Key Points
-
Four different glial cell line-derived neurotrophic factor (GDNF)-family ligand (GFL)– receptor (GFRα) binding pairs exist, and they all signal through the transmembrane RET receptor tyrosine kinase.
-
Recruitment of RET to lipid rafts, induced by GFL binding to glycolipid-anchored GFRα receptors, is necessary for efficient downstream signalling. RET stimulation by soluble or matrix-bound GFL–GFRα complex activates distinct signalling pathways outside the rafts, and leads to sustained signalling inside the rafts.
-
Regulation of GFL and soluble GFRα receptor production, their interactions with the extracellular matrix, as well as internalization and degradation of the GFL–GFRα–RET receptor complex, are poorly understood.
-
GDNF acts in synergy with other growth factors, including transforming growth factor-β, but the mechanisms are unclear. Nerve growth factor (NGF) can activate RET by its tyrosine kinase receptor TrkA through an unknown intracellular pathway, independently of GFLs and GFRα receptors. GDNF can activate Src-family kinases through GFRα1 and an unknown transmembrane linker protein in a RET-independent manner.
-
GFLs might regulate the expression of their cognate co-receptors. Regulation of neurotransmitter release by GDNF implies a role in synaptic plasticity.
-
Sympathetic precursors require artemin, which is produced locally or by intermediate target cells, primarily for migration, but also for proliferation and early differentiation. Similarly, parasympathetic and enteric precursors require GDNF.
-
During target innervation, sympathetic neurons become dependent on NGF rather than artemin for their survival. By contrast, parasympathetic neurons switch their requirements from GDNF to target-derived neurturin for terminal innervation and the maintenance of cell size.
-
In somatic sensory neurons, GFLs regulate soma size, target innervation and nociception, but are not required for survival in vivo.
-
A subpopulation of motor neurons requires GDNF, which is produced by Schwann cells, to avoid programmed cell death. GDNF- but not brain-derived neurotrophic factor-mediated protection of injured motor neurons requires inhibitor of apoptosis proteins. So, trophic signalling differs between neurotrophins and GFLs.
-
Apart from promoting neuronal maintenance and regeneration, GFL-like drugs might be useful in the treatment of disorders such as neuropathic pain and addiction.
Abstract
Members of the nerve growth factor (NGF) and glial cell line-derived neurotrophic factor (GDNF) families — comprising neurotrophins and GDNF-family ligands (GFLs), respectively — are crucial for the development and maintenance of distinct sets of central and peripheral neurons. Knockout studies in the mouse have revealed that members of these two families might collaborate or act sequentially in a given neuron. Although neurotrophins and GFLs activate common intracellular signalling pathways through their receptor tyrosine kinases, several clear differences exist between these families of trophic factors.
This is a preview of subscription content, access via your institution
Access options
Subscribe to this journal
Receive 12 print issues and online access
$189.00 per year
only $15.75 per issue
Buy this article
- Purchase on Springer Link
- Instant access to full article PDF
Prices may be subject to local taxes which are calculated during checkout
Similar content being viewed by others
References
Airaksinen, M. S., Titievsky, A. & Saarma, M. GDNF family neurotrophic factor signaling: four masters, one servant? Mol. Cell. Neurosci. 13, 313–325 (1999).
Baloh, R. H., Enomoto, H., Johnson, E. M. J. & Milbrandt, J. The GDNF family ligands and receptors — implications for neural development. Curr. Opin. Neurobiol. 10, 103–110 (2000).
Ibáñez, C. F. Emerging themes in structural biology of neurotrophic factors. Trends Neurosci. 21, 438–444 (1998).
Hamilton, J. F. et al. Heparin coinfusion during convection-enhanced delivery (CED) increases the distribution of the glial-derived neurotrophic factor (GDNF) ligand family in rat striatum and enhances the pharmacological activity of neurturin. Exp. Neurol. 168, 155–161 (2001).
Golden, J. P., DeMaro, J. A., Osborne, P. A., Milbrandt, J. & Johnson, E. M. Jr. Expression of neurturin, GDNF, and GDNF family-receptor mRNA in the developing and mature mouse. Exp. Neurol. 158, 504–528 (1999).
Lee, R., Kermani, P., Teng, K. K. & Hempstead, B. L. Regulation of cell survival by secreted proneurotrophins. Science 294, 1945–1948 (2001).
Takahashi, M. The GDNF/RET signaling pathway and human diseases. Cytokine Growth Factor Rev. 12, 361–373 (2001).
Lindahl, M. et al. Human glial cell line-derived neurotrophic factor receptor α4 is the receptor for persephin and is predominantly expressed in normal and malignant thyroid medullary cells. J. Biol. Chem. 276, 9344–9351 (2001).
Paratcha, G. et al. Released GFRα1 potentiates downstream signaling, neuronal survival, and differentiation via a novel mechanism of recruitment of c-Ret to lipid rafts. Neuron 29, 171–184 (2001).Together with reference 15 , this paper shows that released GFRα1–GDNF potentiates RET signalling. Moreover, it shows that RET stimulation by immobilized GFRα1–GDNF enhances axonal growth cone formation, and that soluble GFRα1 can recruit RET to lipid rafts by a novel mechanism that requires the RET tyrosine kinase.
Eketjäll, S., Fainzilber, M., Murray-Rust, J. & Ibáñez, C. F. Distinct structural elements in GDNF mediate binding to GFRα1 and activation of the GFRα1–c-Ret receptor complex. EMBO J. 18, 5901–5910 (1999).
Simons, K. & Toomre, D. Lipid rafts and signal transduction. Nature Rev. Mol. Cell Biol. 1, 31–39 (2000).
Poteryaev, D. et al. GDNF triggers a novel Ret-independent Src kinase family-coupled signaling via a GPI-linked GDNF receptor α1. FEBS Lett. 463, 63–66 (1999).Together with reference 27 , this paper provides the first demonstration that GDNF signals in a RET-independent manner through GFRα1 in lipid rafts.
Tansey, M. G., Baloh, R. H., Milbrandt, J. & Johnson, E. M. Jr. GFRα-mediated localization of RET to lipid rafts is required for effective downstream signaling, differentiation, and neuronal survival. Neuron 25, 611–623 (2000).The first demonstration that the recruitment of RET to lipid rafts by GFL binding to GFRα is required for effective signalling.
Coulpier, M., Anders, J. & Ibáñez, C. F. Coordinated activation of autophosphorylation sites in the RET receptor tyrosine kinase. Importance of tyrosine 1062 for GDNF mediated neuronal differentiation and survival. J. Biol. Chem. 277, 1991–1999 (2002).
Worley, D. S. et al. Developmental regulation of GDNF response and receptor expression in the enteric nervous system. Development 127, 4383–4393 (2000).The first demonstration of endogenous soluble GFRα1, which is released by cultured gut cells in a developmentally regulated manner.
Manie, S., Santoro, M., Fusco, A. & Billaud, M. The RET receptor: function in development and dysfunction in congenital malformation. Trends Genet. 17, 580–589 (2001).
Schlessinger, J. Cell signaling by receptor tyrosine kinases. Cell 103, 211–225 (2000).
Kaplan, D. R. & Miller, F. D. Neurotrophin signal transduction in the nervous system. Curr. Opin. Neurobiol. 10, 381–391 (2000).
Yang, F. et al. PI-3 kinase and IP3 are both necessary and sufficient to mediate NT3-induced synaptic potentiation. Nature Neurosci. 4, 19–28 (2001).
de Graaff, E. et al. Differential activities of the RET tyrosine kinase receptor isoforms during mammalian embryogenesis. Genes Dev. 15, 2433–2444 (2001).Using a knock-in approach, this study shows that the short RET isoform mediates most of the biological activities of RET in vivo.
Tsui-Pierchala, B. A., Milbrandt, J. & Johnson, E. M. NGF utilizes c-Ret via a novel GFL-independent, inter-RTK signaling mechanism to maintain the trophic status of mature sympathetic neurons. Neuron 33, 261–273 (2002).Identifies a new pathway for RET activation by NGF through TrkA.
Bordeaux, M. C. et al. The RET proto-oncogene induces apoptosis: a novel mechanism for Hirschsprung disease. EMBO J. 19, 4056–4063 (2000).
Peterziel, H., Unsicker, K. & Krieglstein, K. Molecular mechanisms underlying the cooperative effect of glial cell line-derived neurotrophic factor and transforming growth factor-β on neurons. Soc. Neurosci. Abstr. 27, 364.35 (2001).
Erickson, J. T., Brosenitsch, T. A. & Katz, D. M. Brain-derived neurotrophic factor and glial cell line-derived neurotrophic factor are required simultaneously for survival of dopaminergic primary sensory neurons in vivo. J. Neurosci. 21, 581–589 (2001).
Poo, M. M. Neurotrophins as synaptic modulators. Nature Rev. Neurosci. 2, 24–32 (2001).
Fukuda, T., Kiuchi, K. & Takahashi, M. Novel mechanism of regulation of Rac activity and lamellipodia formation by RET tyrosine kinase. J. Biol. Chem. 8 March 2002 (10.1074/jbc.M200643200).
Trupp, M., Scott, R., Whittemore, S. R. & Ibáñez, C. F. Ret-dependent and -independent mechanisms of glial cell line-derived neurotrophic factor signaling in neuronal cells. J. Biol. Chem. 274, 20885–20894 (1999).
Pezeshki, G., Franke, B. & Engele, J. Evidence for a ligand-specific signaling through GFRα-1, but not GFRα-2, in the absence of Ret. J. Neurosci. Res. 66, 390–395 (2001).
Nishino, J. et al. GFRα3, a component of the artemin receptor, is required for migration and survival of the superior cervical ganglion. Neuron 23, 725–736 (1999).The first demonstration that ARTN–GFRα3 signalling controls the migration of sympathetic precursors in vivo.
Lindahl, M., Timmusk, T., Rossi, J., Saarma, M. & Airaksinen, M. S. Expression and alternative splicing of mouse Gfra4 suggest roles in endocrine cell development. Mol. Cell. Neurosci. 15, 522–533 (2000).
Hiltunen, P. et al. Initial characterization of GDNF-family receptor GFRα4-deficient mice. Soc. Neurosci. Abstr. 27, 364.31 (2001).
Taraviras, S. et al. Signalling by the RET receptor tyrosine kinase and its role in the development of the mammalian enteric nervous system. Development 126, 2785–2797 (1999).
Homma, Y. et al. Artemin is required for the sympathetic nervous system development. Soc. Neurosci. Abstr. 27, 798.4 (2001).
Enomoto, H. et al. RET signaling is essential for migration, axonal growth and axon guidance of developing sympathetic neurons. Development 128, 3963–3974 (2001).
Andres, R. et al. Multiple effects of artemin on sympathetic neurone generation, survival and growth. Development 128, 3685–3695 (2001).
Brodski, C., Schnurch, H. & Dechant, G. Neurotrophin-3 promotes the cholinergic differentiation of sympathetic neurons. Proc. Natl Acad. Sci. USA 97, 9683–9688 (2000).
Thang, S. H., Kobayashi, M. & Matsuoka, I. Regulation of glial cell line-derived neurotrophic factor responsiveness in developing rat sympathetic neurons by retinoic acid and bone morphogenetic protein-2. J. Neurosci. 20, 2917–2925 (2000).
Enomoto, H., Heuckeroth, R. O., Golden, J. P., Johnson, E. M. & Milbrandt, J. Development of cranial parasympathetic ganglia requires sequential actions of GDNF and neurturin. Development 127, 4877–4889 (2000).Together with reference 39 , this paper indicates an early role for GDNF in parasympathetic precursor development.
Rossi, J., Tomac, A., Saarma, M. & Airaksinen, M. S. Distinct roles for GFRα1 and GFRα2 signalling in different cranial parasympathetic ganglia in vivo. Eur. J. Neurosci. 12, 3944–3952 (2000).
Heathcote, R. D. & Sargent, P. B. Growth and morphogenesis of an autonomic ganglion. II. Establishment of neuron position. J. Neurosci. 7, 2502–2509 (1987).
Hashino, E. et al. GDNF and neurturin are target-derived factors essential for cranial parasympathetic neuron development. Development 128, 3773–3782 (2001).
Shen, L. et al. Gdnf haploinsufficiency causes Hirschsprung-like intestinal obstruction and early-onset lethality in mice. Am. J. Hum. Genet. 70, 435–447 (2002).
Gershon, M. D. Lessons from genetically engineered animal models. II. Disorders of enteric neuronal development: insights from transgenic mice. Am. J. Physiol. 277, G262–G267 (1999).
Auricchio, A. et al. Double heterozygosity for a RET substitution interfering with splicing and an EDNRB missense mutation in Hirschsprung disease. Am. J. Hum. Genet. 64, 1216–1221 (1999).
Snider, W. D. & McMahon, S. B. Tackling pain at the source: new ideas about nociceptors. Neuron 20, 629–632 (1998).
Bennett, D. L. et al. The glial cell line-derived neurotrophic factor family receptor components are differentially regulated within sensory neurons after nerve injury. J. Neurosci. 20, 427–437 (2000).
Fundin, B. T., Mikaels, A., Westphal, H. & Ernfors, P. A rapid and dynamic regulation of GDNF-family ligands and receptors correlate with the developmental dependency of cutaneous sensory innervation. Development 126, 2597–2610 (1999).
Jongen, J. L., Dalm, E., Vecht, C. J. & Holstege, J. C. Depletion of GDNF from primary afferents in adult rat dorsal horn following peripheral axotomy. Neuroreport 10, 867–871 (1999).
Baudet, C. et al. Positive and negative interactions of GDNF, NTN and ART in developing sensory neuron subpopulations, and their collaboration with neurotrophins. Development 127, 4335–4344 (2000).
Oppenheim, R. W. et al. Glial cell line-derived neurotrophic factor and developing mammalian motoneurons: regulation of programmed cell death among motoneuron subtypes. J. Neurosci. 20, 5001–5011 (2000).
Stucky, C. L., Rossi, J., Airaksinen, M. S. & Lewin, G. R. The heat sensitivity of isolectin-B4 positive nociceptors is selectively lost in mice lacking the neurturin receptor GFRα2. Soc. Neurosci. Abstr. 94, 8 (1999).
Arce, V. et al. Synergistic effects of Schwann- and muscle-derived factors on motoneuron survival involve GDNF and cardiotrophin-1 (CT-1). J. Neurosci. 18, 1440–1448 (1998).
Garces, A. et al. GFRα1 is required for development of distinct subpopulations of motoneuron. J. Neurosci. 20, 4992–5000 (2000).
Keller-Peck, C. R. et al. Glial cell line-derived neurotrophic factor administration in postnatal life results in motor unit enlargement and continuous synaptic remodeling at the neuromuscular junction. J. Neurosci. 21, 6136–6146 (2001).
Zwick, M., Teng, L., Mu, X., Springer, J. E. & Davis, B. M. Overexpression of GDNF induces and maintains hyperinnervation of muscle fibers and multiple end-plate formation. Exp. Neurol. 171, 342–350 (2001).
Åkerud, P., Alberch, J., Eketjäll, S., Wagner, J. & Arenas, E. Differential effects of glial cell line-derived neurotrophic factor and neurturin on developing and adult substantia nigra dopaminergic neurons. J. Neurochem. 73, 70–78 (1999).
Granholm, A. C. et al. Glial cell line-derived neurotrophic factor is essential for postnatal survival of midbrain dopamine neurons. J. Neurosci. 20, 3182–3190 (2000).
Batchelor, P. E., Liberatore, G. T., Porritt, M. J., Donnan, G. A. & Howells, D. W. Inhibition of brain-derived neurotrophic factor and glial cell line-derived neurotrophic factor expression reduces dopaminergic sprouting in the injured striatum. Eur. J. Neurosci. 12, 3462–3468 (2000).
Meng, X. et al. Regulation of cell fate decision of undifferentiated spermatogonia by GDNF. Science 287, 1489–1493 (2000).The first demonstration that GDNF regulates spermatogonia differentiation in vivo.
Hottinger, A. F., Azzouz, M., Deglon, N., Aebischer, P. & Zurn, A. D. Complete and long-term rescue of lesioned adult motoneurons by lentiviral-mediated expression of glial cell line-derived neurotrophic factor in the facial nucleus. J. Neurosci. 20, 5587–5593 (2000).
Perrelet, D. et al. IAPs are essential for GDNF-mediated neuroprotective effects in injured motor neurons in vivo. Nature Cell Biol. 4, 175–179 (2002).The first demonstration of a difference in trophic signalling between GFLs and neurotrophins.
Zhou, X. F., Deng, Y. S., Xian, C. J. & Zhong, J. H. Neurotrophins from dorsal root ganglia trigger allodynia after spinal nerve injury in rats. Eur. J. Neurosci. 12, 100–105 (2000).
Li, L. & Zhou, X. F. Pericellular Griffonia simplicifolia I isolectin B4-binding ring structures in the dorsal root ganglia following peripheral nerve injury in rats. J. Comp. Neurol. 439, 259–274 (2001).
Boucher, T. J. et al. Potent analgesic effects of GDNF in neuropathic pain states. Science 290, 124–127 (2000).Shows that GDNF supresses neuropathic pain, possibly by preventing the upregulation of Na+ channel subunits.
Ramer, M. S., Priestley, J. V. & McMahon, S. B. Functional regeneration of sensory axons into the adult spinal cord. Nature 403, 312–316 (2000).The first demonstration that axons can regenerate through the dorsal root entry zone into the spinal cord and form functional synapses if provided with the right growth factors.
Akkina, S. K., Patterson, C. L. & Wright, D. E. GDNF rescues nonpeptidergic unmyelinated primary afferents in streptozotocin-treated diabetic mice. Exp. Neurol. 167, 173–182 (2001).
Wang, Y., Lin, S. Z., Chiou, A. L., Williams, L. R. & Hoffer, B. J. Glial cell line-derived neurotrophic factor protects against ischemia-induced injury in the cerebral cortex. J. Neurosci. 17, 4341–4348 (1997).
Kitagawa, H. et al. Reduction of ischemic brain injury by topical application of glial cell line-derived neurotrophic factor after permanent middle cerebral artery occlusion in rats. Stroke 29, 1417–1422 (1998).
Arvidsson, A., Kokaia, Z., Airaksinen, M. S., Saarma, M. & Lindvall, O. Stroke induces widespread changes of gene expression for glial cell line-derived neurotrophic factor family receptors in the adult rat brain. Neuroscience 106, 27–41 (2001).
Nicole, O. et al. Neuroprotection mediated by glial cell line-derived neurotrophic factor: involvement of a reduction of NMDA-induced calcium influx by the mitogen-activated protein kinase pathway. J. Neurosci. 21, 3024–3033 (2001).
Nanobashvili, A. et al. Development and persistence of kindling epilepsy are impaired in mice lacking glial cell line-derived neurotrophic factor family receptor α2. Proc. Natl Acad. Sci. USA 97, 12312–12317 (2000).
Grondin, R. & Gash, D. M. Glial cell line-derived neurotrophic factor (Gdnf) — a drug candidate for the treatment of Parkinson's disease. J. Neurol. 245, P35–42 (1998).
Kordower, J. H. et al. Clinicopathological findings following intraventricular glial-derived neurotrophic factor treatment in a patient with Parkinson's disease. Ann. Neurol. 46, 419–424 (1999).
Kordower, J. H. et al. Neurodegeneration prevented by lentiviral vector delivery of GDNF in primate models of Parkinson's disease. Science 290, 767–773 (2000).
Åkerud, P., Canals, J. M., Snyder, E. Y. & Arenas, E. Neuroprotection through delivery of glial cell line-derived neurotrophic factor by neural stem cells in a mouse model of Parkinson's disease. J. Neurosci. 21, 8108–8118 (2001).
Björklund, A. et al. Towards a neuroprotective gene therapy for Parkinson's disease: use of adenovirus, AAV and lentivirus vectors for gene transfer of GDNF to the nigrostriatal system in the rat Parkinson model. Brain Res. 886, 82–98 (2000).
Zurn, A. D., Widmer, H. R. & Aebischer, P. Sustained delivery of GDNF: towards a treatment for Parkinson's disease. Brain Res. Brain Res. Rev. 36, 222–229 (2001).
Nestler, E. J. Molecular basis of long-term plasticity underlying addiction. Nature Rev. Neurosci. 2, 119–128 (2001).
Messer, C. J. et al. Role for GDNF in biochemical and behavioral adaptations to drugs of abuse. Neuron 26, 247–257 (2000).Indicates a role for endogenous GDNF in dopamine plasticity in vivo after cocaine or morphine exposure.
Pattyn, A., Morin, X., Cremer, H., Goridis, C. & Brunet, J. F. The homeobox gene Phox2b is essential for the development of autonomic neural crest derivatives. Nature 399, 366–370 (1999).
Lang, D. et al. Pax3 is required for enteric ganglia formation and functions with Sox10 to modulate expression of c-ret. J. Clin. Invest. 106, 963–971 (2000).
Gerlai, R. et al. Impaired water maze learning performance without altered dopaminergic function in mice heterozygous for the GDNF mutation. Eur. J. Neurosci. 14, 1153–1163 (2001).
Wang, C. Y. et al. Ca2+ binding protein frequenin mediates GDNF-induced potentiation of Ca2+ channels and transmitter release. Neuron 32, 99–112 (2001).
Yang, F. et al. GDNF acutely modulates excitability and A-type K+ channels in midbrain dopaminergic neurons. Nature Neurosci. 4, 1071–1078 (2001).
Scott, R. P. & Ibáñez, C. F. Determinants of ligand binding specificity in the glial cell line-derived neurotrophic factor family receptor αs. J. Biol. Chem. 276, 1450–1458 (2001).
Baloh, R. H., Tansey, M. G., Johnson, E. M. J. & Milbrandt, J. Functional mapping of receptor specificity domains of glial cell line-derived neurotrophic factor (GDNF) family ligands and production of GFRα1 RET-specific agonists. J. Biol. Chem. 275, 3412–3420 (2000).
Anders, J., Kjar, S. & Ibáñez, C. F. Molecular modeling of the extracellular domain of the RET receptor tyrosine kinase reveals multiple cadherin-like domains and a calcium-binding site. J. Biol. Chem. 276, 35808–35817 (2001).
Acknowledgements
We thank U. Arumäe, M. Paveliev, J. Rossi and P. Runeberg-Roos for critical reading of the manuscript. Our work is supported by the Academy of Finland, TEKES, Biocentrum Helsinki and the Sigrid Jusélius Foundation. Owing to space limitations, we have cited original references only from the last four years; we apologize for the omission of earlier papers.
Author information
Authors and Affiliations
Related links
Related links
DATABASES
LocusLink
OMIM
congenital central hypoventilation syndrome
FURTHER INFORMATION
Encyclopedia of Life Sciences
Glossary
- CYSTINE KNOT
-
A structural motif that consists of six cysteine residues that are linked together by three disulphide bonds. It is involved in protein stabilization and dimer formation.
- HEPARAN SULPHATE
-
A glycosaminoglycan that consists of repeated units of hexuronic acid and glucosamine residues. It usually attaches to proteins through a xylose residue to form proteoglycans.
- RECEPTOR TYROSINE KINASE
-
Any of a family of transmembrane receptors, the intracellular domains of which catalyse the phosphorylation, by ATP, of specific tyrosine residues on their target proteins.
- GLYCOSYL PHOSPHATIDYLINOSITOL
-
A post-translational modification, the function of which is to attach proteins to the exoplasmic leaflet of membranes, possibly to specific domains therein. The anchor is made of one molecule of phosphatidylinositol to which a carbohydrate chain is linked through the C-6 hydroxyl of the inositol, and is attached to the protein through an ethanolamine phosphate moiety.
- PETROSAL GANGLION
-
A structure that contains the cell bodies of the sensory neurons of the glossopharyngeal nerve, which innervate the tongue, pharynx, middle ear and carotid body.
- LAMELLIPODIA
-
Sheet-like extensions at the edge of cells that contain a crosslinked F-actin meshwork.
- C-FOS
-
An immediate early gene that is rapidly turned on when many types of neuron increase their activity. It can therefore be used to identify responsive neurons.
- ENDOTHELIN
-
A molecule with potent vasoconstrictor activity. It is expressed by vascular cells, as well as in brain, kidney and lung.
- CAROTID BODY
-
A chemoreceptor organ that is located above the bifurcation of the common carotid artery. It monitors changes in blood O2 and CO2 content, and pH, thus helping to control respiratory activity.
- SKIN–NERVE PREPARATION
-
An in vitro preparation that is used to study the functional properties of sensory neurons that innervate the skin. Single sensory afferents are isolated by recording from axons in microdissected filaments of a cutaneous nerve, and are classified on the basis of their conduction velocity, mechanical threshold and adaptation properties.
- INTRATHECAL
-
Administered into the outer sheath of the spinal cord.
- KINDLING
-
An experimental model of epilepsy in which an increased susceptibility to seizures arises after daily focal stimulation of specific brain areas (for example, the amygdala) — stimulation that does not reach the threshold to elicit a seizure by itself.
Rights and permissions
About this article
Cite this article
Airaksinen, M., Saarma, M. The GDNF family: Signalling, biological functions and therapeutic value. Nat Rev Neurosci 3, 383–394 (2002). https://doi.org/10.1038/nrn812
Issue Date:
DOI: https://doi.org/10.1038/nrn812
This article is cited by
-
Unraveling the role of glial cell line–derived neurotrophic factor in the treatment of Parkinson’s disease
Neurological Sciences (2024)
-
Effects of gestational inflammation on age-related cognitive decline and hippocampal Gdnf-GFRα1 levels in F1 and F2 generations of CD-1 Mice
BMC Neuroscience (2023)
-
Optogenetic dissection of RET signaling reveals robust activation of ERK and enhanced filopodia-like protrusions of regenerating axons
Molecular Brain (2023)
-
GDNF gene therapy for alcohol use disorder in male non-human primates
Nature Medicine (2023)
-
A class of secreted mammalian peptides with potential to expand cell-cell communication
Nature Communications (2023)
