α10: A determinant of nicotinic cholinergic receptor function in mammalian vestibular and cochlear mechanosensory hair cells

Elgoyhen, Ana Belén; Vetter, Douglas E.; Katz, Eleonora; Rothlin, Carla V.; Heinemann, Stephen F.; Boulter, Jim

doi:10.1073/pnas.051622798

Cited by 634 publications

(873 citation statements)

References 26 publications

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“…The chick ␣8 subunit forms homomeric receptors that desensitize, at least in oocytes, with the same order of magnitude as ␣7 receptors but at much lower concentrations of nicotine or ACh Gotti et al, 1994). Both the rate and extent of desensitization of slowly/ nondesensitizing cochlear ␣9 homomeric receptors are enhanced when these subunits are expressed together with ␣10 subunits (Elgoyhen et al, 2001; but see Sgard et al, 2002).…”

Section: Homomeric ␣-Receptorsmentioning

confidence: 99%

Desensitization of neuronal nicotinic receptors

2002

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ABSTRACT:The loss of functional response upon continuous or repeated exposure to agonist, desensitization, is an intriguing phenomenon if not as yet a welldefined physiological mechanism. However, detailed evaluation of the properties of desensitization, especially for the superfamily of ligand-gated ion channels, reveals how the nervous system could make important use of this process that goes far beyond simply curtailing excessive receptor stimulation and the prevention of excitotoxicity. Here we will review the mechanistic basis of desensitization and discuss how the subunit-dependent properties and regulation of nicotinic acetylcholine receptor (nAChR) desensitization contribute to the functional diversity of these channels. These studies provide the essential framework for understanding how the physiological regulation of desensitization could be a major determinant of synaptic efficacy by controlling, in both the short and long term, the number of functional receptors. This type of mechanism can be extended to explain how the continuous occupation of desensitized receptors during chronic nicotine exposure contributes to drug addiction, and highlights the potential significance of prolonged nAChR desensitization that would also occur as a result of extended acetylcholine lifetime during treatment of Alzheimer's disease with cholinesterase inhibitors. Thus, a clearer picture of the importance of nAChR desensitization in both normal information processing and in various diseased states is beginning to emerge.

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Section: Homomeric ␣-Receptorsmentioning

confidence: 99%

Desensitization of neuronal nicotinic receptors

2002

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“…Each individual nAChR channel is composed of five membrane-spanning subunits arranged to form a central ion channel pore. To date, 17 nAChR subunit genes have been cloned from vertebrates (Elgoyhen et al, 2001). This large multigene family encodes subunits of the neuronal and skeletal muscle type nAChRs.…”

Section: Diversity Of Nachr Subtypesmentioning

confidence: 99%

Regulatory mechanisms that govern nicotinic synapse formation in neurons

et al. 2002

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Individual cholinoceptive neurons express high levels of different neuronal nicotinic acetylcholine receptor (nAChR) subtypes, and target them to the appropriate synaptic regions for proper function. This review focuses on the intercellular and intracellular processes that regulate nAChR expression in vertebrate peripheral nervous system (PNS) and central nervous system (CNS) neurons. Specifically, we discuss the cellular and molecular mechanisms that govern the induction and maintenance of nAChR expression-innervation, target tissue interactions, soluble factors, and activity. We define the regulatory principles of interneuronal nicotinic synapse differentiation that have emerged from these studies. We also discuss the molecular players that target nAChRs to the surface membrane and the interneuronal synapse.

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“…In other cells, 12 'neuronal' nAChR subunit genes encoding a pentameric protein have been identified and designated a2-a10 and b2-b4. [12][13][14][15] Each subunit has four putative transmembrane-spanning domains and a similar topological structure. The a7 and a9 subunits are capable of forming homomeric nAChR channels, which are a-bungarotoxin sensitive.…”

Section: Introductionmentioning

confidence: 99%

“…The heteromeric channels can be composed of a2, a3, a4, a5, a6, b2, b3 and b4 subunits, for example, a3(b2/b4)±a5 and also a9 can form a heteromeric channel with a10. 15 The mAChRs are single-subunit transmembrane glycoproteins that mediate the metabolic response to ACh through the interactions of G proteins with signal transducing enzymes, leading to increases or decreases in second messengers, ion concentrations and modulations of protein kinase activities. The mAChR family is comprised of five, M 1 -M 5 , G protein-coupled receptor subtypes.…”

Section: Introductionmentioning

confidence: 99%

Plasticity of the murine spleen T-cell cholinergic receptors and their role in in vitro differentiation of naïve CD4 T cells toward the Th1, Th2 and Th17 lineages

et al. 2011

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Acetylcholine (ACh) regulates vital functions of T cells by acting on the nicotinic and muscarinic classes of cholinergic receptors, nAChR and mAChRs, respectively. This study was performed in murine splenic T cells. In freshly isolated CD4 and CD8 T cells, we detected mRNAs encoding a5, a9, a10, b1, b2, b4 nAChR subunits and M 1 , M 3 , M 4 and M 5 mAChR subtypes, whereas a2 was detected only in CD8 T cells. In vitro activation of CD4 T cells through T-cell receptor (TCR)/CD3 cross-linking was associated with the appearance of a4 and a7, upregulation of a5, a10, b4, M 1 and M 5 and downregulation of a9 and b2, whereas in vitro activation of CD8 T cells also featured the appearance of a4 and a7, as well as upregulation of a2, a5, b4, M 1 and M 4 , and downregulation of a10, b1, b2 and M 3 . In vitro polarization toward T helper (Th) 1 lineage was associated with a decrease of b2, b4 and M 3 expression; that toward Th2 cells with downregulation of a9 and M 3 , and upregulation of M 1 and M 5 ; and that toward Th17 phenotype with downregulation of a9, a10, b2 and M 3 mAChR. Polarized T cells also expressed a4, but not a1, a2, a3, a6, b3 or M 2 . To determine the role of cholinergic receptors in mediating the immunoregulatory action of autocrine/paracrine ACh, we analyzed the effects of nicotinic and muscarinic agonists ± antagonists on cytokine production in the CD4 þ CD62L þ T cells co-stimulated via TCR/CD3 cross-linking. The nicotinergic stimulation upregulated interferon-g (IFN-g) and downregulated interleukin (IL)-17 secretion, whereas the muscarinic stimulation enhanced IL-10 and IL-17 and inhibited INF-g secretion. These results demonstrated plasticity of the T-cell cholinergic system.

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α10: A determinant of nicotinic cholinergic receptor function in mammalian vestibular and cochlear mechanosensory hair cells

Cited by 634 publications

References 26 publications

Desensitization of neuronal nicotinic receptors

Desensitization of neuronal nicotinic receptors

Regulatory mechanisms that govern nicotinic synapse formation in neurons

Plasticity of the murine spleen T-cell cholinergic receptors and their role in in vitro differentiation of naïve CD4 T cells toward the Th1, Th2 and Th17 lineages

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