Four members of the glial cell line-derived neurotrophic factor family have been identified (GDNF, neurturin, persephin, and enovin/artemin). They bind to a specific membrane-anchored GDNF family receptor as follows: GFRα-1 for GDNF, GFRα-2 for neurturin, GFRα-3 for enovin/artemin, and (chicken) GFRα-4 for persephin. Subsequent signaling occurs through activation of a common transmembrane tyrosine kinase, cRET. GFRα-4, the coreceptor for persephin, was previously identified in chicken only. We describe the cloning and characterization of a mammalian persephin receptor GFRα-4. The novel GFRα receptor is substantially different in sequence from all known GFRαs, including chicken GFRα-4, and lacks the first cysteine-rich domain present in all previously characterized GFRαs. At least two different GFRα-4 splice variants exist in rat tissues, differing at their respective COOH termini. GFRα-4 mRNA is expressed at low levels in different brain areas in the adult as well as in some peripheral tissues including testis and heart. Recombinant rat GFRα-4 variants were expressed in mammalian cells and shown to be at least partially secreted from the cells. Persephin binds specifically and with high affinity (KD = 6 nM) to the rat GFRα-4 receptor, but no cRET activation could be demonstrated. Although the newly characterized mammalian GFRα-4 receptor is structurally divergent from previously characterized GFRα family members, we suggest that it is a mammalian orthologue of the chicken persephin receptor. This discovery will allow a more detailed investigation of the biological targets of persephin action and its potential involvement in diseases of the nervous system.
CITATION STYLE
Masure, S., Cik, M., Hoefnagel, E., Nosrat, C. A., Van Der Linden, I., Scott, R., … Gordon, R. D. (2000). Mammalian GFRα-4, a divergent member of the GFRα family of coreceptors for glial cell line-derived neurotrophic factor family ligands, is a receptor for the neurotrophic factor persephin. Journal of Biological Chemistry, 275(50), 39427–39434. https://doi.org/10.1074/jbc.M003867200
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