| Literature DB >> 32791100 |
Sheng Hui1, Alexis J Cowan2, Xianfeng Zeng2, Lifeng Yang2, Tara TeSlaa2, Xiaoxuan Li2, Caroline Bartman2, Zhaoyue Zhang2, Cholsoon Jang2, Lin Wang2, Wenyun Lu2, Jennifer Rojas3, Joseph Baur3, Joshua D Rabinowitz4.
Abstract
Mammalian organs are nourished by nutrients carried by the blood circulation. These nutrients originate from diet and internal stores, and can undergo various interconversions before their eventual use as tissue fuel. Here we develop isotope tracing, mass spectrometry, and mathematical analysis methods to determine the direct sources of circulating nutrients, their interconversion rates, and eventual tissue-specific contributions to TCA cycle metabolism. Experiments with fifteen nutrient tracers enabled extensive accounting for both circulatory metabolic cycles and tissue TCA inputs, across fed and fasted mice on either high-carbohydrate or ketogenic diet. We find that a majority of circulating carbon flux is carried by two major cycles: glucose-lactate and triglyceride-glycerol-fatty acid. Futile cycling through these pathways is prominent when dietary content of the associated nutrients is low, rendering internal metabolic activity robust to food choice. The presented in vivo flux quantification methods are broadly applicable to different physiological and disease states.Entities:
Keywords: TCA cycle; circulating metabolites; energy metabolism; in vivo flux quantification; isotope tracing; ketogenic diet; metabolic cycling
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Year: 2020 PMID: 32791100 PMCID: PMC7544659 DOI: 10.1016/j.cmet.2020.07.013
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 31.373