EGFR Activation Mediates Inhibition of Axon Regeneration by Myelin and Chondroitin Sulfate Proteoglycans

Koprivica, Vuk; Cho, Kin‐Sang; Park, Jong Bae; Yiu, Glenn; Atwal, Jasvinder K.; Gore, Bryan B.; Kim, Jieun A.; Lin, Estelle; Tessier‐Lavigne, Marc; Chen, Dong Feng; He, Zhigang

doi:10.1126/science.1115462

Cited by 328 publications

(335 citation statements)

References 29 publications

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“…Both in vitro and in vivo results indicate that PKC is one of the signaling mediators of myelin inhibition. Another study also by He and colleagues concluded that EGFR mediates myelin inhibition (Koprivica et al, 2005). They showed that myelin inhibitors trigger EGFR phosphorylation and in vivo administration of EGFR inhibitors stimulate optic nerve regeneration.…”

Section: Intracellular Signalingmentioning

confidence: 93%

“…For instance, Rho/ROCK, PKC and EGFR appear to be common mediators of neurite inhibition by both the prototypical myelin inhibitors and the CSPGs (Lehmann et al, 1999;Monnier et al, 2003;Sivasankaran et al, 2004;Koprivica et al, 2005). These observations indicate that such common downstream effectors may offer certain advantages as therapeutic targets.…”

Section: Intracellular Signalingmentioning

confidence: 96%

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White matter inhibitors in CNS axon regeneration failure

Xie

Zheng

2008

Experimental Neurology

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Multiple lines of evidence have indicated that the inability of adult mammalian central nervous system (CNS) axons to regenerate after injury is partly due to the growth inhibitory property of central myelin. Three prototypical myelin-associated inhibitors of neurite outgrowth have been identified, including Nogo, myelin-associated glycoprotein (MAG), oligodendrocyte-myelin glycoprotein (OMgp). These inhibitory ligands, their receptors and signaling pathways are being intensively investigated for their roles in CNS axon regeneration failure. In addition, several members of the axon guidance molecules have been implicated in restricting CNS axon regeneration, some of which are expressed by mature oligodendrocytes. Here we review in vitro and in vivo studies of these molecules in neurite growth and in axon regeneration failure and discuss the implications of these studies. While the increasing number of potential axon regeneration inhibitors highlights the complexity of the restrictive CNS environment, it provides new windows of opportunity as well as new challenges for therapeutic development for spinal cord injury and related neurological conditions.

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Section: Intracellular Signalingmentioning

confidence: 93%

Section: Intracellular Signalingmentioning

confidence: 96%

White matter inhibitors in CNS axon regeneration failure

Xie

Zheng

2008

Experimental Neurology

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“…MAG inhibits neurite outgrowth from the postnatal CGNs, and this effect is mediated by several factors, including RhoA, conventional PKC, and the EGF receptor. 6,9 These findings prompted us to examine if the effect of MAG-Fc on neurite outgrowth is also dependent on Rap1 activity. We generated TAT-Rap1A DN and TAT-Rap1A DA -DN and DA forms of Rap1A fused with the N-terminal 11-amino-acid protein transduction domain of the human immunodeficiency virus protein TAT 19 -to enable the protein to gain entry into the cell.…”

Section: Mc192+mag-fcmentioning

confidence: 99%

“…7,8 In addition, phosphorylation of the epidermal growth factor (EGF) receptor is triggered by these myelin-derived inhibitors and is necessary for the inhibitory effect. 9 These multiple signals are responsible for the effects of the myelin-derived inhibitors at least in vitro.In addition to the role of MAG in axon regeneration, experiments with MAG-deficient mice implicate this protein in regulating axonal caliber and the levels of neurofilament spacing in mature myelinated fibers. 10 MAG is suggested to modulate the maturation and viability of myelinated axons.…”

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confidence: 99%

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Rap1 is involved in the signal transduction of myelin-associated glycoprotein

et al. 2007

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Myelin-associated glycoprotein (MAG) is a well-characterized axon growth inhibitor in the adult vertebrate nervous system. Several signals that play roles in inhibiting axon growth have been identified. Here, we report that soluble MAG induces activation of Rap1 in postnatal cerebellar granule neurons (CGNs) and dorsal root ganglion (DRG) neurons. The p75 receptor associates with activated Rap1 and is internalized in response to MAG. After MAG is applied to the distal axons of the sciatic nerves, the activated Rap1, internalized p75 receptor, and MAG are retrogradely trafficked via axons to the cell bodies of the DRG neurons. Rap1 activity is required for survival of the DRG neurons as well as CGNs when treated with MAG. Myelin-associated glycoprotein (MAG) is a member of the I-type lectin subgroup of the immunoglobulin (Ig) gene superfamily and is expressed exclusively by myelinating cells where it is enriched in the adaxonal membrane of the myelin internode. MAG inhibits neurite outgrowth from the adult dorsal root ganglion (DRG) and the postnatal ages of the cerebellar, retinal, spinal, hippocampal, and superior cervical ganglion neurons. 1,2 To date, two additional neurite growth inhibitors that are expressed by oligodendrocytes and myelinated fiber tracts have been identified. 3 These are Nogo and oligodendrocyte-myelin glycoprotein. All these proteins act on neurons through the Nogo receptor complex. This is a trimolecular complex comprising the Nogo receptor, Lingo-1, and p75/Troy. 4 A key intracellular effector for neurite growth inhibitory signaling by myelin was previously shown to be the small guanine nucleoside triphosphatase, RhoA. In its active GTP-bound form, RhoA rigidifies the actin cytoskeleton, thereby inhibiting axon elongation and mediating growth cone collapse. RhoA is activated by these proteins through a p75-dependent mechanism, thus inhibiting neurite outgrowth from the postnatal sensory neurons and cerebellar neurons. 5,6 It was also demonstrated that conventional protein kinase C (PKC), including PKC-a, -b, and -g, was activated by the neurite growth inhibitory proteins, and the inhibition of conventional PKC eliminated the effect of these proteins on neurite outgrowth. 7,8 In addition, phosphorylation of the epidermal growth factor (EGF) receptor is triggered by these myelin-derived inhibitors and is necessary for the inhibitory effect. 9 These multiple signals are responsible for the effects of the myelin-derived inhibitors at least in vitro.In addition to the role of MAG in axon regeneration, experiments with MAG-deficient mice implicate this protein in regulating axonal caliber and the levels of neurofilament spacing in mature myelinated fibers. 10 MAG is suggested to modulate the maturation and viability of myelinated axons. These findings suggest the diverse functions of MAG in the nervous system.In the course of identifying signals downstream of MAG, we found that Rap1 is activated in response to soluble MAG. Rap1 is a member of the Ras family of small guanine nucleotidebinding ...

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Myelin‐associated glycoprotein alters the neuronal secretome and stimulates the release of TGFβ and proteins that affect neural plasticity

et al. 2022

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Myelin‐associated glycoprotein (MAG) and Nogo inhibit neurite outgrowth by binding to receptors such as NgR1, PirB and LRP1, and they have also been shown to induce phosphorylation of Smad2, a key intermediate in the transforming growth factor β (TGFβ) signalling pathway. In this study, we determined that MAG and Nogo do not transactivate the TGFβ receptor through their canonical receptors or discoidin domain receptor 1, which we identified as a novel receptor for MAG and Nogo. Instead, MAG and Nogo promoted Smad2 phosphorylation by stimulating secretion of TGFβ. Proteomic analysis of the neuronal secretome revealed that MAG also regulated the secretion of proteins that affect central nervous system plasticity—inducing the secretion of S100A6, septin‐7 and neurofascin 186, while inhibiting the secretion of frataxin, MAP6, syntenin‐1 and GAP‐43. This represents a novel function for MAG that has broad implications for the treatment for spinal cord injury.

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EGFR Activation Mediates Inhibition of Axon Regeneration by Myelin and Chondroitin Sulfate Proteoglycans

Cited by 328 publications

References 29 publications

White matter inhibitors in CNS axon regeneration failure

White matter inhibitors in CNS axon regeneration failure

Rap1 is involved in the signal transduction of myelin-associated glycoprotein

Myelin‐associated glycoprotein alters the neuronal secretome and stimulates the release of TGFβ and proteins that affect neural plasticity

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