Department of Molecular Biology, College of Natural Sciences, Pusan National University, Pusan 609-735, Republic of Korea.
Department of Internal Medicine and Institute of Health Science, Gyeongsang National University School of Medicine and Hospital, Jinju 52828, Republic of Korea.
Oxid Med Cell Longev. 2018 Dec 23;2018:1027453. doi: 10.1155/2018/1027453. eCollection 2018.
Metastasis is a major obstacle to the efficient and successful treatment of cancer. Initiation of metastasis requires epithelial-mesenchymal transition (EMT) that is regulated by several transcription factors, including Snail and ZEB1/2. EMT is closely linked to the acquisition of cancer stem cell (CSC) properties and chemoresistance, which contribute to tumor malignancy. Tumor suppressor p53 inhibits EMT and metastasis by negatively regulating several EMT-inducing transcription factors and regulatory molecules; thus, its inhibition is crucial in EMT, invasion, metastasis, and stemness. Metabolic alterations are another hallmark of cancer. Most cancer cells are more dependent on glycolysis than on mitochondrial oxidative phosphorylation for their energy production, even in the presence of oxygen. Cancer cells enhance other oncogenic metabolic pathways, such as glutamine metabolism, pentose phosphate pathway, and the synthesis of fatty acids and cholesterol. Metabolic reprogramming in cancer is regulated by the activation of oncogenes or loss of tumor suppressors that contribute to tumor progression. Oncogenic metabolism has been recently linked closely with the induction of EMT or CSC phenotypes by the induction of several metabolic enzyme genes. In addition, several transcription factors and molecules involved in EMT or CSCs, including Snail, Dlx-2, HIF-1, STAT3, TGF-, Wnt, and Akt, regulate oncogenic metabolism. Moreover, p53 induces metabolic change by directly regulating several metabolic enzymes. The collective data indicate the importance of oncogenic metabolism in the regulation of EMT, cell invasion and metastasis, and adoption of the CSC phenotype, which all contribute to malignant transformation and tumor development. In this review, we highlight the oncogenic metabolism as a key regulator of EMT and CSC, which is related with tumor progression involving metastasis and chemoresistance. Targeting oncometabolism might be a promising strategy for the development of effective anticancer therapy.
转移是癌症有效和成功治疗的主要障碍。转移的启动需要上皮-间充质转化(EMT),这受几个转录因子的调节,包括 Snail 和 ZEB1/2。EMT 与癌症干细胞(CSC)特性的获得和化学抗性密切相关,这有助于肿瘤恶性转化。肿瘤抑制因子 p53 通过负调控几个 EMT 诱导转录因子和调节分子抑制 EMT 和转移;因此,其抑制在 EMT、侵袭、转移和干性中至关重要。代谢改变是癌症的另一个标志。大多数癌细胞比线粒体氧化磷酸化更依赖糖酵解来产生能量,即使在有氧气的情况下也是如此。癌细胞增强了其他致癌代谢途径,如谷氨酰胺代谢、戊糖磷酸途径以及脂肪酸和胆固醇的合成。癌症中的代谢重编程受致癌基因的激活或肿瘤抑制因子的失活调节,这些因素有助于肿瘤进展。最近,致癌代谢与 EMT 或 CSC 表型的诱导密切相关,通过诱导几种代谢酶基因来实现。此外,参与 EMT 或 CSCs 的几个转录因子和分子,包括 Snail、Dlx-2、HIF-1、STAT3、TGF-β、Wnt 和 Akt,调节致癌代谢。此外,p53 通过直接调节几种代谢酶来诱导代谢变化。这些数据表明,致癌代谢在 EMT、细胞侵袭和转移以及 CSC 表型的获得中的重要性,这些都有助于恶性转化和肿瘤发展。在这篇综述中,我们强调了致癌代谢作为 EMT 和 CSC 的关键调节剂的重要性,这与涉及转移和化学抗性的肿瘤进展有关。针对致癌代谢可能是开发有效抗癌治疗的有前途的策略。
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