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Citations to this article

Measurement of de novo hepatic lipogenesis in humans using stable isotopes.
M K Hellerstein, … , N S Hellerstein, C H Shackleton
M K Hellerstein, … , N S Hellerstein, C H Shackleton
Published May 1, 1991
Citation Information: J Clin Invest. 1991;87(5):1841-1852. https://doi.org/10.1172/JCI115206.
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Measurement of de novo hepatic lipogenesis in humans using stable isotopes.

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Abstract

Direct measurement of de novo lipogenesis has not previously been possible in humans. We measured de novo hepatic lipogenesis in normal men by means of stable isotopes and by combining the acetylated-xenobiotic probe technique with mass isotopomer analysis of secreted very low density lipoprotein-fatty acids (VLDL-FA). Sulfamethoxazole (SMX) was administered with [13C]acetate during an overnight fast followed by refeeding with intravenous glucose (7-10 mg/kg of weight per min), oral Ensure (7-10 mg of carbohydrate/kg of weight per min), or a high-carbohydrate mixed-meal breakfast (3.5 g of carbohydrate/kg of weight). Respiratory quotients remained less than 1.0. High-performance liquid chromatography/mass spectrometry-determined enrichments in SMX-acetate attained stable plateau values, and hepatic acetyl-coenzyme A (CoA) dilution rate did not increase with refeeding (approximately 0.024 mmol/kg per min). The fraction of VLDL-palmitate derived from de novo lipogenesis was only 0.91 +/- 0.27% (fasted) and 1.64-1.97% (fed). For stearate, this was 0.37 +/- 0.08% and 0.47-0.64%. Precursor enrichments predicted from isotopomer ratios were close to measured SMX-acetate enrichments, indicating that SMX-acetate samples the true lipogenic acetyl-CoA pool. Stearate synthesis was less than palmitate and the two did not move in parallel. Estimated total VLDL-FA synthesis is less than 500 mg/day. Thus, de novo hepatic lipogenesis is a quantitatively minor pathway, consistent with gas exchange estimates; fatty acid futile cycling (oxidation/resynthesis) is not thermogenically significant; and synthesis rates of different nonessential fatty acids by human liver are not identical in nonoverfed normal men. The contribution and regulation of de novo lipogenesis in other settings can be studied using this technique.

Authors

M K Hellerstein, M Christiansen, S Kaempfer, C Kletke, K Wu, J S Reid, K Mulligan, N S Hellerstein, C H Shackleton

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Citations to this article in year 2019 (7)

Title and authors Publication Year
Improved Sensitivity for Protein Turnover Quantification by Monitoring Immonium Ion Isotopologue Abundance
TE Angel, BC Naylor, JC Price, C Evans, M Szapacs
Analytical Chemistry 2019
Separation of postprandial lipoproteins: improved purification of chylomicrons using an ApoB100 immunoaffinity method
GM Jones, R Caccavello, SP Palii, CR Pullinger, JP Kane, K Mulligan, A Gugliucci, JM Schwarz
Journal of lipid research 2019
Palmitate and Stearate are Increased in the Plasma in a 6-OHDA Model of Parkinson’s Disease
A Shah, P Han, MY Wong, R Chang, C Legido-Quigley
Metabolites 2019
An ANGPTL4–ceramide–protein kinase Cζ axis mediates chronic glucocorticoid exposure–induced hepatic steatosis and hypertriglyceridemia in mice
TC Chen, RA Lee, SL Tsai, D Kanamaluru, NE Gray, N Yiv, RT Cheang, JH Tan, JY Lee, MD Fitch, MK Hellerstein, JC Wang
The Journal of biological chemistry 2019
Growth impairment in individuals with citrin deficiency
C Numakura, Tamiya, M Ueki, T Okada, S Maisawa, K Kojima-Ishii, J Murakami, R Horikawa, D Tokuhara, K Ito, M Adachi, T Abiko, T Mitsui, K Hayasaka
Journal of Inherited Metabolic Disease 2019
Translational Research Methods in Diabetes, Obesity, and Nonalcoholic Fatty Liver Disease: A Focus on Early Phase Clinical Drug Development
AJ Krentz, C Weyer, M Hompesch
2019
The role of short-chain fatty acids in microbiota–gut–brain communication
B Dalile, LV Oudenhove, B Vervliet, K Verbeke
Nature Reviews Gastroenterology & Hepatology 2019

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