%0 Generic %A J.-Y., Chung %A S.-J., Lee %A S.-H., Lee %A Y.S., Jung %A N.-C., Ha %A W., Seol %A B.-J., Park %D 2011 %T Supplementary Material for: Direct Interaction of α-Synuclein and AKT Regulates IGF-1 Signaling: Implication of Parkinson Disease %U https://karger.figshare.com/articles/dataset/Supplementary_Material_for_Direct_Interaction_of_-Synuclein_and_AKT_Regulates_IGF-1_Signaling_Implication_of_Parkinson_Disease/5121766 %R 10.6084/m9.figshare.5121766.v1 %2 https://karger.figshare.com/ndownloader/files/8706463 %K α-Synuclein %K AKT %K Parkinsonߣs disease %K IGF-1 signaling %X Genetic mutation of α-synuclein (α-SYN) is clearly verified as the causal factor of human and mouse Parkinson’s disease. However, biological function of α-SYN has not been clearly demonstrated until now. In this investigation, we reveal that α-SYN is a co-regulator of growth factor-induced AKT activation. Elimination of SYN reduces the IGF-1-mediated AKT activation. Similarly, mutant SYN suppresses the IGF-1-induced AKT activation. Wild-type SYN can interact with AKT and enhance the solubility and plasma localization of AKT in response to IGF-1, whereas mutant α-SYNs do not interact with AKT. In addition, elevated expression of SYN blocks the AKT activation. We also find that si-RNA against α-SYN abolished the protective effect of IGF-1 against DNA damage-induced apoptosis. Our result strongly indicates that Parkinson’s disease, induced by α-SYN mutation, is evoked by deregulation of the AKT-signaling cascade. %I Karger Publishers