Immune Cell Toll-like Receptor 4 Mediates the Development of Obesity- and Endotoxemia-Associated Adipose Tissue Fibrosis

Vila, Isabelle K.; Badin, Pierre Marie; Marqués, Marie-Adeline; Monbrun, Laurent; Lefort, Corinne; Mir, Lucile; Louche, Katie; Bourlier, Virginie; Roussel, Bruno; Gui, Philippe; Grober, Jacques; Štich, Vladimír; Rossmeislová, Lenka; Zakaroff-Girard, Alexia; Bouloumié, Anne; Viguerie, Nathalie; Moro, Cédric; Tavernier, Geneviève; Langin, Dominique

doi:10.1016/j.celrep.2014.03.062

Cited by 127 publications

(121 citation statements)

References 43 publications

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“…In vivo, stimulation of lipolysis promoted accumulation of neutral lipids in ATMs without change in number and phenotypes. Lipid droplet accumulation into ATMs occurred without a change in the number of crown-like structures that result from the recruitment of macrophages around dead adipocytes, which is a TLR4-dependent mechanism [24,40,41]. These data point to the presence of lipids from dead adipocytes rather than to FAs released from lipolysis in eliciting the proinflammatory response through TLR4-dependent signalling.…”

Section: Discussionmentioning

confidence: 78%

“…To investigate the in vivo relationship between AT lipolysis and inflammation, we treated two strains of high-fat diet-fed mice in the morning with the antilipolytic drug HSLi for 15 days. C3H/HeOuJ mice have intact TLR4 signalling (WT), whereas C3H/HeJ mice show defective TLR4 signalling (TLR4 mut ) [24]. The chronic inhibition of lipolysis was shown by a robust decrease in plasma glycerol levels in the two strains (ESM Fig.…”

Section: Resultsmentioning

confidence: 99%

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Fatty acids from fat cell lipolysis do not activate an inflammatory response but are stored as triacylglycerols in adipose tissue macrophages

et al. 2015

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Aims/hypothesis Activation of macrophages by fatty acids (FAs) is a potential mechanism linking obesity to adipose tissue (AT) inflammation and insulin resistance. Here, we investigated the effects of FAs released during adipocyte lipolysis on AT macrophages (ATMs). Methods Human THP-1 macrophages were treated with media from human multipotent adipose-derived stem (hMADS) adipocytes stimulated with lipolytic drugs. Macrophages were also treated with mixtures of FAs and an inhibitor of Toll-like receptor 4, since this receptor is activated by saturated FAs.Levels of mRNA and the secretion of inflammation-related molecules were measured in macrophages. FA composition was determined in adipocytes, conditioned media and macrophages. The effect of chronic inhibition or acute activation of fat cell lipolysis on ATM response was investigated in vivo in mice. Results Whereas palmitic acid alone activates THP-1, conditioned media from hMADS adipocyte lipolysis had no effect on IL, chemokine and cytokine gene expression, and secretion by macrophages. Mixtures of FAs representing de novo lipogenesis or habitual dietary conditions also had no effect. FAs derived from adipocyte lipolysis were taken up by macrophages and stored as triacylglycerol droplets. In vivo, chronic treatment with an antilipolytic drug did not modify gene expression and number of ATMs in mice with intact or defective Tlr4. Stimulation of adipocyte lipolysis increased storage of neutral lipids by macrophages without change in number and phenotype.

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Section: Discussionmentioning

confidence: 78%

Section: Resultsmentioning

confidence: 99%

Fatty acids from fat cell lipolysis do not activate an inflammatory response but are stored as triacylglycerols in adipose tissue macrophages

et al. 2015

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“…Although opposite in terms of excess vs. deficiency of fat mass, obesity and lipodystrophy share common WAT alterations, including inflammation and macrophage infiltration, as shown in several lipodystrophic mouse models (1-3) and in patients with HIV-associated lipodystrophy (4-6). Enhanced extracellular matrix (ECM) deposition and fibrosis are additional signatures of WAT pathology in both conditions (4,7,8). These local alterations are accompanied by systemic inflammation and insulin resistance, the most prevalent outcomes of WAT dysfunction common to obesity and lipodystrophy (9).…”

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confidence: 99%

Adipose tissue adaptive response totrans‐10,cis‐12‐conjugated linoleic acid engages alternatively activated M2 macrophages

et al. 2015

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In mice, nutritional supplementation with the trans-10,cis-12 isomer of linoleic acid (t10,c12-CLA) promotes lipoatrophy, hyperinsulinemia, and macrophage infiltration in white adipose tissue (WAT). We explored the dynamics of these interrelated responses over 2 consecutive 7 d periods of t10,c12-CLA administration and withdrawal. t10,c12-CLA down-regulated lipogenic and lipolytic gene expression and increased collagen deposition, but with no evidence of cross-linking. An abundant CD45 + cell infiltrate, comprising prominently CD206 + CD11c 2 macrophages, was found in WAT in association with an anti-inflammatory gene signature. Infiltration of natural killer (NK) and dendritic cells contributed to WAT's innate immune response to t10,c12-CLA. Less abundant adaptive immune cells colonized WAT, including B, NK T, gd T, and ab T cells. By contrast, T-regulatory cell abundance was not affected. Interruption of treatment allowed recovery of WAT mass and normalization of insulinemia, coincident with regain of WAT homeostasis owing to a coordinated reversion of genic, structural, and immune deregulations. These data revealed a striking resilience of WAT after a short-term metabolic injury induced by t10,c12-CLA, which relies on alternatively activated M2 macrophage engagement. In addition, the temporal links between variations in WAT alterations and insulinemia upon t10,c12-CLA manipulation strengthen the view that WAT dysfunctional status is critically involved in altered glucose homeostasis.-Pini, M., Touch, S., Poirier, H., Dalmas, E., Niot, I., Rouault, C., Druart, C., Delzenne, N., Clément, K., André, S., Guerre-Millo, M. Adipose tissue adaptive response to trans-10,cis-12-conjugated linoleic acid engages alternatively activated M2 macrophages. It is broadly agreed that accumulation of proinflammatory macrophages is a key component of white adipose tissue (WAT) response to nutrient overload in obesity. Through the release of an array of proinflammatory chemokines and cytokines, macrophages are thought to perpetuate and propagate inflammation in WAT, leading eventually to a chronic pathologic state. Although opposite in terms of excess vs. deficiency of fat mass, obesity and lipodystrophy share common WAT alterations, including inflammation and macrophage infiltration, as shown in several lipodystrophic mouse models (1-3) and in patients with HIV-associated lipodystrophy (4-6). Enhanced extracellular matrix (ECM) deposition and fibrosis are additional signatures of WAT pathology in both conditions (4,7,8). These local alterations are accompanied by systemic inflammation and insulin resistance, the most prevalent outcomes of WAT dysfunction common to obesity and lipodystrophy (9).The time frame necessary for WAT macrophage accumulation and insulin resistance to occur is usually long, ranging from months in mice fed a high-fat diet to years in obese humans. Conversely, caloric restriction attenuates WAT inflammation and improves glycemic status in obese humans and mice after prolonged periods of weight reducti...

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“…White adipose tissue (WAT) fibrosis is significant because of its intimate relationship with WAT dysfunction, chronic inflammation, and insulin resistance in humans and mice (Khan et al 2009;Pasarica et al 2009;Divoux et al 2010;Sun et al 2013;Vila et al 2014 …”

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confidence: 99%

PDGFRα signaling drives adipose tissue fibrosis by targeting progenitor cell plasticity

et al. 2015

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Fibrosis is a common disease process in which profibrotic cells disturb organ function by secreting disorganized extracellular matrix (ECM). Adipose tissue fibrosis occurs during obesity and is associated with metabolic dysfunction, but how profibrotic cells originate is still being elucidated. Here, we use a developmental model to investigate perivascular cells in white adipose tissue (WAT) and their potential to cause organ fibrosis. We show that a Nestin-Cre transgene targets perivascular cells (adventitial cells and pericyte-like cells) in WAT, and Nestin-GFP specifically labels pericyte-like cells. Activation of PDGFRα signaling in perivascular cells causes them to transition into ECM-synthesizing profibrotic cells. Before this transition occurs, PDGFRα signaling up-regulates mTOR signaling and ribosome biogenesis pathways and perturbs the expression of a network of epigenetically imprinted genes that have been implicated in cell growth and tissue homeostasis. Isolated Nestin-GFP+ cells differentiate into adipocytes ex vivo and form WAT when transplanted into recipient mice. However, PDGFRα signaling opposes adipogenesis and generates profibrotic cells instead, which leads to fibrotic WAT in transplant experiments. These results identify perivascular cells as fibro/adipogenic progenitors in WAT and show that PDGFRα targets progenitor cell plasticity as a profibrotic mechanism.

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Immune Cell Toll-like Receptor 4 Mediates the Development of Obesity- and Endotoxemia-Associated Adipose Tissue Fibrosis

Cited by 127 publications

References 43 publications

Fatty acids from fat cell lipolysis do not activate an inflammatory response but are stored as triacylglycerols in adipose tissue macrophages

Fatty acids from fat cell lipolysis do not activate an inflammatory response but are stored as triacylglycerols in adipose tissue macrophages

Adipose tissue adaptive response totrans‐10,cis‐12‐conjugated linoleic acid engages alternatively activated M2 macrophages

PDGFRα signaling drives adipose tissue fibrosis by targeting progenitor cell plasticity

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