AI Article Synopsis

  • Systemic inflammation, characterized by high levels of inflammatory cytokines and macrophage infiltration, is linked to low-grade inflammation often seen in obesity without damaging the tissue involved.
  • Recent studies highlight adipose tissue inflammation as a critical factor in low-grade systemic inflammation, detailing the role of macrophage activation through toll-like receptors and metabolic damage-associated patterns.
  • Understanding these molecular mechanisms is essential for developing targeted anti-inflammatory therapies to combat cardio-metabolic diseases like insulin resistance and type 2 diabetes in obese individuals.

Article Abstract

Background: Systemic inflammation is characterised by high circulating levels of inflammatory cytokines and increased macrophage infiltration in peripheral tissues. Most importantly, this inflammatory state does not involve damage or loss of function of the infiltrated tissue, which is a distinctive feature of the low-grade systemic inflammation. The term "meta-inflammation" has also been used to refer to the low-grade systemic inflammation due to its strong relationship with the development of cardio-metabolic diseases in obesity.

Objective: A review is presented on the recent clinical and experimental evidence concerning the role of adipose tissue inflammation as a key mediator of low-grade systemic inflammation. Furthermore, the main molecular mechanisms involved in the inflammatory polarization of macrophages with the ability to infiltrate both the adipose tissue and the vascular endothelium via activation of toll-like receptors by metabolic damage-associated molecular patterns, such as advanced glycation-end products and oxidized lipoproteins, is discussed. Finally, a review is made of the pathogenic mechanisms through which the low-grade systemic inflammation contributes to develop insulin resistance, dyslipidaemia, atherogenesis, type 2 diabetes, and hypertension in obese individuals.

Conclusions: A better understanding of the molecular mechanisms of low-grade systemic inflammation in promoting cardio-metabolic diseases is necessary, in order to further design novel anti-inflammatory therapies that take into consideration clinical data, as well as the circulating levels of cytokines, immune cells, and metabolic damage-associated molecular patterns in each patient.

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Source
http://dx.doi.org/10.1016/j.circir.2015.05.041DOI Listing

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