PPARγ is a nexus controlling alternative activation of macrophages via glutamine metabolism

Nelson, Victoria L.; Nguyen, Hoang Cong; García-Cañaveras, Juan Carlos; Briggs, Erika R.; Ho, Wesley Y.; DiSpirito, Joanna R.; Marinis, Jill M.; Hill, David R.C.; Lazar, Mitchell A.

doi:10.1101/gad.312355.118

Cited by 96 publications

(82 citation statements)

References 55 publications

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“…For the alternative activation of macrophage (IL-4), glutamine is required [57,58]. Through glutaminolysis, the alpha-ketoglutarate is generated; thus, it endorses the differentiation of macrophages M2 [59,60] peroxisome proliferator-activated receptor (PPAR alpha) which has been reported to be needed for glutamine oxidation, gene expression (IL-4) and to stimulate the respiration of a macrophage. Therefore, the metabolism of glutamine plays an essential role as a modulator and synergetic supporter for the activation of a macrophage.…”

Section: Macrophagesmentioning

confidence: 99%

RETRACTED: Glutamine Metabolism and Its Role in Immunity, a Comprehensive Review

Shah

Wang

2020

Animals

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In the body of an animal, glutamine is a plentiful and very useful amino acid. Glutamine consumption in the body of animals in normal or disease conditions is the same or higher than the glucose. Many in vivo as well as in vitro experiments have been conducted to evaluate the importance of glutamine. Glutamine is a valuable nutrient for the proliferation of the lymphocytes. It also plays a crucial role in the production of cytokines, macrophages, phagocytic, and neutrophil to kill the bacteria. Most of the metabolic organs like the liver, gut, and skeletal muscles control the circulation and availability secretion of glutamine. In catabolic and hypercatabolic conditions, glutamine can turn out to be essential and plays a vital role in metabolism; however, availability may be compromised due to the impairment of homeostasis in the inter-tissue metabolism of amino acids. This is why the supplementation of glutamine is commonly used in clinical nutrition and is especially recommended to immune-suppressed persons. Despite this, in catabolic and hyper-catabolic conditions, it is challenging due to the amino acid concentration in plasma/bloodstream and glutamine should be provided via either the oral, enteral or parenteral route. However, the effect of glutamine as an immune-based supplement has been previously recognized as many research studies conducted in vivo and in-vitro evaluated the beneficial effects of glutamine. Hence, the present study delivers a combined review of glutamine metabolism in essential organs of the cell immune system. In this review, we have also reviewed the metabolism and action of glutamine and crucial problems due to glutamine supplementation in catabolic conditions.

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Section: Macrophagesmentioning

confidence: 99%

RETRACTED: Glutamine Metabolism and Its Role in Immunity, a Comprehensive Review

Shah

Wang

2020

Animals

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“…Thus, our data and methodology provide a proof of principle for a mechanistic understanding of how natural genetic variants control individual responses to antidiabetic drugs. These principles could be extended to different cell types, such as macrophages, where PPARg is relatively abundant and TZDs generally favor an anti-inflammatory alternative activation phenotype (Nelson et al, 2018).…”

Section: Discussionmentioning

confidence: 99%

Patient Adipose Stem Cell-Derived Adipocytes Reveal Genetic Variation that Predicts Antidiabetic Drug Response

Jiang

Guan

et al. 2019

Cell Stem Cell

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“…PPARγ can sense fatty acids, and it has been shown to mediate the transcription of M2 signature genes upon oleic acid and IL4 stimulation (35). Interestingly, PPARγ was recently found to mediate M2 polarization by promoting the oxidation of glutamine (36), an amino acid that fuels OXPHOS (37). In spite of these advances, it is still not fully understood how FAO and OXPHOS are mechanistically linked to the anti-inflammatory phenotype of M2 macrophages.…”

Section: Fatty Acid Oxidation Fuels the Anti-inflammatory Function Ofmentioning

confidence: 99%

New Insights on the Role of Lipid Metabolism in the Metabolic Reprogramming of Macrophages

et al. 2020

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Macrophage activation is intimately linked to metabolic reprogramming. Inflammatory (M1) macrophages are able to sustain inflammatory responses and to kill pathogens, mostly by relying on aerobic glycolysis and fatty acid biosynthesis. Glycolysis is a fast way of producing ATP, and fatty acids serve as precursors for the synthesis of inflammatory mediators. On the opposite side, anti-inflammatory (M2) macrophages mediate the resolution of inflammation and tissue repair, switching their metabolism to fatty acid oxidation and oxidative phosphorylation. Over the years, this classical view has been challenged by recent discoveries pointing to a more complex metabolic network during macrophage activation. Lipid metabolism plays a critical role in the activation of both M1 and M2 macrophages. Recent evidence shows that fatty acid oxidation is also essential for inflammasome activation in M1 macrophages, and glycolysis is now known to fuel fatty acid oxidation in M2 macrophages. Ultimately, targeting lipid metabolism in macrophages can improve the outcome of metabolic diseases. Here, we review the main aspects of macrophage immunometabolism from the perspective of the metabolism of lipids. Building a reliable metabolic network during macrophage activation will bring us closer to targeting macrophages for improving human health.

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PPARγ is a nexus controlling alternative activation of macrophages via glutamine metabolism

Cited by 96 publications

References 55 publications

RETRACTED: Glutamine Metabolism and Its Role in Immunity, a Comprehensive Review

RETRACTED: Glutamine Metabolism and Its Role in Immunity, a Comprehensive Review

Patient Adipose Stem Cell-Derived Adipocytes Reveal Genetic Variation that Predicts Antidiabetic Drug Response

New Insights on the Role of Lipid Metabolism in the Metabolic Reprogramming of Macrophages

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