Cardiac natriuretic peptides act via p38 MAPK to induce the brown fat thermogenic program in mouse and human adipocytes

Bordicchia, Marica; Liu, Dianxin; Amri, Ez-Zoubir; Ailhaud, Gérard; Dessı̀-Fulgheri, Paolo; Zhang, Chaoying; Takahashi, Nobuyuki; Sarzani, Riccardo; Collins, Sheila

doi:10.1172/jci59701

Cited by 749 publications

(579 citation statements)

References 78 publications

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“…In addition, multiple novel nonadrenergic soluble molecules that are capable of inducing BAT activity and WAT browning have been identified [53] . Although some of these molecules act indirectly by modulating sympathetic activation and the subsequent noradrenergic pathways, several agents [e.g., fibroblast growth factor-21 (FGF21) and the cardiac peptides (ANP/BNP)] appear to have direct effects on brown adipocytes and the browning process [54][55][56] . Recently, the Spiegelman group identified irisin [57] , a novel hormonal factor that converts white fat into the more thermogenic beige fat.…”

Section: Formation Of Beige/brite Adipocytes (Browning)mentioning

confidence: 99%

Distinction of white, beige and brown adipocytes derived from mesenchymal stem cells

Park

Kim

Bae

2014

WJSC

209

182

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pattern distinct from that of either white or brown fat cells. The current epidemic of obesity has increased the interest in studying adipocyte formation (adipogenesis), especially in beige/brite cells. This review summarizes the developmental process of adipose tissues that originate from the mesenchymal stem cells and the features of these three different types of adipocytes.© 2014 Baishideng Publishing Group Co., Limited. All rights reserved.Key words: White adipocytes; Brown adipocytes; Beige/ brite adipocytes; Mesenchymal stem cells; Adipogenesis; Thermogenesis; Browning Core tip: Here, we summarize the characteristic differences of the white, brown and beige adipocytes derived from mesenchymal stem cells, including their anatomical location. In particular, we focus on the newly discovered brown-like adipocytes called beige/brite adipocytes. A deeper understanding of the molecular mechanism of these adipocytes may provide clues for overcoming obesity and its associated metabolic diseases. AbstractAdipose tissue is a major metabolic organ, and it has been traditionally classified as either white adipose tissue (WAT) or brown adipose tissue (BAT). WAT and BAT are characterized by different anatomical locations, morphological structures, functions, and regulations. WAT and BAT are both involved in energy balance. WAT is mainly involved in the storage and mobilization of energy in the form of triglycerides, whereas BAT specializes in dissipating energy as heat during cold-or diet-induced thermogenesis. Recently, brownlike adipocytes were discovered in WAT. These brownlike adipocytes that appear in WAT are called beige or brite adipocytes. Interestingly, these beige/brite cells resemble white fat cells in the basal state, but they respond to thermogenic stimuli with increased levels of thermogenic genes and increased respiration rates. In addition, beige/brite cells have a gene expression

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Section: Formation Of Beige/brite Adipocytes (Browning)mentioning

confidence: 99%

Distinction of white, beige and brown adipocytes derived from mesenchymal stem cells

Park

Kim

Bae

2014

WJSC

209

182

View full text Add to dashboard Cite

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“…The master (107)). Among these, secreted factors such as ANP (NPPA), BMP8B, irisin and FGF21 that affect brown adipocyte activation and recruitment seem to be particularly promising for the development of new anti-obesity drugs in the near future (22,122,123,124,125).…”

Section: Human Adipose Organ Plasticity and Therapeutic Prospectsmentioning

confidence: 99%

MECHANISMS IN ENDOCRINOLOGY: White, brown and pink adipocytes: the extraordinary plasticity of the adipose organ

Giordano

Smorlesi

Frontini

et al. 2014

European Journal of Endocrinology

213

168

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In mammals, adipocytes are lipid-laden cells making up the parenchyma of the multi-depot adipose organ. White adipocytes store lipids for release as free fatty acids during fasting periods; brown adipocytes burn glucose and lipids to maintain thermal homeostasis. A third type of adipocyte, the pink adipocyte, has recently been characterised in mouse subcutaneous fat depots during pregnancy and lactation. Pink adipocytes are mammary gland alveolar epithelial cells whose role is to produce and secrete milk. Emerging evidence suggests that they derive from the transdifferentiation of subcutaneous white adipocytes. The functional response of the adipose organ to a range of metabolic and environmental challenges highlights its extraordinary plasticity. Cold exposure induces an increase in the 'brown' component of the organ to meet the increased thermal demand; in states of positive energy balance, the 'white' component expands to store excess nutrients; finally, the 'pink' component develops in subcutaneous depots during pregnancy to ensure litter feeding. At the cell level, plasticity is provided not only by stem cell proliferation and differentiation but also, distinctively, by direct transdifferentiation of fully differentiated adipocytes by the stimuli that induce genetic expression reprogramming and through it a change in phenotype and, consequently function. A greater understanding of adipocyte transdifferentiation mechanisms would have the potential to shed light on their biology as well as inspire novel therapeutic strategies against metabolic syndrome (browning) and breast cancer (pinking).

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“…Whereas short-term exposure of hMADS to the peroxisome proliferator-activated receptor g (PPAR g) agonist rosiglitazone induced their differentiation to white adipocytes, chronic treatment with this compound stimulated the development of brown-adipose-like cells (Elabd et al 2009). Moreover, treatment of hMADS with T3 hormone, a well-known activator thermogenesis, or with natriuretic peptides, promotes the expression of UCP1, PPARGC1A, and other factors known to promote mitochondriogenesis and mitochondrial respiration (Bordicchia et al 2012, Lee et al 2012a. Globally considered, this suggests that hMADS could possibly represent a suitable model to study the conversion of white mature adipocyte to brown-adipose-like, although cell numbers obtained are again limited.…”

Section: Human Adipose-derived Stem Cellsmentioning

confidence: 99%

Adipogenesis: new insights into brown adipose tissue differentiation

Carobbio

Rosen

Vidal-Puig

2013

Journal of Molecular Endocrinology

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Confirmation of the presence of functional brown adipose tissue (BAT) in humans has renewed interest in investigating the potential therapeutic use of this tissue. The finding that its activity positively correlates with decreased BMI, decreased fat content, and augmented energy expenditure suggests that increasing BAT mass/activity or browning of white adipose tissue (WAT) could be a strategy to prevent or treat obesity and its associated morbidities. The challenge now is to find a safe and efficient way to develop this idea. Whereas BAT has being widely studied in murine models both in vivo and in vitro, there is an urgent need for human cellular models to investigate BAT physiology and functionality from a molecular point of view. In this review, we focus on the latest insights surrounding BAT development and activation in rodents and humans. Then, we discuss how the availability of murine models has been essential to identify BAT progenitors and trace their lineage. Finally, we address how this information can be exploited to develop human cellular models for BAT differentiation/activation. In this context, human embryonic stem and induced pluripotent stem cells-based cellular models represent a resource of great potential value, as they can provide a virtually inexhaustible supply of starting material for functional genetic studies, -omics based analysis and validation of therapeutic approaches. Moreover, these cells can be readily genetically engineered, opening the possibility of generating patient-specific cellular models, allowing the investigation of the influence of different genetic backgrounds on BAT differentiation in pathological or in physiological states.

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Cardiac natriuretic peptides act via p38 MAPK to induce the brown fat thermogenic program in mouse and human adipocytes

Cited by 749 publications

References 78 publications

Distinction of white, beige and brown adipocytes derived from mesenchymal stem cells

Distinction of white, beige and brown adipocytes derived from mesenchymal stem cells

MECHANISMS IN ENDOCRINOLOGY: White, brown and pink adipocytes: the extraordinary plasticity of the adipose organ

Adipogenesis: new insights into brown adipose tissue differentiation

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