Citations to this article

Tissue-specific metabolic reprogramming drives nutrient flux in diabetic complications
Kelli M. Sas, … , Frank C. Brosius III, Subramaniam Pennathur
Kelli M. Sas, … , Frank C. Brosius III, Subramaniam Pennathur
Published September 22, 2016
Citation Information: JCI Insight. 2016;1(15):e86976. https://doi.org/10.1172/jci.insight.86976.
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Research Article Metabolism Nephrology

Tissue-specific metabolic reprogramming drives nutrient flux in diabetic complications

Abstract

Diabetes is associated with altered cellular metabolism, but how altered metabolism contributes to the development of diabetic complications is unknown. We used the BKS db/db diabetic mouse model to investigate changes in carbohydrate and lipid metabolism in kidney cortex, peripheral nerve, and retina. A systems approach using transcriptomics, metabolomics, and metabolic flux analysis identified tissue-specific differences, with increased glucose and fatty acid metabolism in the kidney, a moderate increase in the retina, and a decrease in the nerve. In the kidney, increased metabolism was associated with enhanced protein acetylation and mitochondrial dysfunction. To confirm these findings in human disease, we analyzed diabetic kidney transcriptomic data and urinary metabolites from a cohort of Southwestern American Indians. The urinary findings were replicated in 2 independent patient cohorts, the Finnish Diabetic Nephropathy and the Family Investigation of Nephropathy and Diabetes studies. Increased concentrations of TCA cycle metabolites in urine, but not in plasma, predicted progression of diabetic kidney disease, and there was an enrichment of pathways involved in glycolysis and fatty acid and amino acid metabolism. Our findings highlight tissue-specific changes in metabolism in complication-prone tissues in diabetes and suggest that urinary TCA cycle intermediates are potential prognostic biomarkers of diabetic kidney disease progression.

Authors

Kelli M. Sas, Pradeep Kayampilly, Jaeman Byun, Viji Nair, Lucy M. Hinder, Junguk Hur, Hongyu Zhang, Chengmao Lin, Nathan R. Qi, George Michailidis, Per-Henrik Groop, Robert G. Nelson, Manjula Darshi, Kumar Sharma, Jeffrey R. Schelling, John R. Sedor, Rodica Pop-Busui, Joel M. Weinberg, Scott A. Soleimanpour, Steven F. Abcouwer, Thomas W. Gardner, Charles F. Burant, Eva L. Feldman, Matthias Kretzler, Frank C. Brosius III, Subramaniam Pennathur

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Citations to this article in year 2018 (9)

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The Warburg Effect in Diabetic Kidney Disease
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S Park, JH Jeon, BK Min, CM Ha, T Thoudam, BY Park, IK Lee 		Diabetes & Metabolism Journal 2018
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An integrative systems biology approach for precision medicine in diabetic kidney disease
S Mulder, H Hamidi, M Kretzler, W Ju 		Diabetes, obesity & metabolism 2018
Dyslipidemia impairs mitochondrial trafficking and function in sensory neurons
AE Rumora, SI Lentz, LM Hinder, SW Jackson, A Valesano, GE Levinson, EL Feldman 		The FASEB Journal 2018
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Risk factors for retinal microvascular impairment in type 2 diabetic patients without diabetic retinopathy
DH Lee, HC Yi, SH Bae, JH Cho, SW Choi, H Kim, RA Malik 		PloS one 2018

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