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线粒体溶质载体SLC25在癌症代谢重编程中的作用:当前见解与未来展望

The Role of Mitochondrial Solute Carriers SLC25 in Cancer Metabolic Reprogramming: Current Insights and Future Perspectives.

作者信息

Ahmed Amer, Iaconisi Giorgia Natalia, Di Molfetta Daria, Coppola Vincenzo, Caponio Antonello, Singh Ansu, Bibi Aasia, Capobianco Loredana, Palmieri Luigi, Dolce Vincenza, Fiermonte Giuseppe

机构信息

Department of Biosciences, Biotechnologies and Biopharmaceutics, University of Bari, 70125 Bari, Italy.

Department of Biological and Environmental Sciences and Technologies, University of Salento, 73100 Lecce, Italy.

出版信息

Int J Mol Sci. 2024 Dec 26;26(1):92. doi: 10.3390/ijms26010092.

Abstract

Cancer cells undergo remarkable metabolic changes to meet their high energetic and biosynthetic demands. The Warburg effect is the most well-characterized metabolic alteration, driving cancer cells to catabolize glucose through aerobic glycolysis to promote proliferation. Another prominent metabolic hallmark of cancer cells is their increased reliance on glutamine to replenish tricarboxylic acid (TCA) cycle intermediates essential for ATP production, aspartate and fatty acid synthesis, and maintaining redox homeostasis. In this context, mitochondria, which are primarily used to maintain energy homeostasis and support balanced biosynthesis in normal cells, become central organelles for fulfilling the heightened biosynthetic and energetic demands of proliferating cancer cells. Mitochondrial coordination and metabolite exchange with other cellular compartments are crucial. The human SLC25 mitochondrial carrier family, comprising 53 members, plays a pivotal role in transporting TCA intermediates, amino acids, vitamins, nucleotides, and cofactors across the inner mitochondrial membrane, thereby facilitating this cross-talk. Numerous studies have demonstrated that mitochondrial carriers are altered in cancer cells, actively contributing to tumorigenesis. This review comprehensively discusses the role of SLC25 carriers in cancer pathogenesis and metabolic reprogramming based on current experimental evidence. It also highlights the research gaps that need to be addressed in future studies. Understanding the involvement of these carriers in tumorigenesis may provide valuable novel targets for drug development.

摘要

癌细胞会发生显著的代谢变化,以满足其对能量和生物合成的高需求。瓦伯格效应是最具特征的代谢改变,促使癌细胞通过有氧糖酵解分解葡萄糖以促进增殖。癌细胞的另一个突出的代谢特征是它们对谷氨酰胺的依赖性增加,以补充三羧酸(TCA)循环中间体,这些中间体对于ATP生成、天冬氨酸和脂肪酸合成以及维持氧化还原稳态至关重要。在这种情况下,线粒体在正常细胞中主要用于维持能量稳态并支持平衡的生物合成,而在线粒体在满足增殖癌细胞增加的生物合成和能量需求方面成为核心细胞器。线粒体与其他细胞区室的协调和代谢物交换至关重要。人类SLC25线粒体载体家族由53个成员组成,在跨线粒体内膜转运TCA中间体、氨基酸、维生素、核苷酸和辅因子方面发挥着关键作用,从而促进这种相互作用。大量研究表明,线粒体载体在癌细胞中发生改变,积极促进肿瘤发生。本综述基于当前的实验证据全面讨论了SLC25载体在癌症发病机制和代谢重编程中的作用。它还强调了未来研究中需要解决的研究空白。了解这些载体在肿瘤发生中的作用可能为药物开发提供有价值的新靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f36/11719790/70e5223a9f7a/ijms-26-00092-g001.jpg

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