Distinct Redox Signalling following Macrophage Activation Influences Profibrotic Activity.
Caitlin V LewisAntony VinhHenry DiepChrishan S SamuelGrant R DrummondBarbara K Kemp-HarperPublished in: Journal of immunology research (2019)
We show that superoxide generation is not only enhanced with stimuli associated with M1 macrophage activation but also with the M2 stimulus IL-4. Macrophages activated with IL-4 also exhibited enhanced hydrogen peroxide generation which in turn increased aortic fibroblast collagen production. Thus, M2 macrophage-derived ROS is identified as a potentially important contributor to aortic fibrosis.