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Bidirectional crosstalk between neutrophils and adipocytes promotes adipose tissue inflammation. | LitMetric

AI Article Synopsis

  • Chronic activation of the IL-1β system in adipose tissue links to metabolic disorders, but the expression mechanism remains unclear.
  • Researchers found that neutrophils in lean mice's white adipose tissue (WAT) produced high levels of IL-1β when interacting with adipocytes, activating the NF-κB pathway.
  • This interaction also led to neutrophil accumulation before macrophages, which was influenced by leukotriene B (LTB) production, emphasizing neutrophils' previously unknown role in promoting inflammation in adipose tissue.

Article Abstract

Chronic activation of the IL-1β system in adipose tissue on metabolic disorders is well demonstrated. However, a mechanism for its expression and activation in the tissue has remained unexplored. Here, we demonstrate that IL-1β transcript was enriched in neutrophils of white adipose tissue (WAT) from lean mice. Mechanistically, the interaction of neutrophils with adipocytes induced IL-1β expression NF-κB pathway. Lipolysis of adipocytes accumulated neutrophils prior to macrophages in WAT and produced high levels of IL-1β an inflammasome pathway. Leukotriene B (LTB) production in WAT also contributed to neutrophil accumulation. Furthermore, an LTB-inflammasome axis contributed to the expression of chemotactic molecules involved in high-fat diet-induced macrophage infiltration into WAT. We have identified previously unappreciated roles for neutrophils in the development of adipose tissue inflammation: robust IL-1β production and infiltration of macrophages to initiate chronic inflammation.-Watanabe, Y., Nagai, Y., Honda, H., Okamoto, N., Yanagibashi, T., Ogasawara, M., Yamamoto, S., Imamura, R., Takasaki, I., Hara, H., Sasahara, M., Arita, M., Hida, S., Taniguchi, S., Suda, T., Takatsu, K. Bidirectional crosstalk between neutrophils and adipocytes promotes adipose tissue inflammation.

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Source
http://dx.doi.org/10.1096/fj.201900477RRDOI Listing

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