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在糖酵解和氧化磷酸化之间做出选择:肿瘤的困境?

Choosing between glycolysis and oxidative phosphorylation: a tumor's dilemma?

作者信息

Jose Caroline, Bellance Nadège, Rossignol Rodrigue

机构信息

MRGM, Laboratoire Maladies Rares: Génétique et Métabolisme, F-33076 Bordeaux, France.

出版信息

Biochim Biophys Acta. 2011 Jun;1807(6):552-61. doi: 10.1016/j.bbabio.2010.10.012. Epub 2010 Oct 16.

Abstract

A considerable amount of knowledge has been produced during the last five years on the bioenergetics of cancer cells, leading to a better understanding of the regulation of energy metabolism during oncogenesis, or in adverse conditions of energy substrate intermittent deprivation. The general enhancement of the glycolytic machinery in various cancer cell lines is well described and recent analyses give a better view of the changes in mitochondrial oxidative phosphorylation during oncogenesis. While some studies demonstrate a reduction of oxidative phosphorylation (OXPHOS) capacity in different types of cancer cells, other investigations revealed contradictory modifications with the upregulation of OXPHOS components and a larger dependency of cancer cells on oxidative energy substrates for anabolism and energy production. This apparent conflictual picture is explained by differences in tumor size, hypoxia, and the sequence of oncogenes activated. The role of p53, C-MYC, Oct and RAS on the control of mitochondrial respiration and glutamine utilization has been explained recently on artificial models of tumorigenesis. Likewise, the generation of induced pluripotent stem cells from oncogene activation also showed the role of C-MYC and Oct in the regulation of mitochondrial biogenesis and ROS generation. In this review article we put emphasis on the description of various bioenergetic types of tumors, from exclusively glycolytic to mainly OXPHOS, and the modulation of both the metabolic apparatus and the modalities of energy substrate utilization according to tumor stage, serial oncogene activation and associated or not fluctuating microenvironmental substrate conditions. We conclude on the importance of a dynamic view of tumor bioenergetics.

摘要

在过去五年中,关于癌细胞生物能量学已产生了大量知识,这使人们对肿瘤发生过程中或能量底物间歇性剥夺的不利条件下能量代谢的调节有了更好的理解。各种癌细胞系中糖酵解机制的普遍增强已得到充分描述,最近的分析让人们对肿瘤发生过程中线粒体氧化磷酸化的变化有了更清晰的认识。虽然一些研究表明不同类型癌细胞的氧化磷酸化(OXPHOS)能力降低,但其他研究却揭示了相互矛盾的变化,即OXPHOS组分上调,且癌细胞在合成代谢和能量产生方面对氧化性能量底物的依赖性更大。这种明显矛盾的情况可由肿瘤大小、缺氧以及激活的癌基因序列的差异来解释。最近在肿瘤发生的人工模型中解释了p53、C-MYC、Oct和RAS在控制线粒体呼吸和谷氨酰胺利用方面的作用。同样,由癌基因激活产生诱导多能干细胞也显示了C-MYC和Oct在线粒体生物发生和活性氧生成调节中的作用。在这篇综述文章中,我们着重描述了从完全糖酵解型到主要氧化磷酸化型的各种生物能量类型的肿瘤,以及根据肿瘤阶段、连续癌基因激活和相关或不相关的波动微环境底物条件对代谢装置和能量底物利用方式的调节。我们得出结论,动态看待肿瘤生物能量学非常重要。

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