Axonal elongation and guidance are controlled by extracellular factors such as the neurotrophins. Indeed, nerve growth factor (NGF) seems to promote axon growth through binding to its p75(NTR) receptor and inactivating RhoA. Furthermore, the local inhibition of glycogen synthase kinase (GSK)-3 beta by NGF also favors microtubule polymerization and axon extension. Inactivation of GSK-3 beta may be due to the NGF/TrkA-mediated activation of phosphatidylinositol-3 kinase (PI-3 kinase), which increases the levels of phosphatydilinositol 3-phosphate [PIMP]. However, we show here that NGF may inactivate GSK-3 beta through an alternative mechanism. In cultured hippocampal neurons, the capacity of NGF to promote axon elongation is mostly mediated by p75(NTR), and the activation of this pathway leads to the inactivation of GSK-3 beta. However, the signaling pathway triggered by NGF/p75(NTR) acts through casein kinase II (CK2). NGF/p75(NTR_) activated CK2 phosphorylates the phosphatase and tensin homologue deleted on chromosome 10 (PTEN), thus rendering this phosphatase inactive. Like activation of the PI-3 kinase, PTEN inactivation allows PIMP levels to increase, thus favoring GSK-3 beta inactivation and axon outgrowth. This newly disclosed mechanism may help to extend the repertoire of pharmacological agents that activate CK2 or that inhibit PTEN to stimulate axon regeneration after trauma or disease.

• 出版日期2006-8