Macrophage PPARγ is required for normal skeletal muscle and hepatic insulin sensitivity and full antidiabetic effects of thiazolidinediones

Hevener, Andrea L.; Olefsky, Jerrold M.; Reichart, Donna; Nguyen, MT A; Bandyopadyhay, Gautarn; Leung, Ho-Yin; Watt, Matthew J.; Benner, Chris; Febbraio, Mark A.; Nguyen, Anh-Khoi; Folian, Brian J; Subramaniam, Shankar; Gonzalez, Frank J.; Glass, Christopher K.; Ricote, Mercedes

doi:10.1172/jci31561

Cited by 433 publications

(404 citation statements)

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“…The same effect was observed after depletion of Cd11c+ cells that correspond to the main M1 macrophage subset in muscle [242]. Inversely, even lean animals with myeloid deletion of PPAR developed muscle insulin resistance, which deteriorated in the obese state due to impaired M2 macrophage polarization [243]. In contrast, myeloid deletion of PPAR/ or TLR4 did not entail any effect on muscle insulin sensitivity [219,230].…”

Section: Obesity and Inflammationmentioning

confidence: 61%

Functional crosstalk of PGC-1 coactivators and inflammation in skeletal muscle pathophysiology

Eisele

Handschin

2013

Semin Immunopathol

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(150 -250 words) [165] Skeletal muscle is an organ involved in whole body movement and energy metabolism with the ability to dynamically adapt to different states of (dis-)use. At a molecular level, the peroxisome proliferatoractivated receptor  coactivators 1 (PGC-1) are important mediators of oxidative metabolism in skeletal muscle and in other organs. Musculoskeletal disorders as well as obesity and its sequelae are associated with PGC-1 dysregulation in muscle with a concomitant local or systemic inflammatory reaction. In this review, we outline the function of PGC-1 coactivators in physiological and pathological conditions as well as the complex interplay of metabolic dysregulation and inflammation in obesity with special focus on skeletal muscle. We further put forward the hypothesis that in this tissue, oxidative metabolism and inflammatory processes mutually antagonize each other. The nuclear factor κB (NF-B) pathway thereby plays a key role in linking metabolic and inflammatory programs in muscle cells. We conclude this review with a perspective about the consequences of such a negative crosstalk on the immune system and the possibilities this opens for clinical applications.

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Section: Obesity and Inflammationmentioning

confidence: 61%

Functional crosstalk of PGC-1 coactivators and inflammation in skeletal muscle pathophysiology

Eisele

Handschin

2013

Semin Immunopathol

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“…The relative degree of insulin resistance became more severe when these mice where subjected to HFD compared to HFD-fed controls. Interestingly, the ability of TZD treatment to improve insulin sensitivity was attenuated in these animals, indicating that the anti-inflammatory properties of TZDs in tissueresident macrophages are a component of their insulin-sensitizing effects [55].…”

Section: Cbl-associated Proteinmentioning

confidence: 98%

Inflammation and insulin resistance

2007

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Obesity-induced chronic inflammation is a key component in the pathogenesis of insulin resistance and the Metabolic syndrome. In this review, we focus on the interconnection between obesity, inflammation and insulin resistance. Proinflammatory cytokines can cause insulin resistance in adipose tissue, skeletal muscle and liver by inhibiting insulin signal transduction. The sources of cytokines in insulin resistant states are the insulin target tissue themselves, primarily fat and liver, but to a larger extent the activated tissue resident macrophages. While the initiating factors of this inflammatory response remain to be fully determined, chronic inflammation in these tissues could cause localized insulin resistance via autocrine/paracrine cytokine signaling and systemic insulin resistance via endocrine cytokine signaling all of which contribute to the abnormal metabolic state.

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“…Indeed, activation of PPARγ by pioglitazone, a thiazolidinedione class of insulin sensitizer, improves the unbalanced M1/M2 phenotype of adipose tissue macrophages in diet-induced obese mice [32]. Interestingly, a recent study suggests that antidiabetic effects of thiazolidinediones may be mediated, at least partly, through PPARγ in macrophages [33]. Moreover, both M1 and M2 markers are detected in circulating monocytes [34,35].…”

Section: Heterogeneity Of Adipose Tissue Macrophagesmentioning

confidence: 99%