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Citations to this article

Dietary dicarboxylic acids provide a nonstorable alternative fat source that protects mice against obesity
Eric S. Goetzman, … , Steven F. Dobrowolski, Birgit Schilling
Eric S. Goetzman, … , Steven F. Dobrowolski, Birgit Schilling
Published April 30, 2024
Citation Information: J Clin Invest. 2024;134(12):e174186. https://doi.org/10.1172/JCI174186.
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Dietary dicarboxylic acids provide a nonstorable alternative fat source that protects mice against obesity

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Abstract

Dicarboxylic fatty acids are generated in the liver and kidney in a minor pathway called fatty acid ω-oxidation. The effects of consuming dicarboxylic fatty acids as an alternative source of dietary fat have not been explored. Here, we fed dodecanedioic acid, a 12-carbon dicarboxylic (DC12), to mice at 20% of daily caloric intake for 9 weeks. DC12 increased metabolic rate, reduced body fat, reduced liver fat, and improved glucose tolerance. We observed DC12-specific breakdown products in liver, kidney, muscle, heart, and brain, indicating that oral DC12 escaped first-pass liver metabolism and was utilized by many tissues. In tissues expressing the “a” isoform of acyl-CoA oxidase-1 (ACOX1), a key peroxisomal fatty acid oxidation enzyme, DC12 was chain shortened to the TCA cycle intermediate succinyl-CoA. In tissues with low peroxisomal fatty acid oxidation capacity, DC12 was oxidized by mitochondria. In vitro, DC12 was catabolized even by adipose tissue and was not stored intracellularly. We conclude that DC12 and other dicarboxylic acids may be useful for combatting obesity and for treating metabolic disorders.

Authors

Eric S. Goetzman, Bob B. Zhang, Yuxun Zhang, Sivakama S. Bharathi, Joanna Bons, Jacob Rose, Samah Shah, Keaton J. Solo, Alexandra V. Schmidt, Adam C. Richert, Steven J. Mullett, Stacy L. Gelhaus, Krithika S. Rao, Sruti S. Shiva, Katherine E. Pfister, Anne Silva Barbosa, Sunder Sims-Lucas, Steven F. Dobrowolski, Birgit Schilling

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Total citations by year

Year: 2025 2024 Total
Citations: 3 5 8
Citation information
This citation data is accumulated from CrossRef, which receives citation information from participating publishers, including this journal. Not all publishers participate in CrossRef, so this information is not comprehensive. Additionally, data may not reflect the most current citations to this article, and the data may differ from citation information available from other sources (for example, Google Scholar, Web of Science, and Scopus).

Citations to this article (8)

Title and authors Publication Year
Genetically Predicted Leucine Level Mediates Association Between CD4/CD8br T Lymphocytes and Insomnia
Luo S, Yin J, Zhang J, Li P, Wen T, Li K, Tang J, Wang X, Li A, Chen L
Cellular and Molecular Neurobiology 2025
Proteomics and succinylation modification characterization in clear cell renal cell carcinoma
Yue D, Zheng M
Discover Oncology 2025
Tubule-Specific Compensatory Responses to Cpt1a Deletion in Aged Mice
Funk SD, Kern JT, Viquez OM, Sulvaran-Guel E, Koenitzer JR, Feola KC, Blum JS, Zent R, Humphreys BD, Huen SC, Gewin LS
Kidney360 2025
Dicarboxylic acids counteract the metabolic effects of a Western diet by boosting energy expenditure
1Lidia Castagneto-Gissey, 2,3Stefan R. Bornstein,3,4,5Geltrude Mingrone,
Journal of Clinical Investigation 2024
Sirt2 Regulates Liver Metabolism in a Sex-Specific Manner
Schmidt AV, Bharathi SS, Solo KJ, Bons J, Rose JP, Schilling B, Goetzman ES
Biomolecules 2024
Dodecanedioic acid prevents and reverses metabolic‐associated liver disease and obesity and ameliorates liver fibrosis in a rodent model of diet‐induced obesity
Angelini G, Russo S, Carli F, Infelise P, Panunzi S, Bertuzzi A, Caristo ME, Lembo E, Calce R, Bornstein SR, Gastaldelli A, Mingrone G
The FASEB Journal 2024
Sirtuin-5 Is Recruited to Hepatic Peroxisomes in Mice Fed Dodecanedioic Acid but Has Little Impact on the Peroxisomal Succinylome
Zhang Y, Zhang BB, Bharathi SS, Bons J, Rose JP, Shah S, Dobrowolski SF, Sims-Lucas S, Schilling B, Goetzman ES
Biomolecules 2024
The Synergistic and Opposing Roles of ω-Fatty Acid Hydroxylase (CYP4A11) and ω-1 Fatty Acid Hydroxylase (CYP2E1) in Chronic Liver Disease
Hardwick JP, Garcia V
Genome biology & molecular genetics 2024

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