the Supplemental Information.Entities:
Keywords: cancer drug resistance; cell-to-cell variability; laser-capture microdissection; live-cell microscopy; pharmacogenomics; single-cell; systems biology; transcriptomics
Year: 2020 PMID: 33099406 DOI: 10.1016/j.cels.2020.08.019
Source DB: PubMed Journal: Cell Syst ISSN: 2405-4712 Impact factor: 10.304