Adipose tissue glycogen accumulation is associated with obesity-linked inflammation in humans

Ceperuelo-Mallafré, Victòria; Ejarque, Miriam; Serena, Carolina; Durán, Xavier; Montori-Grau, Marta; Rodrı́guez, Miguel A.; Yanes, Óscar; Núñez‐Roa, Catalina; Roche, Kelly; Puthanveetil, Prasanth; Garrido‐Sánchez, Lourdes; Sáez, Enrique; Tinahones, Francisco J.; García-Rovés, Pablo M.; Gómèz-Foix, Anna M.; Saltiel, Alan R.; Vendrell, Joan; Fernández‐Veledo, Sonia

doi:10.1016/j.molmet.2015.10.001

Cited by 53 publications

(52 citation statements)

References 69 publications

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“…These previous findings highlight the importance of our discovery that glycogen synthase (GYS1), the key biosynthetic enzyme for the synthesis of glycogen (103), is enriched in the SOGA1 interactome. While the role of glycogen autophagy in adipocytes was only recently examined (104), it is possible to hypothesize that SOGA1 may regulate glucose and glycogen metabolism by directly cooperating with glycogen synthase and the glycogen synthase-associated protein glycogenin, which was also detected in the SOGA1…”

Section: Discussionmentioning

confidence: 99%

Characterization of the CLASP2 Protein Interaction Network Identifies SOGA1 as a Microtubule-Associated Protein

Kruse

Krantz

Barker

et al. 2017

Molecular & Cellular Proteomics

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SummaryCLASP2 is a microtubule-associated protein that undergoes insulin-stimulated phosphorylation and co-localization with reorganized actin and GLUT4 at the plasma membrane.To gain insight to the role of CLASP2 in this system, we developed and successfully executed a streamlined interactome approach and built a CLASP2 protein network in 3T3-L1 adipocytes.Using two different commercially available antibodies for CLASP2 and an antibody for epitopetagged, overexpressed CLASP2, we performed multiple affinity purification coupled with mass spectrometry (AP-MS) experiments in combination with label-free quantitative proteomics and analyzed the data with the bioinformatics tool Significance Analysis of Interactome (SAINT). We discovered that CLASP2 co-immunoprecipitates (co-IPs) the novel protein SOGA1, the microtubule-associated protein kinase MARK2, and the microtubule/actin-regulating protein G2L1. The GTPase-activating proteins AGAP1 and AGAP3 were also enriched in the CLASP2 interactome, although subsequent AGAP3 and CLIP2 interactome analysis suggests a preference of AGAP3 for CLIP2. Follow-up MARK2 interactome analysis confirmed reciprocal co-IP of CLASP2 and also revealed MARK2 can co-IP SOGA1, glycogen synthase, and glycogenin.Investigating the SOGA1 interactome confirmed SOGA1 can reciprocal co-IP both CLASP2 and MARK2 as well as glycogen synthase and glycogenin. SOGA1 was confirmed to colocalize with CLASP2 and also with tubulin, which identifies SOGA1 as a new microtubule-associated protein.These results introduce the metabolic function of these proposed novel protein networks and their relationship with microtubules as new fields of cytoskeleton-associated protein biology. 5

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Section: Discussionmentioning

confidence: 99%

Characterization of the CLASP2 Protein Interaction Network Identifies SOGA1 as a Microtubule-Associated Protein

Kruse

Krantz

Barker

et al. 2017

Molecular & Cellular Proteomics

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“…To prevent spontaneous differentiation, primary cultures of ASCs at passage 0 (P0) were grown to 90% confluence and harvested with trypsin-EDTA, and aliquots (1 × 10 6 cells) were cryopreserved in liquid nitrogen until required ( Pachon-Pena et al., 2011 ). ATMs were also isolated from the stromal vascular fraction of AT biopsies as described previously ( Ceperuelo-Mallafre et al., 2016 , Serena et al., 2016 , Titos et al., 2011 ). The AT-cell number ratio was defined as the ratio of the number of cells proliferating at P0 per gram of AT digested.…”

Section: Methodsmentioning

confidence: 99%

Crohn's Disease Disturbs the Immune Properties of Human Adipose-Derived Stem Cells Related to Inflammasome Activation

et al. 2017

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SummaryCrohn's disease (CD) is characterized by the expansion of mesenteric fat, also known as “creeping fat.” We explored the plasticity and immune properties of adipose-derived stem cells (ASCs) in the context of CD as potential key players in the development of creeping fat. Mesenteric CD-derived ASCs presented a more proliferative, inflammatory, invasive, and phagocytic phenotype than equivalent cells from healthy donors, irrespective of the clinical stage. Remarkably, ASCs from the subcutaneous depot of patients with CD also showed an activated immune response that was associated with a reduction in their immunosuppressive properties. The invasive phenotype of mesenteric CD ASCs was governed by an inflammasome-mediated inflammatory state since blocking inflammasome signaling, mainly the secretion of interleukin-1β, reversed this characteristic. Thus, CD alters the biological functions of ASCs as adipocyte precursors, but also their immune properties. Selection of ASCs with the best immunomodulatory properties is advocated for the success of cell-based therapies.

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“…Glycogen is an important carbohydrate fuel reserve and glycogen metabolism has been previously reported in myeloid cells of the immune system including dendritic cells and macrophages [14][15][16] . Our recent studies additionally found that CD8 + memory T cells actively mobilize glycogen metabolism to generate glucose-6-phosphate (G6P) via glycogenolysis and channel the G6P to the PPP 17 .…”

mentioning

confidence: 99%

Glycogen metabolism regulates macrophage-mediated acute inflammatory responses

et al. 2020

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Our current understanding of how sugar metabolism affects inflammatory pathways in macrophages is incomplete. Here, we show that glycogen metabolism is an important event that controls macrophage-mediated inflammatory responses. IFN-γ/LPS treatment stimulates macrophages to synthesize glycogen, which is then channeled through glycogenolysis to generate G6P and further through the pentose phosphate pathway to yield abundant NADPH, ensuring high levels of reduced glutathione for inflammatory macrophage survival. Meanwhile, glycogen metabolism also increases UDPG levels and the receptor P2Y 14 in macrophages. The UDPG/P2Y 14 signaling pathway not only upregulates the expression of STAT1 via activating RARβ but also promotes STAT1 phosphorylation by downregulating phosphatase TC45. Blockade of this glycogen metabolic pathway disrupts acute inflammatory responses in multiple mouse models. Glycogen metabolism also regulates inflammatory responses in patients with sepsis. These findings show that glycogen metabolism in macrophages is an important regulator and indicate strategies that might be used to treat acute inflammatory diseases.

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Adipose tissue glycogen accumulation is associated with obesity-linked inflammation in humans

Cited by 53 publications

References 69 publications

Characterization of the CLASP2 Protein Interaction Network Identifies SOGA1 as a Microtubule-Associated Protein

Characterization of the CLASP2 Protein Interaction Network Identifies SOGA1 as a Microtubule-Associated Protein

Crohn's Disease Disturbs the Immune Properties of Human Adipose-Derived Stem Cells Related to Inflammasome Activation

Glycogen metabolism regulates macrophage-mediated acute inflammatory responses

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