Phosphorylation of insulin receptor substrate-1 serine 307 correlates with JNK activity in atrophic skeletal muscle
Thomas L Hilder, Janet C L Tou, Richard E Grindeland, Charles E Wade, Lee M Graves, C E Wade, L M Graves, Thomas L Hilder, Janet C L Tou, Richard E Grindeland, Charles E Wade, Lee M Graves, C E Wade, L M Graves
Abstract
c-Jun NH(2)-terminal kinase (JNK) has been shown to negatively regulate insulin signaling through serine phosphorylation of residue 307 within the insulin receptor substrate-1 (IRS-1) in adipose and liver tissue. Using a rat hindlimb suspension model for muscle disuse atrophy, we found that JNK activity was significantly elevated in atrophic soleus muscle and that IRS-1 was phosphorylated on Ser(307) prior to the degradation of the IRS-1 protein. Moreover, we observed a corresponding reduction in Akt activity, providing biochemical evidence for the development of insulin resistance in atrophic skeletal muscle.
Source: PubMed