DNA Methylation Changes More Slowly Than Physiological States in Response to Weight Loss in Genetically Diverse Mouse Strains

Edillor, Chantle; Parks, Brian W.; Mehrabian, Margarete; Lusis, Aldons J.; Pellegrini, Matteo

doi:10.3389/fendo.2019.00882

Cited by 8 publications

(5 citation statements)

References 39 publications

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“…Interestingly, we find no evidence that genetic background affects metabolic response to HFD in HS rats. These results are surprising considering that previous work has shown a wide range of metabolic responses to HFD in inbred mouse strains, with some strains showing little to no effect while others are negatively impacted 64,65 . Genetic loci that interact with diet have also been identified in DO mice 51,53 , further suggesting that diet interacts with genetics to impact metabolic traits.…”

Section: Discussioncontrasting

confidence: 56%

Sex and genetic specific effects on behavioral, but not metabolic, responses to a high fat diet in heterogeneous stock rats

Deal

Thurman

Seshie

et al. 2022

Preprint

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Obesity is a growing epidemic associated with a range of comorbidities, including anxiety and depression. Genetics and environmental factors such as diet contribute to both adiposity and anxiety/depression. Heterogeneous stock (HS) rats are an outbred colony and useful for genetic mapping of complex traits. We have previously shown that HS male rats exhibit worsened metabolic and behavioral health in response to high fat diet (HFD). This study aims to determine if females have similar response to diet and if response to diet interacts with genetic background. We measured multiple metabolic (body weight, fat pad weight, glucose tolerance, fasting glucose and insulin) and behavioral (elevated plus maze, open field test, and forced swim test) outcomes in a large cohort of male and female rats on either HFD or low fat diet (LFD). We estimated overall heritability as well as heritability of response to diet for each outcome. Both sexes showed worsened metabolic measures when fed HFD compared to LFD. In contrast, only males exhibited altered behavioral responses to HFD relative to LFD, with no effect in females. Most metabolic and behavioral measures showed overall heritability in both sexes. In contrast, although there was some evidence for gene by diet (GxD) interactions for behavioral measures in males, GxD interactions were generally not found for the metabolic measures. These data demonstrate an important role of diet, sex and genetics in metabolic and behavioral phenotypes in HS rats, with a potential role of gene by diet interactions for behavioral outcomes only in males.

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Section: Discussioncontrasting

confidence: 56%

Sex and genetic specific effects on behavioral, but not metabolic, responses to a high fat diet in heterogeneous stock rats

Deal

Thurman

Seshie

et al. 2022

Preprint

View full text Add to dashboard Cite

show abstract

“…Still, in liver analysis of HFHS fed animals, gene expression analysis showed decreased PPARγ levels, consistent with recent reports showing PPARγ as target of epigenetic modifications after high-fat diets, which is demethylated and overexpressed after 12 weeks of HFD [ 55 ], and which is hypermethylated and downregulated after longer HFD feeding [ 56 ]. The HFHS diet has also been shown to promote epigenetic modifications, leading to changes in the expression of a set of genes involved in metabolism and homeostasis [ 57 , 58 ]. It is important to highlight that in all diets used in our study, KI animals presented decreased PPARγ expression, which may be intrinsic of this lineage, but also related to epigenetic modifications.…”

Section: Discussionmentioning

confidence: 99%

Obesity-Linked PPARγ Ser273 Phosphorylation Promotes Beneficial Effects on the Liver, despite Reduced Insulin Sensitivity in Mice

et al. 2023

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Since the removal of thiazolidinediones (TZDs) from the market, researchers have been exploring alternative anti-diabetic drugs that target PPARγ without causing adverse effects while promoting insulin sensitization by blocking serine 273 phosphorylation (Ser273 or S273). Nonetheless, the underlying mechanisms of the relationship between insulin resistance and S273 phosphorylation are still largely unknown, except for the involvement of growth differentiation factor (GDF3) regulation in the process. To further investigate potential pathways, we generated a whole organism knockin mouse line with a single S273A mutation (KI) that blocks the occurrence of its phosphorylation. Our observations of KI mice on different diets and feeding schedules revealed that they were hyperglycemic, hypoinsulinemic, presented more body fat at weaning, and presented an altered plasma and hepatic lipid profile, distinctive liver morphology and gene expression. These results suggest that total blockage of S273 phosphorylation may have unforeseen effects that, in addition to promoting insulin sensitivity, could lead to metabolic disturbances, particularly in the liver. Therefore, our findings demonstrate both the beneficial and detrimental effects of PPAR S273 phosphorylation and suggest selective modulation of this post translational modification is a viable strategy to treat type 2 diabetes.

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“…A similar conclusion may be drawn from animal studies. In mice, HFD-induced changes in DNA methylation, chromatin modifications and accessibility were to some extent reversible following the return to a normal diet and body weight, including for H3K27ac and DNA methylation ( 219 , 220 ). This included restoration of high H3K27ac enrichment at regulatory elements containing binding sites of important hepatic TF families including HNF4, SREBP and C/EBP ( 220 ).…”

Section: Altering the Liver Epigenomementioning

confidence: 99%

“…This included restoration of high H3K27ac enrichment at regulatory elements containing binding sites of important hepatic TF families including HNF4, SREBP and C/EBP ( 220 ). However, some hepatic DNA methylation marks induced by a high-fat, high-sucrose diet were reported to be more persistent and to revert more slowly than weight loss ( 219 ). The persistence of HFD-induced epigenetic changes may depend on the genetic background ( 221 ), as well as on the tissue type.…”

Section: Altering the Liver Epigenomementioning

confidence: 99%

Epigenetics of Hepatic Insulin Resistance

2021

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Insulin resistance (IR) is largely recognized as a unifying feature that underlies metabolic dysfunction. Both lifestyle and genetic factors contribute to IR. Work from recent years has demonstrated that the epigenome may constitute an interface where different signals may converge to promote IR gene expression programs. Here, we review the current knowledge of the role of epigenetics in hepatic IR, focusing on the roles of DNA methylation and histone post-translational modifications. We discuss the broad epigenetic changes observed in the insulin resistant liver and its associated pathophysiological states and leverage on the wealth of ‘omics’ studies performed to discuss efforts in pinpointing specific loci that are disrupted by these changes. We envision that future studies, with increased genomic resolution and larger cohorts, will further the identification of biomarkers of early onset hepatic IR and assist the development of targeted interventions. Furthermore, there is growing evidence to suggest that persistent epigenetic marks may be acquired over prolonged exposure to disease or deleterious exposures, highlighting the need for preventative medicine and long-term lifestyle adjustments to avoid irreversible or long-term alterations in gene expression.

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DNA Methylation Changes More Slowly Than Physiological States in Response to Weight Loss in Genetically Diverse Mouse Strains

Cited by 8 publications

References 39 publications

Sex and genetic specific effects on behavioral, but not metabolic, responses to a high fat diet in heterogeneous stock rats

Sex and genetic specific effects on behavioral, but not metabolic, responses to a high fat diet in heterogeneous stock rats

Obesity-Linked PPARγ Ser273 Phosphorylation Promotes Beneficial Effects on the Liver, despite Reduced Insulin Sensitivity in Mice

Epigenetics of Hepatic Insulin Resistance

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