Oxidative Metabolism Drives Immortalization of Neural Stem Cells during Tumorigenesis.

François Bonnay, Ana Veloso,Victoria Steinmann,Thomas Köcher,Merve Deniz Abdusselamoglu,Sunanjay Bajaj,Elisa Rivelles,Lisa Landskron,Harald Esterbauer,Robert P Zinzen,Juergen A Knoblich

CELL（2020）

引用 110|浏览12

暂无评分

摘要

Metabolic reprogramming is a key feature of many cancers, but how and when it contributes to tumorigenesis remains unclear. Here we demonstrate that metabolic reprogramming induced by mitochondrial fusion can be rate-limiting for immortalization of tumor-initiating cells (TICs) and trigger their irreversible dedication to tumorigenesis. Using single-cell transcriptomics, we find that Drosophila brain tumors contain a rapidly dividing stem cell population defined by upregulation of oxidative phosphorylation (OxPhos). We combine targeted metabolomics and in vivo genetic screening to demonstrate that OxPhos is required for tumor cell immortalization but dispensable in neural stem cells (NSCs) giving rise to tumors. Employing an in vivo NADH/NAD+ sensor, we show that NSCs precisely increase OxPhos during immortalization. Blocking OxPhos or mitochondrial fusion stalls TICs in quiescence and prevents tumorigenesis through impaired NAD+ regeneration. Our work establishes a unique connection between cellular metabolism and immortalization of tumor-initiating cells.

查看译文

关键词

bioenergetics,cell immortalization,mitochondrial dynamics,neural stem cells,tumor heterogeneity,tumorigenesis

AI 理解论文

溯源树

样例

生成溯源树，研究论文发展脉络

Chat Paper

正在生成论文摘要