<i>All-Trans</i>-Retinoic Acid Enhances Mitochondrial Function in Models of Human Liver

Tripathy, Sasmita; Chapman, J. D.; Han, Chang Y; Hogarth, Cathryn A.; Arnold, Samuel; Onken, Jennifer L; Kent, Travis; Goodlett, David R.; Isoherranen, Nina

doi:10.1124/mol.116.103697

Cited by 25 publications

(22 citation statements)

References 50 publications

(64 reference statements)

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“…Overexpression of the atRAinducible RARb in mouse liver enhances fatty acid oxidation and energy expenditure (31), whereas the RARb2-specific agonist AC261066 reduces liver steatosis in HFD-fed mice (49). Increasing endogenous atRA concentrations by inhibiting the atRA-catabolic Cyp26 isozymes enhances expression of mitochondrial biogenesis markers Nrf1 and Pgc1b 5-to 10-fold (32). These data are consistent with atRA enhancing fatty acid oxidation and mitochondrial biogenesis in vivo and suggest processes contributing to the liver steatosis phenotype.…”

Section: Discussionsupporting

confidence: 54%

“…We undertook this research to reveal postnatal Rdh10 contributions to atRA function and to assess endogenous atRA actions. Previous studies focusing on specific organs or using vitamin A deficiency models revealed that atRA has widespread impact on metabolism, consistent with organ autonomous effects (15)(16)(17)20,(29)(30)(31)(32). Total Rdh10 ablation impairs the biogenesis of multiple organs, including the pancreas, and causes embryonic lethality between E10.5 and E13, but Rdh10 +/2 mice reportedly were "indistinguishable" from WT (33).…”

Section: Discussionmentioning

confidence: 56%

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Modest Decreases in Endogenous All-trans-Retinoic Acid Produced by a MouseRdh10Heterozygote Provoke Major Abnormalities in Adipogenesis and Lipid Metabolism

et al. 2018

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Pharmacological dosing of all--retinoic acid (atRA) controls adiposity in rodents by inhibiting adipogenesis and inducing fatty acid oxidation. Retinol dehydrogenases (Rdh) catalyze the first reaction that activates retinol into atRA. This study examined postnatal contributions of Rdh10 to atRA biosynthesis and physiological functions of endogenous atRA. Embryonic fibroblasts from heterozygote hypomorphs or with a total knockout exhibit decreased atRA biosynthesis and escalated adipogenesis. atRA or a retinoic acid receptor (RAR) pan-agonist reversed the phenotype. Eliminating one copy in vivo ( ) yielded a modest decrease (≤25%) in the atRA concentration of liver and adipose but increased adiposity in male and female mice fed a high-fat diet (HFD); increased liver steatosis, glucose intolerance, and insulin resistance in males fed an HFD; and activated bone marrow adipocyte formation in females, regardless of dietary fat. Chronic dosing with low-dose atRA corrected the metabolic defects. These data resolve physiological actions of endogenous atRA, reveal sex-specific effects of atRA in vivo, and establish the importance of Rdh10 to metabolic control by atRA. The consequences of a modest decrease in tissue atRA suggest that impaired retinol activation may contribute to diabesity, and low-dose atRA therapy may ameliorate adiposity and its sequelae of glucose intolerance and insulin resistance.

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Section: Discussionsupporting

confidence: 54%

Section: Discussionmentioning

confidence: 56%

Modest Decreases in Endogenous All-trans-Retinoic Acid Produced by a MouseRdh10Heterozygote Provoke Major Abnormalities in Adipogenesis and Lipid Metabolism

et al. 2018

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“…At 72 hrs, cells were harvested for mRNA analysis. CYP2D6 and SHP mRNA were quantified using q-RT-PCR (StepOnePlus ™ , Applied Biosystems, Carlsbad, CA) as previously described [27] using GAPDH as a housekeeping gene. Cells were harvested using Tri-reagent (Invitrogen, Grand Island, NY) and mRNA extracted according to the manufacturer’s recommendations.…”

Section: Methodsmentioning

confidence: 99%

“…At 72 hrs, cells were harvested for protein analysis. Western blot analysis was done to measure CYP2D6 expression with β-actin as aloading control as previously described [27]. In brief, for western blotting, proteins from HepG2 cells were extracted as whole cell extract using whole cell lysis buffer in the presence of protease (Roche Applied Science, Indianapolis, IN) and phosphatase inhibitors (1 mM β-glycerol phosphate, 2.5 mM Na-pyrophosphate, 1 mM Na 3 VO 4 ).…”

Section: Methodsmentioning

confidence: 99%

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In vitro to in vivo extrapolation of the complex drug-drug interaction of bupropion and its metabolites with CYP2D6; simultaneous reversible inhibition and CYP2D6 downregulation

Sager

Tripathy

Price

et al. 2017

Biochemical Pharmacology

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Bupropion is a widely used antidepressant and smoking cessation aid and a strong inhibitor of CYP2D6 in vivo. Bupropion is administered as a racemic mixture of R- and S-bupropion and has stereoselective pharmacokinetics. Four primary metabolites of bupropion, threo- and erythrohydrobupropion and R,R- and S,S-OH-bupropion, circulate at higher concentrations than the parent drug and are believed to contribute to the efficacy and side effects of bupropion as well as to the CYP2D6 inhibition. However, bupropion and its metabolites are only weak inhibitors of CYP2D6 in vitro, and the magnitude of the in vivo drug-drug interactions (DDI) caused by bupropion cannot be explained by the in vitro data even when CYP2D6 inhibition by the metabolites is accounted for. The aim of this study was to quantitatively explain the in vivo CYP2D6 DDI magnitude by in vitro DDI data. Bupropion and its metabolites were found to inhibit CYP2D6 stereoselectively with up to 10-fold difference in inhibition potency between enantiomers. However, the reversible inhibition or active uptake into hepatocytes did not explain the in vivo DDIs. In HepG2 cells and in plated human hepatocytes bupropion and its metabolites were found to significantly downregulate CYP2D6 mRNA in a concentration dependent manner. The in vivo DDI was quantitatively predicted by significant down-regulation of CYP2D6 mRNA and reversible inhibition of CYP2D6 by bupropion and its metabolites. This study is the first example of a clinical DDI resulting from CYP down-regulation and first demonstration of a CYP2D6 interaction resulting from transcriptional regulation.

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Hepatic retinoic acid receptor alpha mediates all‐trans retinoic acid's effect on diet‐induced hepatosteatosis

Bawa

Gopoju

et al. 2022

Hepatol Commun

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All-trans retinoic acid (AtRA) is an active metabolite of vitamin A that influences many biological processes in development, differentiation, and metabolism. AtRA functions through activation of retinoid acid receptors (RARs).AtRA is shown to ameliorate hepatic steatosis, but the underlying mechanism is not well understood. In this study, we investigated the role of hepatocyte RAR alpha (RARα) in mediating the effect of AtRA on hepatosteatosis in mice. Hepatocyte-specific Rarα −/− (L-Rarα −/− ) mice and their control mice were fed a chow diet, high-fat diet (HFD), or a high-fat/cholesterol/fructose (HFCF) diet. Some of the mice were also treated with AtRA. Loss of hepatocyte RARα-induced hepatosteatosis in chow-fed aged mice and HFD-fed mice. AtRA prevented and reversed HFCF diet-induced obesity and hepatosteatosis in the control mice but not in L-Rarα −/− mice. Furthermore, AtRA reduced hepatocyte fatty acid uptake and lipid droplet formation, dependent on hepatocyte RARα. Our data suggest that hepatocyte RARα plays an important role in preventing hepatosteatosis and mediates AtRA's effects on diet-induced hepatosteatosis.

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All-Trans-Retinoic Acid Enhances Mitochondrial Function in Models of Human Liver

Cited by 25 publications

References 50 publications

Modest Decreases in Endogenous All-trans-Retinoic Acid Produced by a MouseRdh10Heterozygote Provoke Major Abnormalities in Adipogenesis and Lipid Metabolism

Modest Decreases in Endogenous All-trans-Retinoic Acid Produced by a MouseRdh10Heterozygote Provoke Major Abnormalities in Adipogenesis and Lipid Metabolism

In vitro to in vivo extrapolation of the complex drug-drug interaction of bupropion and its metabolites with CYP2D6; simultaneous reversible inhibition and CYP2D6 downregulation

Hepatic retinoic acid receptor alpha mediates all‐trans retinoic acid's effect on diet‐induced hepatosteatosis

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