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Publication : Origin and Function of Stress-Induced IL-6 in Murine Models.

First Author  Qing H Year  2020
Journal  Cell Volume  182
Issue  2 Pages  372-387.e14
PubMed ID  32610084 Mgi Jnum  J:295371
Mgi Id  MGI:6448307 Doi  10.1016/j.cell.2020.05.054
Citation  Qing H, et al. (2020) Origin and Function of Stress-Induced IL-6 in Murine Models. Cell 182(2):372-387.e14
abstractText  Acute psychological stress has long been known to decrease host fitness to inflammation in a wide variety of diseases, but how this occurs is incompletely understood. Using mouse models, we show that interleukin-6 (IL-6) is the dominant cytokine inducible upon acute stress alone. Stress-inducible IL-6 is produced from brown adipocytes in a beta-3-adrenergic-receptor-dependent fashion. During stress, endocrine IL-6 is the required instructive signal for mediating hyperglycemia through hepatic gluconeogenesis, which is necessary for anticipating and fueling "fight or flight" responses. This adaptation comes at the cost of enhancing mortality to a subsequent inflammatory challenge. These findings provide a mechanistic understanding of the ontogeny and adaptive purpose of IL-6 as a bona fide stress hormone coordinating systemic immunometabolic reprogramming. This brain-brown fat-liver axis might provide new insights into brown adipose tissue as a stress-responsive endocrine organ and mechanistic insight into targeting this axis in the treatment of inflammatory and neuropsychiatric diseases.
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