Author:
Xu Tong,Junge Jason A.,Delfarah Alireza,Lu Yi-Tsung,Arnesano Cosimo,Iqbal Maheen,Delijani Kevin,Hsieh Tien-Chan,Hodara Emmanuelle,Mehta Hemal H.,Cohen Pinchas,Graham Nicholas A.,Fraser Scott E.,Goldkorn Amir
Abstract
AbstractGenetic mutations have long been recognized as drivers of cancer drug resistance, but recent work has defined additional non-genetic mechanisms of plasticity, wherein cancer cells assume a drug resistant phenotype marked by altered epigenetic and transcriptional states. Currently, little is known about the real-time, dynamic nature of this phenotypic shift. Using a bladder cancer model of nongenetic plasticity, we discovered that rapid transition to drug resistance entails upregulation of mitochondrial gene expression and a corresponding metabolic shift towards the tricarboxylic acid cycle and oxidative phosphorylation. Based on this distinction, we were able to track cancer cell metabolic profiles in real time using fluorescence lifetime microscopy (FLIM). We observed single cells transitioning spontaneously to an oxidative phosphorylation state over hours to days, a trend that intensified with exposure to cisplatin chemotherapy. Conversely, pharmacological inhibition of oxidative phosphorylation significantly reversed the FLIM metabolic signature and reduced cisplatin resistance. These rapid, spontaneous metabolic shifts offer a new means of tracking nongenetic cancer plasticity and forestalling the emergence of drug resistance.
Funder
National Cancer Institute
2020 AACR-Bayer Innovation and Discovery Grant
Publisher
Springer Science and Business Media LLC
Cited by
9 articles.
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