Inflammation of brown/beige adipose tissues in obesity and metabolic disease

Inflammation of brown/beige adipose tissues in obesity and metabolic disease

Many of the comorbidities of obesity, including type 2 diabetes and cardiovascular diseases, are related to the low‐grade chronic inflammation of white adipose tissue. Under white adipocyte stress, local infiltration of immune cells and enhanced production of pro‐inflammatory cytokines together redu...

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Veröffentlicht in:Journal of internal medicine 2018-11, Vol.284 (5), p.492-504
Hauptverfasser: Villarroya, F., Cereijo, R., Gavaldà‐Navarro, A., Villarroya, J., Giralt, M.
Format: Artikel
Sprache:eng
Schlagworte:
Adipocytes
Adipogenesis
Adipose tissue
Adipose tissue (brown)
Body fat
brown adipose
Browning
Cardiovascular diseases
cytokine
Cytokines
Diabetes mellitus
Diabetes mellitus (non-insulin dependent)
Energy expenditure
Energy storage
Heart diseases
Hyperglycemia
Hyperlipidemia
Immune system
Infiltration
Inflammation
Insulin
macrophage
Metabolic disorders
Metabolic syndrome
Metabolism
Metabolites
Obesity
Substrates
Thermogenesis
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container_end_page 504
container_issue 5
container_start_page 492
container_title Journal of internal medicine
container_volume 284
creator Villarroya, F.
Cereijo, R.
Gavaldà‐Navarro, A.
Villarroya, J.
Giralt, M.
description Many of the comorbidities of obesity, including type 2 diabetes and cardiovascular diseases, are related to the low‐grade chronic inflammation of white adipose tissue. Under white adipocyte stress, local infiltration of immune cells and enhanced production of pro‐inflammatory cytokines together reduce metabolic flexibility and lead to insulin resistance in obesity. Whereas white adipocytes act in energy storage, brown and beige adipocytes specialize in energy expenditure. Brown and beige activity protects against obesity and associated metabolic disorders, such as hyperglycaemia and hyperlipidaemia. Compared to white fat, brown adipose tissue depots are less susceptible to developing local inflammation in response to obesity; however, strong obesogenic insults ultimately induce a locally pro‐inflammatory environment in brown fat. This condition directly alters the thermogenic activity of brown fat by impairing its energy expenditure mechanism and uptake of glucose for use as a fuel substrate. Pro‐inflammatory cytokines also impair beige adipogenesis, which occurs mainly in subcutaneous adipose tissue. There is evidence that inflammatory processes occurring in perivascular adipose tissues alter their brown‐versus‐white plasticity, impair the extent of browning in these depots and favour the local release of vasculature damaging signals. In summary, the targeting of brown and beige adipose tissues by pro‐inflammatory signals and the subsequent impairment of their thermogenic and metabolite draining activities appears to represent obesity‐driven disturbances that contribute to metabolic syndrome and cardiovascular alterations in obesity. Content List – 14th Key Symposium‐“Metabolic Complications of Obesity”.
doi_str_mv 10.1111/joim.12803
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Under white adipocyte stress, local infiltration of immune cells and enhanced production of pro‐inflammatory cytokines together reduce metabolic flexibility and lead to insulin resistance in obesity. Whereas white adipocytes act in energy storage, brown and beige adipocytes specialize in energy expenditure. Brown and beige activity protects against obesity and associated metabolic disorders, such as hyperglycaemia and hyperlipidaemia. Compared to white fat, brown adipose tissue depots are less susceptible to developing local inflammation in response to obesity; however, strong obesogenic insults ultimately induce a locally pro‐inflammatory environment in brown fat. This condition directly alters the thermogenic activity of brown fat by impairing its energy expenditure mechanism and uptake of glucose for use as a fuel substrate. Pro‐inflammatory cytokines also impair beige adipogenesis, which occurs mainly in subcutaneous adipose tissue. There is evidence that inflammatory processes occurring in perivascular adipose tissues alter their brown‐versus‐white plasticity, impair the extent of browning in these depots and favour the local release of vasculature damaging signals. In summary, the targeting of brown and beige adipose tissues by pro‐inflammatory signals and the subsequent impairment of their thermogenic and metabolite draining activities appears to represent obesity‐driven disturbances that contribute to metabolic syndrome and cardiovascular alterations in obesity. 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subjects Adipocytes
Adipogenesis
Adipose tissue
Adipose tissue (brown)
Body fat
brown adipose
Browning
Cardiovascular diseases
cytokine
Cytokines
Diabetes mellitus
Diabetes mellitus (non-insulin dependent)
Energy expenditure
Energy storage
Heart diseases
Hyperglycemia
Hyperlipidemia
Immune system
Infiltration
Inflammation
Insulin
macrophage
Metabolic disorders
Metabolic syndrome
Metabolism
Metabolites
Obesity
Substrates
Thermogenesis
title Inflammation of brown/beige adipose tissues in obesity and metabolic disease
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