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Blockade of Glutathione Metabolism in IDH1-Mutated Glioma.


ABSTRACT: Mutations in genes encoding isocitrate dehydrogenases (IDH) 1 and 2 are common cancer-related genetic abnormalities. Malignancies with mutated IDHs exhibit similar pathogenesis, metabolic pattern, and resistance signature. However, an effective therapy against IDH1-mutated solid tumor remains unavailable. In this study, we showed that acquisition of IDH1 mutation results in the disruption of NADP+/NADPH balance and an increased demand for glutathione (GSH) metabolism. Moreover, the nuclear factor erythroid 2-related factor 2 (Nrf2) plays a key protective role in IDH1-mutated cells by prompting GSH synthesis and reactive oxygen species scavenging. Pharmacologic inhibition of the Nrf2/GSH pathway via brusatol administration exhibited a potent tumor suppressive effect on IDH1-mutated cancer in vitro and in vivo Our findings highlight a possible therapeutic strategy that could be valuable for IDH1-mutated cancer treatment.

SUBMITTER: Tang X 

PROVIDER: S-EPMC6946871 | biostudies-literature | 2020 Jan

REPOSITORIES: biostudies-literature

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Blockade of Glutathione Metabolism in <i>IDH1</i>-Mutated Glioma.

Tang Xiaoying X   Fu Xiao X   Liu Yang Y   Yu Di D   Cai Sabrina J SJ   Yang Chunzhang C  

Molecular cancer therapeutics 20190923 1


Mutations in genes encoding isocitrate dehydrogenases (<i>IDH</i>) 1 and 2 are common cancer-related genetic abnormalities. Malignancies with mutated <i>IDHs</i> exhibit similar pathogenesis, metabolic pattern, and resistance signature. However, an effective therapy against <i>IDH1</i>-mutated solid tumor remains unavailable. In this study, we showed that acquisition of <i>IDH1</i> mutation results in the disruption of NADP<sup>+</sup>/NADPH balance and an increased demand for glutathione (GSH)  ...[more]

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