Glucocorticoid activation of anti-inflammatory macrophages protects against insulin resistance.
Giorgio CarattiUlrich StifelBozhena CarattiAli J M JamilKyoung-Jin ChungMichael KiehntopfMarkus H GrälerMatthias BlüherAlexander RauchJan P TuckermannPublished in: Nature communications (2023)
Insulin resistance (IR) during obesity is linked to adipose tissue macrophage (ATM)-driven inflammation of adipose tissue. Whether anti-inflammatory glucocorticoids (GCs) at physiological levels modulate IR is unclear. Here, we report that deletion of the GC receptor (GR) in myeloid cells, including macrophages in mice, aggravates obesity-related IR by enhancing adipose tissue inflammation due to decreased anti-inflammatory ATM leading to exaggerated adipose tissue lipolysis and severe hepatic steatosis. In contrast, GR deletion in Kupffer cells alone does not alter IR. Co-culture experiments show that the absence of GR in macrophages directly causes reduced phospho-AKT and glucose uptake in adipocytes, suggesting an important function of GR in ATM. GR-deficient macrophages are refractory to alternative ATM-inducing IL-4 signaling, due to reduced STAT6 chromatin loading and diminished anti-inflammatory enhancer activation. We demonstrate that GR has an important function in macrophages during obesity by limiting adipose tissue inflammation and lipolysis to promote insulin sensitivity.
Keyphrases
- adipose tissue
- insulin resistance
- anti inflammatory
- high fat diet induced
- high fat diet
- dna damage
- oxidative stress
- induced apoptosis
- polycystic ovary syndrome
- dna repair
- dna damage response
- cell cycle arrest
- metabolic syndrome
- type diabetes
- acute myeloid leukemia
- transcription factor
- weight loss
- magnetic resonance
- skeletal muscle
- binding protein
- glycemic control
- cell proliferation
- endoplasmic reticulum stress
- computed tomography
- body mass index
- liquid chromatography
- contrast enhanced