Auerbach A (1993), A statistical analysis of acetylcholine recepto...

XB-ART-22891

J Physiol 1993 Feb 01;461:339-78.

Show Gene links Show Anatomy links

A statistical analysis of acetylcholine receptor activation in Xenopus myocytes: stepwise versus concerted models of gating.

Auerbach A .

???displayArticle.abstract???
1. The kinetic properties of single channel currents from fetal-type acetylcholine receptors in embryonic Xenopus myocytes (60 h old) have been analysed by a maximum-likelihood method. 2. At very high acetylcholine (ACh) concentrations (up to 5 mM) the effective opening rate appears to saturate at approximately 30,000 s-1. 3. The kinetics were analysed according to the standard concerted scheme that postulates a single channel-opening conformational change after two agonists are bound, and a rarely invoked stepwise scheme that postulates semi-independent conformational changes in two distinct gating domains. Both models assume that agonist cannot escape from a channel (or domain) that is in its activated conformation. 4. With either activation scheme the kinetic analyses indicate that ACh binds at a rate of approximately 2 x 10(8) s-1 M-1 and dissociates from doubly liganded receptors at a rate of approximately 28,000 s-1, and that the activation process is asymmetric, i.e. the binding (concerted model) or gating (stepwise model) transitions are not equal and independent. 5. In eighteen of twenty-seven file-by-file comparisons, the likelihood of the stepwise model was greater than that of the concerted model. In seven such comparisons, the likelihood of the concerted model was greater than that of the stepwise model, and in two there was no difference. Log likelihood ratio distributions were obtained from three files (those with the most events) by multiple cycles of resampling and fitting. The means of these distributions were significantly greater than zero, indicating that the stepwise scheme was as good as, or better than, the concerted scheme in describing receptor activation. 6. According to the stepwise view, two binding sites must be occupied and two 'gates' activated for conduction to occur. Although equivalent binding is not an essential aspect of stepwise activation, the binding sites can be identical and have a low affinity for ACh (Kd approximately 130 microM). Either the isomerization rates of the gating domains are different, or they are influenced by the conformational status of its counterpart, with activation increasing approximately 3-fold and deactivation decreasing approximately 10-fold if the complementary domain is in the active conformation. Stepwise activation predicts that the decay of the endplate current is determined by five rates.

???displayArticle.pubmedLink??? 8350269
???displayArticle.pmcLink??? PMC1175261
???displayArticle.link??? J Physiol
???displayArticle.grants??? [+]

References [+] :

Ackers, Molecular code for cooperativity in hemoglobin. 1992, Pubmed

Ackers, Molecular code for cooperativity in hemoglobin. 1992, Pubmed
Auerbach, Single-channel dose-response studies in single, cell-attached patches. 1991, Pubmed , Xenbase
Auerbach, Activation of the primary kinetic modes of large- and small-conductance cholinergic ion channels in Xenopus myocytes. 1987, Pubmed , Xenbase
Auerbach, Heterogeneous kinetic properties of acetylcholine receptor channels in Xenopus myocytes. 1986, Pubmed , Xenbase
Bates, Glutamate receptor-channel gating. Maximum likelihood analysis of gigaohm seal recordings from locust muscle. 1990, Pubmed
Blount, Molecular basis of the two nonequivalent ligand binding sites of the muscle nicotinic acetylcholine receptor. 1989, Pubmed
Colquhoun, Fast events in single-channel currents activated by acetylcholine and its analogues at the frog muscle end-plate. 1985, Pubmed
Colquhoun, On the stochastic properties of bursts of single ion channel openings and of clusters of bursts. 1982, Pubmed
Colquhoun, Activation of ion channels in the frog end-plate by high concentrations of acetylcholine. 1988, Pubmed
Colquhoun, Relaxation and fluctuations of membrane currents that flow through drug-operated channels. 1977, Pubmed
Crouzy, Yet another approach to the dwell-time omission problem of single-channel analysis. 1990, Pubmed
DEL CASTILLO, Interaction at end-plate receptors between different choline derivatives. 1957, Pubmed
Dionne, Characterization of drug iontophoresis with a fast microassay technique. 1976, Pubmed
FATT, Spontaneous subthreshold activity at motor nerve endings. 1952, Pubmed
HODGKIN, A quantitative description of membrane current and its application to conduction and excitation in nerve. 1952, Pubmed
Horn, Statistical properties of single sodium channels. 1984, Pubmed
Horn, Estimating kinetic constants from single channel data. 1983, Pubmed
Horn, Statistical methods for model discrimination. Applications to gating kinetics and permeation of the acetylcholine receptor channel. 1987, Pubmed
Jackson, Perfection of a synaptic receptor: kinetics and energetics of the acetylcholine receptor. 1989, Pubmed
Jackson, Dependence of acetylcholine receptor channel kinetics on agonist concentration in cultured mouse muscle fibres. 1988, Pubmed
Jackson, Kinetics of unliganded acetylcholine receptor channel gating. 1986, Pubmed
Johnson, Decidium. A novel fluorescent probe of the agonist/antagonist and noncompetitive inhibitor sites on the nicotinic acetylcholine receptor. 1987, Pubmed
Joseph, Anatomy of a conformational change: hinged "lid" motion of the triosephosphate isomerase loop. 1990, Pubmed
KATZ, A study of the desensitization produced by acetylcholine at the motor end-plate. 1957, Pubmed
Kidokoro, Acetylcholine receptor channels in Xenopus myocyte culture; brief openings, brief closures and slow desensitization. 1990, Pubmed , Xenbase
Koshland, Comparison of experimental binding data and theoretical models in proteins containing subunits. 1966, Pubmed
Land, Kinetic parameters for acetylcholine interaction in intact neuromuscular junction. 1981, Pubmed
Liu, Opening rate of acetylcholine receptor channels. 1991, Pubmed
Lolis, Crystallographic analysis of the complex between triosephosphate isomerase and 2-phosphoglycolate at 2.5-A resolution: implications for catalysis. 1990, Pubmed
Milburn, Three-dimensional structures of the ligand-binding domain of the bacterial aspartate receptor with and without a ligand. 1991, Pubmed
Ogden, Ion channel block by acetylcholine, carbachol and suberyldicholine at the frog neuromuscular junction. 1985, Pubmed
Pedersen, d-Tubocurarine binding sites are located at alpha-gamma and alpha-delta subunit interfaces of the nicotinic acetylcholine receptor. 1990, Pubmed
Pompliano, Stabilization of a reaction intermediate as a catalytic device: definition of the functional role of the flexible loop in triosephosphate isomerase. 1990, Pubmed
Rohrbough, Changes in kinetics of acetylcholine receptor channels after initial expression in Xenopus myocyte culture. 1990, Pubmed , Xenbase
Roux, A general solution to the time interval omission problem applied to single channel analysis. 1985, Pubmed
Sachs, The automated analysis of data from single ionic channels. 1982, Pubmed
Sakmann, Single acetylcholine-activated channels show burst-kinetics in presence of desensitizing concentrations of agonist. 1980, Pubmed
Sigworth, Data transformations for improved display and fitting of single-channel dwell time histograms. 1987, Pubmed
Sine, Agonists block currents through acetylcholine receptor channels. 1984, Pubmed
Sine, Activation of Torpedo acetylcholine receptors expressed in mouse fibroblasts. Single channel current kinetics reveal distinct agonist binding affinities. 1990, Pubmed