Metabolic importance of adipose tissue monoacylglycerol acyltransferase 1 in mice and humans

Liss, Kim; Lutkewitte, Andrew J.; Pietka, Terri; Finck, Brian N.; Franczyk, Michael P.; Yoshino, Jun; Klein, Samuel; Hall, A. Rupert

doi:10.1194/jlr.m084947

Cited by 25 publications

(49 citation statements)

References 28 publications

(32 reference statements)

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“…A limitation of the current study is that the ASO targeting Mogat1 leads to diminished expression of this enzyme systemically (mainly liver and adipose tissue) rather than a tissue-specific manner. This may be important because we have recently shown that Mogat1 is robustly induced in adipocytes during differentiation and is involved in reesterifying fatty acids to prevent their efflux from these cells (35). There are several points that suggest that the present observations are not due to adipose effects of the ASO.…”

Section: Discussionmentioning

confidence: 68%

“…There was also no observed effect of the Mogat1 ASO on plasma FFAs, MAG concentration, or the relative abundances of several species of lipids. Lastly, our previous work has suggested that the effects of adipocyte MGAT activity on fatty acid retention is most important in the fed state and does not affect lipolytic flux in the fasted state (35). Nonetheless, we cannot exclude the possibility that depletion of Mogat1 in adipose tissue by the ASO does not factor into the phenotype of our mice.…”

Section: Discussionmentioning

confidence: 85%

See 1 more Smart Citation

Hepatic monoacylglycerol acyltransferase 1 is induced by prolonged food deprivation to modulate the hepatic fasting response

Lutkewitte

McCommis

Schweitzer

et al. 2019

Journal of Lipid Research

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Section: Discussionmentioning

confidence: 68%

Section: Discussionmentioning

confidence: 85%

Hepatic monoacylglycerol acyltransferase 1 is induced by prolonged food deprivation to modulate the hepatic fasting response

Lutkewitte

McCommis

Schweitzer

et al. 2019

Journal of Lipid Research

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“…However, adipocyte proliferation rates, determined in vivo by measurement of the incorporation of ingested deuterium into the DNA of adipocytes isolated from SAAT, have been reported as either not different (106) or lower (107) in people who were overweight/obese and insulin sensitive than in people who were overweight/obese and insulin resistant. The capacity for lipogenesis in SAAT, assessed as expression of genes involved in lipogenic pathways (CD36, GLUT4, ChREBP, FASN, and MOGAT1), is greater in people with MHO than MUO (101,102,108,109). Moreover, the expression of these genes is positively correlated with insulin sensitivity (108,109), and increases more after moderate weight gain in people with MHO than MUO (110).…”

Section: Review Series: Mechanisms Underlying the Metabolic Syndromementioning

confidence: 99%

“…The capacity for lipogenesis in SAAT, assessed as expression of genes involved in lipogenic pathways (CD36, GLUT4, ChREBP, FASN, and MOGAT1), is greater in people with MHO than MUO (101,102,108,109). Moreover, the expression of these genes is positively correlated with insulin sensitivity (108,109), and increases more after moderate weight gain in people with MHO than MUO (110). Collectively, these data refute the notion that impaired adipogenesis contributes to insulin resistance in people with MUO (111), but demonstrate that increased adipose tissue gene expression of lipogenic pathways is associated with metabolic health.…”

Section: Review Series: Mechanisms Underlying the Metabolic Syndromementioning

confidence: 99%

Metabolically healthy obesity: facts and fantasies

Smith¹,

Mittendorfer²,

Klein³

2019

Journal of Clinical Investigation

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371

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“…Mogat1 expression is induced during adipogenesis. Mogat1 plays an important role in adipocyte differentiation by contributing to the production and accumulation of triglycerides by catalyzing the conversion of mono-acylglycerides to di-acylglycerides, which are subsequently converted to tri-acylglycerides 66 . The correlation between Nnat and Mogat1 is non-linear, which supports our proposed model that Nnat affects Mogat1 by regulating activation of CREB.…”

Section: Discussionmentioning

confidence: 99%

Epistatic Networks Associated with Parent-of-Origin Effects on Metabolic Traits

Macias-Velasco¹,

Pierre²,

Wayhart³

et al. 2019

Preprint

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Parent-of-origin effects (POE) are unexpectedly common in complex traits, including metabolic and neurological diseases. POE can also be modified by the environment, but the architecture of these gene-by-environmental effects on phenotypes remains to be unraveled. Previously, quantitative trait loci (QTL) showing context-specific POE on metabolic traits were mapped in the F16 generation of an advanced intercross between LG/J and SM/J inbred mice. However, these QTL were not enriched for known imprinted genes, suggesting another mechanism is needed to explain these POE phenomena.Here, we use a simple yet powerful F1 reciprocal cross model to test the hypothesis that non-imprinted genes can generate complex POE on metabolic traits through genetic interactions with imprinted genes.Male and female mice from a F1 reciprocal cross of LG/J and SM/J strains were fed either high or low fat diets. We generated expression profiles from three metabolically-relevant tissues: hypothalamus, white adipose, and liver. We identified two classes of parent-of-origin expression biases: genes showing parent-of-origin-dependent allele-specific expression and biallelic genes that are differentially expressed by reciprocal cross. POE patterns of both gene classes are highly tissue-and context-specific, sometimes occurring only in one sex and/or diet cohort in a particular tissue. We then constructed tissue-specific interaction networks among genes from these two classes of POE. A key subset of gene pairs show significant epistasis in the F16 LG/J x SM/J advanced intercross data in cases where the biallelic gene fell within a previously-identified metabolic POE QTL interval. We highlight one such interaction in adipose, between Nnat and Mogat1, which associates with POE on multiple adiposity traits. Both genes localize to the endoplasmic reticulum of adipocytes and play a role in adipogenesis. Additionally, expression of both genes is significantly correlated in human visceral adipose tissue. The genes and networks we present here represent a set of actionable interacting candidates that can be probed to further identify the machinery driving POE on complex traits. Parent-of-origin effects, where an allele's phenotypic effect depends on whether it is inherited maternally or paternally, are associated with a wide range of common complex traits and diseases 1 .Several mechanisms can cause parent-of-origin effects on phenotype including genomic imprinting, maternal/paternal effects, and sex-biased gene-specific trinucleotide expansions 2-4 . The best characterized parent-of-origin effect on phenotype is genomic imprinting, an epigenetic process in which either the maternally or paternally inherited allele is silenced. Parent-of-origin effects are often associated with diseases related to metabolism, neurological function, or both. Metabolic diseases include transient neonatal diabetes 5-8 , type-1 diabetes 9 , type-2 diabetes 10,11 , some cancers 12,13 , metabolic syndrome, Beckwith-Wiedemann syndrome, Wilm's tumors 14 , insulinomas 12 , Si...

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Metabolic importance of adipose tissue monoacylglycerol acyltransferase 1 in mice and humans

Cited by 25 publications

References 28 publications

Hepatic monoacylglycerol acyltransferase 1 is induced by prolonged food deprivation to modulate the hepatic fasting response

Hepatic monoacylglycerol acyltransferase 1 is induced by prolonged food deprivation to modulate the hepatic fasting response

Metabolically healthy obesity: facts and fantasies

Epistatic Networks Associated with Parent-of-Origin Effects on Metabolic Traits

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