Schematic representation illustrating the protective role of the HO system in glucose metabolism. Inflammatory and oxidative mediators like NF-$\kappa$B, JNK, TGF-$\alpha$, IL1$\beta$ and IL-6 are amongst the pathophysiological factors that impair insulin signalling. Generally these substances stimulate oxidative/inflammatory events destroying tissue. Conversely, other factors including cytokines and inflammatory/oxidative transcription factors like NF-$\kappa$B, JNK stimulate a variety of different pathophysiological pathways to further aggravate oxidative/inflammatory insult, creating a vicious cycle of intense inflammation that would severely damage tissue and compromise many physiological functions including glucose metabolism. However, the HO system suppresses these inflammatory/oxidative mediators and pro-inflammatory cytokines to enhance insulin signalling and improve glucose metabolism.