ADRA2C — Alpha-2C Adrenergic Receptor
Introduction The ADRA2C gene encodes the alpha-2C adrenergic receptor (α2C-AR), a G protein-coupled receptor that mediates sympathetic tone inhibition. The α2C subtype is widely expressed in the central nervous system and peripheral tissues, playing crucial roles in regulating norepinephrine signaling, autonomic function, and stress responses. The receptor is unique among α2-AR subtypes for its distinctive subcellular distribution and functional properties[@szot2006].
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Protein Structure
Transmembrane Domain Architecture ADRA2C encodes a 462-amino acid GPCR with canonical seven transmembrane domain structure:
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ADRA2C — Alpha-2C Adrenergic Receptor
Introduction The ADRA2C gene encodes the alpha-2C adrenergic receptor (α2C-AR), a G protein-coupled receptor that mediates sympathetic tone inhibition. The α2C subtype is widely expressed in the central nervous system and peripheral tissues, playing crucial roles in regulating norepinephrine signaling, autonomic function, and stress responses. The receptor is unique among α2-AR subtypes for its distinctive subcellular distribution and functional properties[@szot2006].
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Protein Structure
Transmembrane Domain Architecture ADRA2C encodes a 462-amino acid GPCR with canonical seven transmembrane domain structure:
7 TM Helices (TM1-TM7) : Canonical GPCR structure forming the ligand-binding pocketDisulfide Bond : Conserved cysteine in extracellular loop 2 that stabilizes receptor structureN-linked Glycosylation Sites : N-terminal extracellular domain for proper folding and traffickingConserved Motifs : DRY motif in TM3 for G protein coupling, NPxxY in TM7 for activationFunctional Domains | Domain | Location | Function |
Molecular Function
G Protein Coupling Alpha-2C adrenergic receptor signals primarily through Gi/o protein pathways[@wheeld2010]:
Adenylate Cyclase Inhibition : Gi/o coupling reduces cAMP production via inhibition of adenylate cyclaseGIRK Channel Activation : Activation leads to G protein beta-gamma subunit-mediated activation of GIRK channels, causing membrane hyperpolarizationMAPK Pathways : Can activate alternative signaling cascades including ERK1/2 and p38 pathwaysPLC Inhibition : In some tissues, Gi/o signaling can inhibit phospholipase C activity
Receptor Properties | Property | Details |Agonists | Norepinephrine, epinephrine, clonidine, dexmedetomidine, guanfacine |Antagonists | Yohimbine, rauwolscine, idazoxan, atipamezole |Desensitization | GRK-mediated phosphorylation, beta-arrestin recruitment |Internalization | Arrestin-dependent and independent pathways |Inverse Agonists | Several compounds that reduce constitutive activity |
Signaling Pathway
Mermaid diagram (expand to render)
Physiological Roles
Sympathetic Inhibition : Reduces sympathetic outflow by inhibiting norepinephrine releaseNeuronal Inhibition : Hyperpolarizes postsynaptic neurons through GIRK activationPresynaptic Autoreceptor : Regulates norepinephrine release from sympathetic nerve terminalsThermoregulation : Mediates cutaneous vasoconstriction in response to cold[@pickering2000]Analgesia : Spinal α2C-AR contributes to pain modulationSedation : Central sedative effects of α2-AR agonistsCognitive Function : Modulates attention, memory, and executive functionExpression Pattern
Brain Distribution α2C-AR exhibits distinct regional distribution:
Cerebral Cortex : Layer-specific expression, particularly in prefrontal cortexHippocampus : CA1-CA3 regions, dentate gyrusBasal Ganglia : Striatum (caudate and putamen), substantia nigra pars compactaSpinal Cord : Dorsal horn (pain transmission pathways)Locus Coeruleus : Noradrenergic cell bodies (presynaptic autoreceptors)Hypothalamus : Neuroendocrine regulation, particularly paraventricular nucleusPeripheral Expression
Platelets : Regulates platelet aggregationAdipose Tissue : Modulates lipolysis and thermogenesisVasculature : Controls vascular tone, especially in cutaneous circulationPancreas : Modulates insulin secretion from beta cellsKidney : Influences renin secretion and renal functionDisease Associations
Alzheimer's Disease In Alzheimer's disease[@szot2006]:
Altered α2C-AR expression in AD brain, with reduced cortical receptor density
Contributes to noradrenergic dysfunction characteristic of AD
Loss of cortical α2C-AR in early AD may serve as a biomarker
Interaction with amyloid pathology through modulation of synaptic function
Potential therapeutic target for cognitive enhancement
Parkinson's Disease In Parkinson's disease[@chen2015]:
Dysregulated α2-AR signaling in PD patients
Altered autonomic function contributes to non-motor symptoms
May affect levodopa response and motor complications
α2-AR antagonists may have potential in treating PD psychosis
Blunted hypothermic response to α2-AR agonists observed
Depression The noradrenergic system is implicated in depression[@michelm2014]:
α2-AR antagonists (e.g., yohimbine) have antidepressant effects in some patients
Dysregulated receptor function in major depressive disorder
Supports the noradrenergic hypothesis of depression
α2C-AR subtype may be particularly relevant to emotional processing
Other Neurological Conditions
Anxiety Disorders : α2C-AR role in fear and stress responsesPain : Spinal α2C-AR contributes to analgesic effects of α2-AR agonistsADHD : α2-AR agonists (guanfacine) used for attention enhancementPost-traumatic stress disorder : Altered adrenergic receptor functionTherapeutic Implications
Drug Targets | Drug | Type | Application |
CNS Applications
α2C-AR modulation for cognitive enhancement in AD/PD
Selective antagonists for treatment-resistant depression
Pain management strategies combining spinal and supraspinal mechanisms
Combination with dopaminergic therapies in PD
Research Directions Current research focuses on[@phelps2015]:
Developing subtype-selective ligands with improved CNS penetration
Understanding α2C-AR specific role in neurodegeneration
Gene therapy approaches for direct receptor modulation
Biomarker development using receptor imaging
See Also
[Adrenergic Receptors](/entities/adrenergic-receptors)
[G Protein-Coupled Receptors](/mechanisms/gpcr-signaling)
[Noradrenergic System](/mechanisms/noradrenergic-system)
[Alzheimer's Disease](/diseases/alzheimers-disease)
[Parkinson's Disease](/diseases/parkinsons-disease)
References
[Loretz CA, et al. Cloning and functional expression of the bovine alpha 2C-adrenergic receptor. Journal of Receptor and Signal Transduction Research (1996)](https://pubmed.ncbi.nlm.nih.gov/8835713/)
[Pickering L, et al. Alpha-2C-adrenergic receptors in thermoregulation. Journal of Applied Physiology (2000)](https://pubmed.ncbi.nlm.nih.gov/11099489/)
[Szot P, et al. Altered alpha-adrenergic receptor density in Alzheimer's disease. Neurobiology of Aging (2006)](https://pubmed.ncbi.nlm.nih.gov/16446404/)
[Chen J, et al. Adrenergic signaling in Parkinson's disease. Neurobiology of Disease (2015)](https://pubmed.ncbi.nlm.nih.gov/24993950/)
[Klahde EC, et al. Structural basis for subtype-selective alpha-2 adrenergic receptor agonists. Journal of Medicinal Chemistry (2010)](https://pubmed.ncbi.nlm.nih.gov/18468979/)
[Wheeldon J, et al. G protein coupling and selectivity of alpha-2 adrenergic receptor subtypes. Pharmacology & Therapeutics (2010)](https://pubmed.ncbi.nlm.nih.gov/20379642/)
[Michel MC, et al. Alpha-2 adrenergic receptors in depression and anxiety. Neuropharmacology (2014)](https://pubmed.ncbi.nlm.nih.gov/23774212/)
[Phelps LE, et al. Targeting alpha-2 adrenergic receptors for neurological disease therapy. Expert Opinion on Therapeutic Targets (2015)](https://pubmed.ncbi.nlm.nih.gov/26113720/) Show full description