Renal Cortical Glucose Uptake Is Decreased in Insulin Resistance and Correlates Inversely With Serum Free-fatty Acids

Author:

Rebelos Eleni123ORCID,Mari Andrea4ORCID,Honka Miikka-Juhani135ORCID,Pekkarinen Laura16,Latva-Rasku Aino16,Laurila Sanna178,Rajander Johan9,Salminen Paulina10ORCID,Iida Hidehiro1,Ferrannini Ele11,Nuutila Pirjo136ORCID

Affiliation:

1. Turku PET Centre, University of Turku , 20520, Turku , Finland

2. Department of Clinical and Experimental Medicine, University of Pisa , Pisa, 56126 , Italy

3. InFLAMES Research Flagship, University of Turku , 20014, Turku , Finland

4. CNR Institute of Neuroscience , Padova, 35121 , Italy

5. Division of Information Science, Nara Institute of Science and Technology , Takayamacho 8916-5, Ikoma, Nara 630-0192 , Japan

6. Department of Endocrinology, Turku University Hospital , 20521, Turku , Finland

7. Heart Center, Turku University Hospital , 20521, Turku , Finland

8. Department of Medicine, University of Turku , 20520, Turku , Finland

9. Turku PET Centre, Accelerator Laboratory, Åbo Akademi University , 20521, Turku , Finland

10. Division of Digestive Surgery and Urology, Turku University Hospital , 20521, Turku , Finland

11. CNR Institute of Clinical Physiology , Pisa, 56124 , Italy

Abstract

Abstract Context Studies on human renal metabolism are scanty. Nowadays, functional imaging allows the characterization of renal metabolism in a noninvasive manner. We have recently demonstrated that fluorodeoxyglucose F18 (18F FDG) positron emission tomography can be used to analyze renal glucose uptake (GU) rates, and that the renal cortex is an insulin-sensitive tissue. Objective To confirm that renal GU is decreased in people with obesity and to test whether circulating metabolites are related to renal GU. Design, Setting and Participants Eighteen people with obesity and 18 nonobese controls were studied with [18F]FDG positron emission tomography during insulin clamp. Renal scans were obtained ∼60 minutes after [18F]FDG injection. Renal GU was measured using fractional uptake rate and after correcting for residual intratubular [18F]FDG. Circulating metabolites were measured using high-throughput proton nuclear magnetic resonance metabolomics. Results Cortical GU was higher in healthy nonobese controls compared with people with obesity (4.7 [3.4-5.6] vs 3.1 [2.2-4.3], P = .004, respectively), and it associated positively with the degree of insulin sensitivity (M value) (r = 0.42, P = .01). Moreover, cortical GU was inversely associated with circulating β-OH-butyrate (r = -0.58, P = .009), acetoacetate (r = -0.48, P = .008), citrate (r = −0.44, P = .01), and free fatty acids (r = −0.68, P < .0001), even when accounting for the M value. On the contrary, medullary GU was not associated with any clinical parameters. Conclusion These data confirm differences in renal cortical GU between people with obesity and healthy nonobese controls. Moreover, the negative correlations between renal cortex GU and free fatty acids, ketone bodies, and citrate are suggestive of substrate competition in the renal cortex.

Funder

EFSD

Emil Aaltonen Foundation

Finnish Cultural Foundation

Paulo Foundation

Maud Kuistilan Muistosäätiö

Finnish Diabetes Foundation

Finnish Medical Foundation

Finnish Diabetes Research Foundation and the Academy of Finland

Sigrid Jusélius Foundation

Publisher

The Endocrine Society

Subject

Biochemistry (medical),Clinical Biochemistry,Endocrinology,Biochemistry,Endocrinology, Diabetes and Metabolism

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