The Journal of Cell Biology, Vol 112, 991-1005, Copyright © 1991 by The Rockefeller University Press

ARTICLES

Monoclonal antibodies show that kinase C phosphorylation of GAP-43 during axonogenesis is both spatially and temporally restricted in vivo

KF Meiri, LE Bickerstaff and JE Schwob
Department of Pharmacology, State University of New York Health Science Center, Syracuse 13210.

To study the role of kinase C phosphorylation in the distribution and function of GAP-43 we have generated a panel of mAbs that distinguish between GAP-43 that has been phosphorylated by kinase C and forms that have not. One class of antibodies, typified by 2G12/C7, reacts with only the phosphorylated form of GAP-43; it recognizes the peptide IQAS(PO4)FR equivalent to residues 38-43 that includes the single kinase C phosphorylation site at serine. Another, exemplified by 10E8/E7, reacts with both phosphorylated and nonphosphorylated forms. We have used the antibodies to study the distribution of kinase C- phosphorylated GAP-43 during axonogenesis and in the adult nervous system. Two major findings emerge. First, there is a lag between the initiation of axon outgrowth and the phosphorylation of GAP-43 by kinase C. The extent of this lag period varies between the different structures studied. In some cases, e.g., the trigeminal nerve, our result suggest that kinase C phosphorylation may be correlated with proximity of the growing axon to its target. Second, kinase C- phosphorylated GAP-43 is always spatially restricted to the distal axon. It is never seen either proximally or in cell bodies, even those with high levels of GAP-43 protein. This result also implies that GAP- 43 is axonally transported in the non-kinase C phosphorylated form. Thus, kinase C phosphorylation of GAP-43 is not required for axon outgrowth or growth cone function per se and may be more related to interactions of the growth cone with its environment.
CiteULike    Complore    Connotea    Del.icio.us    Digg    Reddit    Technorati    What's this?

This article has been cited by other articles:

• Valerio, A., Ghisi, V., Dossena, M., Tonello, C., Giordano, A., Frontini, A., Ferrario, M., Pizzi, M., Spano, P., Carruba, M. O., Nisoli, E. (2006). Leptin Increases Axonal Growth Cone Size in Developing Mouse Cortical Neurons by Convergent Signals Inactivating Glycogen Synthase Kinase-3beta. J. Biol. Chem. 281: 12950-12958 [Abstract] [Full Text]  
• Pagliardini, S., Ren, J., Wevrick, R., Greer, J. J. (2005). Developmental Abnormalities of Neuronal Structure and Function in Prenatal Mice Lacking the Prader-Willi Syndrome Gene Necdin. Am. J. Pathol. 167: 175-191 [Abstract] [Full Text]  
• Ansuini, H., Cicchini, C., Nicosia, A., Tripodi, M., Cortese, R., Luzzago, A. (2002). Biotin-tagged cDNA expression libraries displayed on lambda phage: a new tool for the selection of natural protein ligands. Nucleic Acids Res 30: e78-e78 [Abstract] [Full Text]  
• Christensen, M. D., Holbrook, E. H., Costanzo, R. M., Schwob, J. E. (2001). Rhinotopy is Disrupted During the Re-innervation of the Olfactory Bulb that Follows Transection of the Olfactory Nerve. Chem Senses 26: 359-369 [Abstract] [Full Text]  
• Routtenberg, A., Cantallops, I., Zaffuto, S., Serrano, P., Namgung, U. (2000). Enhanced learning after genetic overexpression of a brain growth protein. Proc. Natl. Acad. Sci. USA 97: 7657-7662 [Abstract] [Full Text]  
• Prevot, V., Bouret, S., Croix, D., Alonso, G., Jennes, L., Mitchell, V., Routtenberg, A., Beauvillain, J.-C. (2000). Growth-Associated Protein-43 Messenger Ribonucleic Acid Expression in Gonadotropin-Releasing Hormone Neurons during the Rat Estrous Cycle. Endocrinology 141: 1648-1657 [Abstract] [Full Text]  
• Reed, J. A., Finnerty, B., Albino, A. P. (1999). Divergent Cellular Differentiation Pathways during the Invasive Stage of Cutaneous Malignant Melanoma Progression. Am. J. Pathol. 155: 549-555 [Abstract] [Full Text]  
• Meiri, K. F., Saffell, J. L., Walsh, F. S., Doherty, P. (1998). Neurite Outgrowth Stimulated by Neural Cell Adhesion Molecules Requires Growth-Associated Protein-43 (GAP-43) Function and Is Associated with GAP-43 Phosphorylation in Growth Cones. J. Neurosci. 18: 10429-10437 [Abstract] [Full Text]  
• Pasterkamp, R. J., De Winter, F., Holtmaat, A. J. G. D., Verhaagen, J. (1998). Evidence for a Role of the Chemorepellent Semaphorin III and Its Receptor Neuropilin-1 in the Regeneration of Primary Olfactory Axons. J. Neurosci. 18: 9962-9976 [Abstract] [Full Text]  
• Iwata, S.-I., Hewlett, G. H. K., Ferrell, S. T., Kantor, L., Gnegy, M. E. (1997). Enhanced Dopamine Release and Phosphorylation of Synapsin I and Neuromodulin in Striatal Synaptosomes after Repeated Amphetamine. J. Pharmacol. Exp. Ther. 283: 1445-1452 [Abstract] [Full Text]  
• Wang, M.-S., Zeleny-Pooley, M., Gold, B. G. (1997). Comparative Dose-Dependence Study of FK506 and Cyclosporin A on the Rate of Axonal Regeneration in the Rat Sciatic Nerve. J. Pharmacol. Exp. Ther. 282: 1084-1093 [Abstract] [Full Text]  
• He, Q., Dent, E. W., Meiri, K. F. (1997). Modulation of Actin Filament Behavior by GAP-43 (Neuromodulin) Is Dependent on the Phosphorylation Status of Serine 41, the Protein Kinase C Site. J. Neurosci. 17: 3515-3524 [Abstract] [Full Text]  
• Goldstein, B. J., Schwob, J. E. (1996). Analysis of the Globose Basal Cell Compartment in Rat Olfactory Epithelium Using GBC-1, a New Monoclonal Antibody against Globose Basal Cells. J. Neurosci. 16: 4005-4016 [Abstract] [Full Text]  
• Gerendasy, D. D., Herron, S. R., Jennings, P. A., Sutcliffe, J. G. (1995). Calmodulin Stabilizes an Amphiphilic alpha-Helix within RC3/Neurogranin and GAP-43/Neuromodulin Only When Ca[IMAGE] Is Absent. J. Biol. Chem. 270: 6741-6750 [Abstract] [Full Text]  
• Neel, V., Young, M. (1994). Igloo, a GAP-43-related gene expressed in the developing nervous system of Drosophila. Development 120: 2235-2243 [Abstract]  

Home | Help | Feedback | Subscriptions | Archive | Search | Table of Contents