@misc{scott_vincent_hudson_neal_jones_lavelle_campbell_halestrap_dick_theodoropoulou_2021, 
  title={Interleukin-33 regulates metabolic reprogramming of the retinal pigment epithelium in response to immune stressors.}, 
  DOI={10.1101/2021.02.04.429634}, 
  abstractNote={<jats:p>It remains unresolved how retinal pigment epithelial (RPE) cell metabolism is regulated following immune activation to maintain retinal homeostasis and retinal function. We exposed RPE to sev-eral stress signals, particularly toll-like receptor stimulation, and uncovered an ability of RPE to adapt their metabolic preference on aerobic glycolysis or oxidative glucose metabolism in re-sponse to different immune stimuli. We have identified interleukin-33 (IL-33) as a key metabolic checkpoint that antagonises the Warburg effect to ensure the functional stability of the RPE. The identification of IL-33 as a key regulator of mitochondrial metabolism suggests roles for the cytokine that go beyond its extracellular alarmin activities. IL-33 exerts control over mitochondrial respiration in RPE by facilitating oxidative pyruvate catabolism. We have also revealed that in the absence of IL-33, mitochondrial function declines and resultant bioenergetic switching is aligned with altered mitochondrial morphology. Our data not only sheds new light in the molecular pathway of activation of mitochondrial respiration in RPE in response to immune stressors, but also uncovers a novel role of nuclear intrinsic IL-33 as a metabolic check-point regulator.</jats:p>}, 
  publisher={Cold Spring Harbor Laboratory}, 
  author={Scott, Louis M and Vincent, Emma E and Hudson, Natalie and Neal, Chris and Jones, Nicholas and Lavelle, Ed and Campbell, Matthew and Halestrap, Andrew and Dick, Andrew D and Theodoropoulou, Sofia}, 
  year={2021}, 
  month={Feb}
  }