Department of Developmental and Molecular Biology, Albert Einstein College of Medicine, Price Center for Genetic and Translational Medicine, 1301 Morris Park Avenue,Room 302, Bronx, NY 10461, USA.
Cancer Res. 2013 Sep 1;73(17):5459-72. doi: 10.1158/0008-5472.CAN-13-1429. Epub 2013 Jun 24.
Rapidly proliferating and neoplastically transformed cells generate the energy required to support rapid cell division by increasing glycolysis and decreasing flux through the oxidative phosphorylation (OXPHOS) pathway, usually without alterations in mitochondrial function. In contrast, little is known of the metabolic alterations, if any, which occur in cells harboring mutations that prime their neoplastic transformation. To address this question, we used a Pten-deficient mouse model to examine thyroid cells where a mild hyperplasia progresses slowly to follicular thyroid carcinoma. Using this model, we report that constitutive phosphoinositide 3-kinase (PI3K) activation caused by PTEN deficiency in nontransformed thyrocytes results in a global downregulation of Krebs cycle and OXPHOS gene expression, defective mitochondria, reduced respiration, and an enhancement in compensatory glycolysis. We found that this process does not involve any of the pathways classically associated with the Warburg effect. Moreover, this process was independent of proliferation but contributed directly to thyroid hyperplasia. Our findings define a novel metabolic switch to glycolysis driven by PI3K-dependent AMPK inactivation with a consequent repression in the expression of key metabolic transcription regulators.
快速增殖和癌变转化的细胞通过增加糖酵解和减少氧化磷酸化 (OXPHOS) 途径的通量来产生支持快速细胞分裂所需的能量,通常不会改变线粒体功能。相比之下,对于携带导致其癌变转化的突变的细胞中发生的代谢变化,如果有的话,我们知之甚少。为了解决这个问题,我们使用 Pten 缺陷型小鼠模型来研究甲状腺细胞,其中轻度增生缓慢进展为滤泡性甲状腺癌。使用这种模型,我们报告称,PTEN 缺陷导致非转化甲状腺细胞中组成型磷酸肌醇 3-激酶 (PI3K) 激活导致三羧酸循环和 OXPHOS 基因表达的全面下调、线粒体功能缺陷、呼吸作用降低以及代偿性糖酵解增强。我们发现,这个过程不涉及与沃伯格效应相关的任何经典途径。此外,这个过程与增殖无关,但直接导致甲状腺增生。我们的发现定义了一种新的代谢开关,即由 PI3K 依赖性 AMPK 失活驱动的糖酵解,随后关键代谢转录调节剂的表达受到抑制。
