Inflammation promotes adipocyte lipolysis via IRE1 kinase | Zendy

Kevin P. Foley | Zendy; Yong Chen | Zendy; Nicole G. Barra | Zendy; Mark Heal | Zendy; Kieran Kwok | Zendy; Akhilesh K. Tamrakar | Zendy; Wendy Chi | Zendy; Brittany M. Duggan | Zendy; Brandyn D. Henriksbo | Zendy; Yong Liu | Zendy; Jonathan D. Schertzer | Zendy

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Open Access

Inflammation promotes adipocyte lipolysis via IRE1 kinase

Author(s) -

Kevin P. Foley,

Yong Chen,

Nicole G. Barra,

Mark Heal,

Kieran Kwok,

Akhilesh K. Tamrakar,

Wendy Chi,

Brittany M. Duggan,

Brandyn D. Henriksbo,

Yong Liu,

Jonathan D. Schertzer

Publication year - 2021

Publication title -

journal of biological chemistry

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.361

H-Index - 513

eISSN - 1067-8816

pISSN - 0021-9258

DOI - 10.1016/j.jbc.2021.100440

Subject(s) - lipolysis , adipocyte , inflammation , kinase , microbiology and biotechnology , chemistry , medicine , endocrinology , adipose tissue , biology

Obesity associates with inflammation, insulin resistance, and higher blood lipids. It is unclear if immune responses facilitate lipid breakdown and release from adipocytes via lipolysis in a separate way from hormones or adrenergic signals. We found that an ancient component of ER stress, inositol-requiring protein 1 (IRE1), discriminates inflammation-induced adipocyte lipolysis versus lipolysis from adrenergic or hormonal stimuli. Our data show that inhibiting IRE1 kinase activity was sufficient to block adipocyte-autonomous lipolysis from multiple inflammatory ligands, including bacterial components, certain cytokines, and thapsigargin-induced ER stress. IRE1-mediated lipolysis was specific for inflammatory triggers since IRE1 kinase activity was dispensable for isoproterenol and cAMP-induced lipolysis in adipocytes and mouse adipose tissue. IRE1 RNase activity was not associated with inflammation-induced adipocyte lipolysis. Inhibiting IRE1 kinase activity blocked NF-κB activation, interleukin-6 secretion, and adipocyte-autonomous lipolysis from inflammatory ligands. Inflammation-induced lipolysis mediated by IRE1 occurred independently from changes in insulin signaling in adipocytes, suggesting that inflammation can promote IRE1-mediated lipolysis independent of adipocyte insulin resistance. We found no role for canonical unfolded protein responses or ABL kinases in linking ER stress to IRE1-mediated lipolysis. Adiponectin-Cre-mediated IRE1 knockout in mice showed that adipocyte IRE1 was required for inflammatory ligand-induced lipolysis in adipose tissue explants and that adipocyte IRE1 was required for approximately half of the increase in blood triglycerides after a bacterial endotoxin-mediated inflammatory stimulus in vivo . Together, our results show that IRE1 propagates an inflammation-specific lipolytic program independent from hormonal or adrenergic regulation. Targeting IRE1 kinase activity may benefit metabolic syndrome and inflammatory lipid disorders.

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