Abstract
Blockade of ion channels passing through the NMDA receptors of isolated rat hippocampus pyramidal neurons with tetraalkylammonium compounds, 9-aminoacridine, and Mg2+was studied using patch-clamp methods in the whole-cell configuration. Currents through NMDA channels were evoked by application of 100 μM aspartate in magnesium-free medium containing glycine (3 μM) to neurons. Analysis of the kinetics, charge transfer, and relationships between the extent of suppression of stationary currents on the one hand and membrane potential, agonist concentration, and blocker concentration on the other showed that blockers had different effects on the closing, desensitization, and agonist dissociation of NMDA channels. The size of the blocker was found to be the decisive factor determining its action on the gating functions of NMDA channels: larger blockers prevented closure and/or desensitization of the channel; smaller blockers only had partial effects on these processes, while the smallest blockers had no effect at all. These experiments showed that the apparent affinity of the blocker for the channel (1/IC50) depended not only on the microscopic equilibrium dissociation constant (K d), but also on the number of blocker binding sites, their mutual influences, and, of particular importance, the interaction of the blocker with the gating structures of the channel. These data led us to propose hypotheses relating to the geometry of the NMDA channel and the structure of its gating mechanism. The channel diameter at the level of activated gates was estimated to be 11 Å.
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REFERENCES
S. G. Koshelev and B. I. Khodorov, “Tetraethylammonium and tetrabutylammonium as tools for studies of NMDA channels in neuron membranes,” Biol. Membrany, 9, 1365-1369 (1992).
S. G. Koshelev and B. I. Khodorov, “Tetrabutylammonium, tacrine, and 9-aminoacridine, which block open NMDA channels, prevent channel closure and desensitization,” Biol. Membrany, 12, 89-104 (1995).
S. M. Antonov, V. E. Gmiro, and J. W. Johnson, “Binding sites for permeant ions in the channel of NMDA receptors and their effects on channel block,” Nat. Neurosci., 1, 451-456 (1998).
S. M. Antonov and J. W. Johnson, “Voltage-dependent interaction of open-channel blocking molecules with gating of NMDA receptors in rat cortical neurons,” J. Physiol., 493, 425-445 (1996).
S. M. Antonov and J. W. Johnson, “Permeant ion regulation of N-methyl-d-aspartate receptor channel block by Mg2+,” Proc. Natl. Acad. Sci. USA, 96, 14571-14576 (1999).
S. M. Antonov, J. W. Johnson, N. Y. Lukomskaya, N. N. Potapyeva, V. E. Gmiro, and L. G. Magazanik, “Novel adamantane derivatives act as blockers of open ligand-gated channels and as anticonvulsants,” Mol. Pharmacol., 47, 558-567 (1995).
P. Ascher, P. Bregestovski, and L. Nowak, “NMDA-activated channels of mouse central neurons in magnesium-free solutions,” J. Physiol., 399, 207-226 (1988).
F. Asztely and B. Gustafsson, “Ionotropic glutamate receptors: Their role in the expression of hippocampal synaptic plasticity,” Mol. Neurobiol., 12, 1-11 (1996).
M. Benveniste and M. L. Mayer, “Kinetic analysis of antagonist action at N-methyl-D-aspartic acid receptors. Two binding sites each for glutamate and glycine,” Biophys. J., 59, 560-573 (1991).
M. Benveniste and M. L. Mayer, “Trapping of glutamate and glycine during open channel block of rat hippocampal neuron NMDA receptors by 9-aminoacridine,” J. Physiol., 483, 367-384 (1995).
M. Benveniste, J.-M. Mienville, E. Sernafor, and M. L. Mayer, “Concentration-jump experimental with NMDA antagonists in mouse cultured hippocampal neurons,” J. Neurophysiol., 63, 1373-1384 (1990).
T. V. Bliss and G. L. Collingridge, “A synaptic model of memory: longterm potentiation in the hippocampus,” Nature, 361, 31-39 (1993).
H. T. Cline, E. A. Debski, and M. Constantine-Paton, “The role of NMDA receptor in the development of the frog visual system,” Adv. Exp. Med. Biol., 268, 197-203 (1990).
M. Constantine-Paton, “NMDA receptor as a mediator of activitydependent synaptogenesis in the developing brain,” Cold. Spring Harb. Symp. Quant. Biol., 55, 431-443 (1990).
A. C. S. Costa and E. X. Albuquerque, “Dynamics of the actions of tetrahydro-9-aminoacridine and 9-aminoacridine on glutamatergic currents. Concentration-jump studies in cultured rat hippocampal neurons,” J. Pharmacol. Exp. Ther., 268, 503-514 (1994).
S. G. Cull-Candy and M. M. Usowich, “On the multiple-conductance single channels activated by excitatory amino acids in large cerebellar neurones of the rat,” J. Physiol., 415, 555-582 (1989).
W. Danysz and C. G. Parsons, “Glycine and N-methyl-D-aspartate receptors. Physiological significance and possible therapeutic application,” Pharmacol. Rev., 50, 597-664 (1998).
W. Danysz, C. G. Parsons, I. Breskink, and G. Quack, “Glutamate in CNS disorders,” Drug News Perspect., 8, 261-277 (1995).
R. Dingledine, K. Borges, D. Bowie, and S. F. Traynelis, “The glutamate receptor ion channels,” Pharmacol. Rev., 51, 7-61 (1999).
C. E. Jahr and C. F. Stevens, “A quantitative description of NMDA receptor channel kinetic behavior,”: J. Neurosci., 10, 1830-1837 (1990).
J. W. Johnson, S. M. Antonov, T. S. Blanpied, and Y. Li-Smerin, “Channel block of NMDA receptor,” in: Excitatory Amino Acids and Synaptic Transmission, H. V. Wheal (ed.), Academic Press Inc., London (1997), pp. 99-113.
J. W. Johnson and P. Ascher, “Glycine potentiates the NMDA response in cultured mouse brain neurons,” Nature, 325, 529-531 (1987).
W. Kauzmann, “Some factors in the interpretation of protein denaturation,” Adv. Protein Chem., 14, 1-63 (1959).
H. Komuro and P. Pakic, “Modulation of neuronal migration by NMDA receptors,” Science, 260, 95-97 (1993).
R. Lester, J. D. Clements, G. L. Westbrook, and C. E. Jahr, “Channel kinetics determine the time course of NMDA receptor-mediated synaptic currents,” Nature, 346, 565-567 (1990).
R. A. J. Lester and C. E. Jahr, “NMDA channel behaviour depends on agonist affinity,” J. Neurosci., 12, 635-643 (1992).
S. A. Lipton, “Prospects for clinically tolerated NMDA antagonists: open-channel blockers and alternative redox states of nitric oxide,” TINS, 16, 527-532 (1993).
A. B. MacDermott, M. L. Mayer, G. L. Westbrook, S. J. Smith, and J. L. Baker, “NMDA receptor activation increases cytoplasmic calcium concentration in cultured spinal cord neurones,” Nature, 321, 519-522 (1986).
S. Maren and M. Baudry, “Properties and mechanisms of long-term synaptic plasticity in the mammalian brain: relationships to learning and memory,” Neurobiol. Learn. Mem., 63, 1-18 (1995).
L. Nowak, P. Bregestovski, P. Ascher, A. Herbert, and A. Prochiantz, “Magnesium gates glutamate-activated channels in mouse central neurones,” Nature, 307, 462-465 (1984).
C. G. Parsons, W. Danysz, and G. Quack, “Glutamate in CNS disorders as a target for drug development: an update,” Drug News Perspect., 11, 523-569 (1998).
C. G. Parsons, W. Danysz, and G. Quack, “Memantine is a clinically well tolerated N-methyl-D-aspartate (NMDA) receptor antagonist-a review of preclinical data,” Neuropharmacology, 38, 735-767 (1999).
A. I. Sobolevsky, “Two-component blocking kinetics of open NMDA channels by organic cations,” Biochim. Biophys. Acta, 1416, 69-91 (1999).
A. Sobolevsky and S. Koshelev, “Two blocking sites of amino-adamantane derivatives in open N-methyl-D-aspartate channels,” Biophys. J., 74, 1305-1319 (1998).
A. I. Sobolevsky, S. G. Koshelev, and B. I. Khodorov, “Probing of NMDA channels with fast blockers,” J. Neurosci., 19, 10611-10626 (1999).
H. G. Traven, L. Brodin, A. Lansner, O. Ekeberg, P. Wallens, and S. Grillner, “Computer simulations of NMDA and non-NMDA receptor-mediated synaptic drive: sensory and supraspinal modulation of neurons and small networks,” J. Neurophysiol., 70, 695-709 (1993). 37. A. Villarroel, N. Bernashev, and B. Sakmann, “Dimensions of the narrow portion of a recombinant NMDA receptor channel,” Biophys. J., 68, 866-875 (1995).
V. S. Vorobjev, “Vibrodissection of sliced mammalian nervous tissue,” J. Neurosci. Methods, 38, 145-150 (1991).
A. M. Woodhull, “Ionic blockage of sodium channels in nerve,” J. Gen. Physiol., 61, 687-708 (1973).
M. M. Zarei and J. A. Dani, “Structural basis for explaining openchannel blockade of the NMDA receptor,” J. Neurosci., 15, 1446-1454 (1995).
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Sobolevskii, A.I., Khodorov, B.I. Blocker Studies of the Functional Architecture of the NMDA Receptor Channel. Neurosci Behav Physiol 32, 157–171 (2002). https://doi.org/10.1023/A:1013927409034
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DOI: https://doi.org/10.1023/A:1013927409034