The α7 Nicotinic Acetylcholine Receptor Subunit Exists in Two Isoforms that Contribute to Functional Ligand-Gated Ion Channels

Severance, Emily G.; Zhang, Hongling; Cruz, Yolmari; Pakhlevaniants, Sergei; Hadley, Stephen; Amin, Jahanshah; Wecker, Lynn; Reed, Crystal; Cuevas, Javier

doi:10.1124/mol.104.000059

Cited by 39 publications

(27 citation statements)

References 40 publications

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“…Although we have immunocytochemical data confirming expression of α7-and β2-subunits in the same enteric neurons (not shown), we have no independent evidence of co-localization in the same nAChR molecule. Furthermore, the presence of α7-isoforms 1 and 2 (Severance et al, 2004) in the ENS remains an open question. Since they differ in their extracellular domain, we could not have distinguished them with mAb 306, which recognizes an intracellular epitope; and since we did not use α-Bgt for functional studies, we could not assess their individual contributions to the overall α7-nAChR pool on the basis of their differential affinities for this toxin.…”

Section: Discussionmentioning

confidence: 99%

Optical studies of nicotinic acetylcholine receptor subtypes in the guinea-pig enteric nervous system

Obaid

Nelson

Lindstrom

et al. 2005

Journal of Experimental Biology

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ErratumObaid, A. L., Nelson, M. E., Lindstrom, J. and Salzberg, B. M. (2005). Optical studies of nicotinic acetylcholine receptor subtypes in the guinea-pig enteric nervous system. J. Exp. Biol. 208, 2981-3001. In the original published on-line version of this paper, the acceptance date was incorrect. It should have read 2 June 2005. The error has been rectified and the current on-line version and print versions are correct.We apologise to authors and readers for any inconvenience this may have caused. 2981Decoding the structure and function of native nicotinic acetylcholine receptors (nAChRs) is complex. Although the expression of defined combinations of nAChR-subunits in Xenopus oocytes permits the comparison of pharmacological properties of individual nAChR-subtypes, single neurones often express more than one subtype, making the physiological roles of nAChRs in intact neuronal networks difficult to assess (Colquhoun and Patrick, 1997). The function of a given nAChR depends upon its pre-, post-or peri-synaptic location as well as the activity of neighbouring non-nicotinic receptors. In addition, the properties of any neuronal ensemble depend not only on the intrinsic conductances of its neurones and the specific attributes of its many synapses but also on the complex and nonlinear dynamic interactions that result from the multiple parallel connectivity of its component cells (Parsons et al., 1991). Therefore, to understand nicotinic responses at the network level, it is necessary to record at high spatial and temporal resolution to characterize the behaviour of individual neurones and at lower spatial resolution to capture a panoramic view of network activity and to assess the directionality of the nicotinic pathways along the circumferential as well as the longitudinal axes.The enteric nervous system (ENS) regulates most gastrointestinal functions. Its neurones are clustered in ganglia that interconnect to form distinct plexuses in the gut wall: the myenteric plexus lies between the longitudinal and circular muscle layers, and the submucous plexus between the circular muscle layer and the mucosa. The behaviour of the effector Nicotinic transmission in the enteric nervous system (ENS) is extensive, but the role of individual nicotinic acetylcholine receptor (nAChR) subtypes in the functional connectivity of its plexuses has been elusive. Using monoclonal antibodies (mAbs) against neuronal α3-, α4-, α3/α5-, β2-, β4-and α7-subunits, combined with radioimmunoassays and immunocytochemistry, we demonstrate that guinea-pig enteric ganglia contain all of these nAChR-subunits with the exception of α4, and so, differ from mammalian brain. This information alone, however, is insufficient to establish the functional role of the identified nAChR-subtypes within the enteric networks and, ultimately, their specific contributions to gastrointestinal physiology. We have used voltagesensitive dyes and a high-speed CCD camera, in conjunction with specific antagonists to various nAChRs, to elucidate some of the distinct cont...

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Section: Discussionmentioning

confidence: 99%

Optical studies of nicotinic acetylcholine receptor subtypes in the guinea-pig enteric nervous system

Obaid

Nelson

Lindstrom

et al. 2005

Journal of Experimental Biology

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“…On the other hand, homomeric ligand-gated channels are also thought to exist in certain cases. Thus, the α7 nicotinic acetylcholine receptor subunit was shown to form functional homomeric AChRs in Xenopus ooctyes (Seguela et al, 1993), and there is now good evidence that native α7-nAChRs are homopentameric structures (Chen and Patrick, 1997;Severance et al, 2004).…”

Section: Introductionmentioning

confidence: 98%

Random Assembly of GABA ρ1 and ρ2 Subunits in the Formation of Heteromeric GABA C Receptors

2006

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1. Various combinations of the rho subunits (rho(1A), rho(1B), rho(2A), rho(2B)) of GABA(C) receptors cloned from white perch retina were expressed in Xenopus oocytes, and electrophysiological and pharmacological methods were used to test their ability to co-assemble into heteromeric receptors. Simultaneous injection of the two subunits, irrespective of their relative proportions, led invariably to the formation of a preponderance of heteromeric receptors. 2. The GABA deactivation responses elicited from these cells could be described by a single exponential decay, and their pharmacological responses deviated significantly from those expected of a simple mixture of two homomeric rho(1) and rho(2) receptors. In contrast, a double exponential function comprising fast and slow components was required to fit the GABA deactivation responses elicited from oocytes sequentially expressing rho(1) and rho(2) subunits, a condition that favors the formation of a mixture of homomeric rho(1) and rho(2) receptors. 3. Both the GABA-response kinetics and the sensitivity to picrotoxin of the heteromeric perch rho(1B)rho(2A) receptor varied with the proportion of the subunit RNA injected, indicating there is no fixed stoichiometry for their co-assembly into heteromeric rho(1)rho(2) receptors. 4. If native GABA(C) receptors in retinal neurons behave in a similar manner as in the oocyte expression system, these finding suggest that the properties of their GABA(C) receptors are likely to be influenced by the transcription/translation efficiency of GABA rho subunit genes.

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“…The role of ␣7 subtype is supported by the finding that ␣7 nAChRmediated currents can also be measured in cultured superior cervical ganglion neurons (97). In addition, two different splice variants of ␣7 nAChRs have been detected in the superior cervical ganglion with distinct desensitization properties (23,147). In the case NE release, ␣3␤4 nAChRs were assumed for both TTX-sensitive and TTXinsensitive release forms in cultured sympathetic neurons (85).…”

Section: B Subtypes Of Nachrs Involved In the Release Of Transmittersmentioning

confidence: 99%

Nonsynaptic Chemical Transmission Through Nicotinic Acetylcholine Receptors

Lendvai¹,

Vizi²

2008

Physiological Reviews

124

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This review attempts to organize the different aspects of nicotinic transmission in the context of nonsynaptic interactions. Nicotinic acetylcholine receptors (nAChRs) dominantly operate in the nonsynaptic mode in the central nervous system despite their ligand-gated ion-channel nature, which would otherwise be better suited for fast synaptic transmission. This fast form of nonsynaptic transmission, most likely unique to nAChRs, represents a new avenue in the communication platforms of the brain. Cholinergic messages received by nAChRs, arriving at a later phase following synaptic activation, can interfere with dendritic signal integration. Nicotinic transmission plays a role in both neural plasticity and cellular learning processes, as well as in long-term changes in basic activity through fast activation, desensitization of receptors, and fluctuations of the steady-state levels of ACh. ACh release can contribute to plastic changes via activation of nAChRs in neurons and therefore plays a role in learning and memory in different brain regions. Assuming that nAChRs in human subjects are ready to receive long-lasting messages from the extracellular space because of their predominantly nonsynaptic distribution, they offer an ideal target for drug therapy at low, nontoxic drug levels.

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The α7 Nicotinic Acetylcholine Receptor Subunit Exists in Two Isoforms that Contribute to Functional Ligand-Gated Ion Channels

Cited by 39 publications

References 40 publications

Optical studies of nicotinic acetylcholine receptor subtypes in the guinea-pig enteric nervous system

Optical studies of nicotinic acetylcholine receptor subtypes in the guinea-pig enteric nervous system

Random Assembly of GABA ρ1 and ρ2 Subunits in the Formation of Heteromeric GABA C Receptors

Nonsynaptic Chemical Transmission Through Nicotinic Acetylcholine Receptors

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