Baenke Franziska, Chaneton Barbara, Smith Matthew, Van Den Broek Niels, Hogan Kate, Tang Haoran, Viros Amaya, Martin Matthew, Galbraith Laura, Girotti Maria R, Dhomen Nathalie, Gottlieb Eyal, Marais Richard
Molecular Oncology Laboratory, Cancer Research UK Manchester Institute, The University of Manchester, Wilmslow Road, Manchester M20 4BX, UK.
Cancer Metabolism Research Unit, Cancer Research UK Beatson Institute, Switchback Road, Glasgow G61 1BD, UK.
Mol Oncol. 2016 Jan;10(1):73-84. doi: 10.1016/j.molonc.2015.08.003. Epub 2015 Aug 20.
BRAF inhibitors can extend progression-free and overall survival in melanoma patients whose tumors harbor mutations in BRAF. However, the majority of patients eventually develop resistance to these drugs. Here we show that BRAF mutant melanoma cells that have developed acquired resistance to BRAF inhibitors display increased oxidative metabolism and increased dependency on mitochondria for survival. Intriguingly, the increased oxidative metabolism is associated with a switch from glucose to glutamine metabolism and an increased dependence on glutamine over glucose for proliferation. We show that the resistant cells are more sensitive to mitochondrial poisons and to inhibitors of glutaminolysis, suggesting that targeting specific metabolic pathways may offer exciting therapeutic opportunities to treat resistant tumors, or to delay emergence of resistance in the first-line setting.
BRAF抑制剂可延长肿瘤携带BRAF突变的黑色素瘤患者的无进展生存期和总生存期。然而,大多数患者最终会对这些药物产生耐药性。在此我们表明,对BRAF抑制剂产生获得性耐药的BRAF突变黑色素瘤细胞表现出氧化代谢增加以及对线粒体生存依赖性增强。有趣的是,氧化代谢增加与从葡萄糖代谢向谷氨酰胺代谢的转变以及增殖过程中对谷氨酰胺而非葡萄糖的依赖性增加有关。我们发现耐药细胞对线粒体毒素和谷氨酰胺分解抑制剂更敏感,这表明靶向特定代谢途径可能为治疗耐药肿瘤或在一线治疗中延迟耐药性出现提供令人兴奋的治疗机会。
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