Interaction between serin phosphorylated IRS-1 and beta1-integrin affects the stability of neuronal processes
Articolo
Data di Pubblicazione:
2007
Citazione:
Interaction between serin phosphorylated IRS-1 and beta1-integrin affects the stability of neuronal processes / J.Y. Wang, E. Gualco, F. Peruzzi, B.E. Sawaya, G. Passiatore, C. Marcinkiewicz, I. Stamiszewska, P. Ferrante, S. Amini, K. Khalili, K. Reiss. - In: JOURNAL OF NEUROSCIENCE RESEARCH. - ISSN 0360-4012. - 85:11(2007 Aug 15), pp. 2360-2373.
Abstract:
Tumor necrosis factor-alpha (TNFalpha) released in the brain by HIV-activated macrophages/microglia is suspected to compromise neuronal survival. Previously, we have demonstrated that activated receptor for insulin-like growth factor I (IGF-IR) protects neurons from TNFalpha-induced neuronal damage (Wang et al. [ 2006] J. Neurosci. Res. 83:7-18). Because TNFalpha triggers phosphorylation of insulin receptor substrate 1 (IRS-1) on serine residues (pS-IRS-1; Rui et al. [ 2001] J. Clin. Invest. 107:181-189), and pS-IRS-1 binds integrins (Reiss et al. [ 2001] Oncogene 20:490-500), we asked how these events affect neuronal processes. We show that beta1-integrin and pS-IRS-1 colocalize in PC12 cells and in primary cortical neurons. TNFalpha treatment elevated membrane-associated pS-IRS-1, enhanced pS-IRS-1 interaction with beta1-integrin, and attenuated cell attachment to collagen IV. In contrast, IGF-I inhibited pS-IRS-1-beta1-integrin complexes and improved cell attachment. The domain of IRS-1 involved in beta1-integrin binding mapped between amino acids 426 and 740, and the expression of 426-740/IRS-1 mutant attenuated neuronal outgrowth. Our results indicate that TNFalpha facilitates the interaction of pS-IRS-1 and beta1-integrin and destabilizes neuronal processes. IGF-I counteracts TNFalpha-mediated accumulation of pS-IRS-1-beta1-integrin complexes supporting the stability of neuronal processes.
Tipologia IRIS:
01 - Articolo su periodico
Keywords:
IGF-I; Integrins; IRS-1; Neuronal damage; TNFα
Elenco autori:
J.Y. Wang, E. Gualco, F. Peruzzi, B.E. Sawaya, G. Passiatore, C. Marcinkiewicz, I. Stamiszewska, P. Ferrante, S. Amini, K. Khalili, K. Reiss
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