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Should we consider subcellular compartmentalization of metabolites, and if so, how do we measure them?

机译:我们应该考虑代谢物的亚细胞分区化,如果是,我们如何衡量它们?

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Purpose of review To examine the consequences of metabolism compartmentalized at the subcellular level, provide prototypical examples of compartmentalized metabolism, and describe methods to examine compartmentalized metabolism. Recent findings Progress in metabolomics and isotope tracing has underscored the importance of subcellular compartments of metabolism. The discovery of biological effects of metabolites as bioenergetic intermediates, anabolic building blocks, signaling mediators, and effectors in posttranslation modifications of proteins and nucleic acids have highlighted the role of compartmentalization in determining metabolic fate. Recent advances in both direct and indirect methods to quantify compartmentalized metabolism have improved upon historical approaches. Genetically encoded metabolite sensors, chemical probes, immunoaffinity purification, and compartment-resolved metabolic modeling have all been recently applied to study compartmentalization. Accurate measurement of metabolites in distinct subcellular compartments is important for understanding and pharmacologically targeting metabolic pathways in diverse disease contexts, including cancer, diabetes, heart failure, obesity, and regulation of the immune system. Direct and indirect approaches to quantify compartmentalized metabolism are advancing rapidly. Yet, major challenges remain in the generalizability, rigor, and interpretation of data from the available methods to quantify compartmentalized metabolism.
机译:审查目的以检查在亚细胞水平下划分的新陈代谢后果,提供分区化代谢的原型实例,并描述检查分区化代谢的方法。最近的结果表明,代谢组和同位素跟踪的进展强调了代谢亚细胞间隔的重要性。将代谢物的生物学效应作为生物能源中间体,合成代谢结构块,信号传导介质和蛋白质和核酸的后翻译修饰中的生物学作用发现突出了分隔率化在确定代谢命运时的作用。直接和间接方法的最新进展在历史方法上提高了分区化新陈代谢。遗传编码的代谢物传感器,化学探针,免疫亲和纯化和隔室分解的代谢建模已被全部应用于研究舱室化。精确测量不同亚细胞室中的代谢物,对理解和药理学靶向不同疾病环境中的代谢途径是重要的,包括癌症,糖尿病,心力衰竭,肥胖症和免疫系统的调节。量化分区代谢的直接和间接方法正在迅速推进。然而,来自可用方法的普遍性,严谨和对数据的普遍性,严谨性和解释来留有大量挑战,以量化分区化新陈代谢。

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