Paracardial fat remodeling affects systemic metabolism through alcohol dehydrogenase 1
Jennifer M. Petrosino, … , Ouliana Ziouzenkova, Federica Accornero
Jennifer M. Petrosino, … , Ouliana Ziouzenkova, Federica Accornero
Published February 15, 2021
Citation Information: J Clin Invest. 2021;131(4):e141799. https://doi.org/10.1172/JCI141799.
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Research Article Cardiology Metabolism

Paracardial fat remodeling affects systemic metabolism through alcohol dehydrogenase 1

Abstract

The relationship between adiposity and metabolic health is well established. However, very little is known about the fat depot, known as paracardial fat (pCF), located superior to and surrounding the heart. Here, we show that pCF remodels with aging and a high-fat diet and that the size and function of this depot are controlled by alcohol dehydrogenase 1 (ADH1), an enzyme that oxidizes retinol into retinaldehyde. Elderly individuals and individuals with obesity have low ADH1 expression in pCF, and in mice, genetic ablation of Adh1 is sufficient to drive pCF accumulation, dysfunction, and global impairments in metabolic flexibility. Metabolomics analysis revealed that pCF controlled the levels of circulating metabolites affecting fatty acid biosynthesis. Also, surgical removal of the pCF depot was sufficient to rescue the impairments in cardiometabolic flexibility and fitness observed in Adh1-deficient mice. Furthermore, treatment with retinaldehyde prevented pCF remodeling in these animals. Mechanistically, we found that the ADH1/retinaldehyde pathway works by driving PGC-1α nuclear translocation and promoting mitochondrial fusion and biogenesis in the pCF depot. Together, these data demonstrate that pCF is a critical regulator of cardiometabolic fitness and that retinaldehyde and its generating enzyme ADH1 act as critical regulators of adipocyte remodeling in the pCF depot.

Authors

Jennifer M. Petrosino, Jacob Z. Longenecker, Srinivasagan Ramkumar, Xianyao Xu, Lisa E. Dorn, Anna Bratasz, Lianbo Yu, Santosh Maurya, Vladimir Tolstikov, Valerie Bussberg, Paul M.L. Janssen, Muthu Periasamy, Michael A. Kiebish, Gregg Duester, Johannes von Lintig, Ouliana Ziouzenkova, Federica Accornero

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Figure 6

Retinaldehyde treatment rescues pCF remodeling and metabolic disorder in Adh1-KO mice.

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Retinaldehyde treatment rescues pCF remodeling and metabolic disorder in...
(A) Schematic of daily i.p. retinaldehyde (Rald) injections. (B) pCF weight normalized to BW for the indicated genotypes and treatments. Veh, vehicle. (C) VO2max, (D) RER, and (E) carbohydrate oxidation in WT vehicle-treated, Adh1-KO vehicle-treated, and Adh1-KO mice treated with retinaldehyde for 1 month (chronic retinaldehyde [cRald]). (F) Representative H&E-stained images of pCF from mice of the indicated genotypes and treatment groups. (G) qPCR quantification of relative mtDNA abundance normalized to nuclear DNA (nDNA) content. n = 4–7 per group for each biological replicate. Data are presented as the mean ± SEM for bar graphs, as dot plots indicating mean points over the course of a test, and as 2D area charts for oxidation graphs. Data were analyzed by 1-way ANOVA with Tukey’s HSD multiple-comparison test. Asterisks indicate significance compared with the WT vehicle-treated group and the pound symbol indicates significance between Adh1-KO vehicle and Adh1-KO chronic retinaldehyde treatment groups at a significance level of P = 0.05.