IDH1 mutations alter citric acid cycle metabolism and increase dependence on oxidative mitochondrial metabolism

IDH1突变会改变柠檬酸循环代谢,并增加对氧化性线粒体代谢的依赖性。

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作者:Alexandra R Grassian,Seth J Parker,Shawn M Davidson,Ajit S Divakaruni,Courtney R Green,Xiamei Zhang,Kelly L Slocum,Minying Pu,Fallon Lin,Chad Vickers,Carol Joud-Caldwell,Franklin Chung,Hong Yin,Erika D Handly,Christopher Straub,Joseph D Growney,Matthew G Vander Heiden,Anne N Murphy,Raymond Pagliarini,Christian M Metallo

Abstract

Oncogenic mutations in isocitrate dehydrogenase 1 and 2 (IDH1/2) occur in several types of cancer, but the metabolic consequences of these genetic changes are not fully understood. In this study, we performed (13)C metabolic flux analysis on a panel of isogenic cell lines containing heterozygous IDH1/2 mutations. We observed that under hypoxic conditions, IDH1-mutant cells exhibited increased oxidative tricarboxylic acid metabolism along with decreased reductive glutamine metabolism, but not IDH2-mutant cells. However, selective inhibition of mutant IDH1 enzyme function could not reverse the defect in reductive carboxylation activity. Furthermore, this metabolic reprogramming increased the sensitivity of IDH1-mutant cells to hypoxia or electron transport chain inhibition in vitro. Lastly, IDH1-mutant cells also grew poorly as subcutaneous xenografts within a hypoxic in vivo microenvironment. Together, our results suggest therapeutic opportunities to exploit the metabolic vulnerabilities specific to IDH1 mutation.

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