Department of Chemistry, Washington University, St. Louis, MO 63130, USA.
Department of Medicine, Washington University School of Medicine, St. Louis, MO 63110, USA.
Cell Rep. 2018 Jan 9;22(2):512-522. doi: 10.1016/j.celrep.2017.12.050.
Gain-of-function mutations in isocitrate dehydrogenase 1 (IDH1) occur in multiple types of human cancer. Here, we show that these mutations significantly disrupt NADPH homeostasis by consuming NADPH for 2-hydroxyglutarate (2-HG) synthesis. Cells respond to 2-HG synthesis, but not exogenous administration of 2-HG, by increasing pentose phosphate pathway (PPP) flux. We show that 2-HG production competes with reductive biosynthesis and the buffering of oxidative stress, processes that also require NADPH. IDH1 mutants have a decreased capacity to synthesize palmitate and an increased sensitivity to oxidative stress. Our results demonstrate that, even when NADPH is limiting, IDH1 mutants continue to synthesize 2-HG at the expense of other NADPH-requiring pathways that are essential for cell viability. Thus, rather than attempting to decrease 2-HG synthesis in the clinic, the consumption of NADPH by mutant IDH1 may be exploited as a metabolic weakness that sensitizes tumor cells to ionizing radiation, a commonly used anti-cancer therapy.
异柠檬酸脱氢酶 1(IDH1)的功能获得性突变发生在多种人类癌症中。在这里,我们表明这些突变通过消耗 NADPH 用于 2-羟戊二酸(2-HG)合成,从而显著破坏 NADPH 稳态。细胞通过增加戊糖磷酸途径(PPP)通量来响应 2-HG 合成,但不响应外源性 2-HG 给药。我们表明 2-HG 的产生与还原性生物合成和氧化应激的缓冲作用竞争,这些过程也需要 NADPH。IDH1 突变体合成棕榈酸的能力降低,对氧化应激的敏感性增加。我们的结果表明,即使在 NADPH 有限的情况下,IDH1 突变体仍继续以牺牲其他需要 NADPH 的途径为代价合成 2-HG,这些途径对细胞活力至关重要。因此,与在临床上试图降低 2-HG 合成不同,突变型 IDH1 消耗 NADPH 可能被利用为代谢弱点,使肿瘤细胞对常用于癌症治疗的电离辐射敏感。
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