Article Information
PubMed
Related Articles
- Structural Basis for Ligand Selectivity of Heteromeric Olfac...Structural Basis for Ligand Selectivity of Heteromeric Olfactory Cyclic Nucleotide-Gated Channels
Biophysical Journal, Volume 78, Issue 5, 1 May 2000, Pages 2307-2320
Mark S. Shapiro and William N. Zagotta
AbstractIn vertebrate olfactory receptors, cAMP produced by odorants opens cyclic nucleotide-gated (CNG) channels, which allow Ca entry and depolarization of the cell. These CNG channels are composed of subunits and at least two types of subunits that are required for increased cAMP selectivity. We studied the molecular basis for the altered cAMP selectivity produced by one of the subunits (CNG5, CNC4, OCNC2) using cloned rat olfactory CNG channels expressed in oocytes. Compared with subunit homomultimers ( channels), channels composed of and subunits (+ channels) were half-activated () by eightfold less cAMP and fivefold less cIMP, but similar concentrations of cGMP. The values for heteromultimers of the subunit and a chimeric subunit with the subunit cyclic nucleotide-binding region (CNBR) (+-CNBR channels) were restored to near the values for channels. Furthermore, a single residue in the CNBR could account for the altered ligand selectivity. Mutation of the methionine residue at position 475 in the subunit to a glutamic acid as in the subunit (-M475E) reverted the / and / ratios of +-M475E channels to be very similar to those of channels. In addition, comparison of +-CNBR channels with +-M475E channels suggests that the CNBR of the subunit contains amino acid differences at positions other than 475 that produce an increase in the apparent affinity for each ligand. Like the wild-type subunit, the chimeric / subunits conferred a shallow slope to the dose-response curves, increased voltage dependence, and caused desensitization. In addition, as for + channels, block of +CNBR channels by internal Mg was not steeply voltage-dependent ( ∼1) as compared to block of channels ( 2.7). Thus, the ligand-independent effects localize outside of the CNBR. We propose a molecular model to explain how the subunit alters ligand selectivity of the heteromeric channels.
Abstract | Full Text | PDF (454 kb) - Multimerization of the Ligand Binding Domains of Cyclic Nucl...Multimerization of the Ligand Binding Domains of Cyclic Nucleotide-Gated Channels
Neuron, Volume 36, Issue 1, 26 September 2002, Pages 93-103
Kimberly Matulef and William N. Zagotta
SummaryCyclic nucleotide-gated (CNG) channels comprise four subunits and are activated by the direct binding of cyclic nucleotide to an intracellular domain on each subunit. This ligand binding domain is thought to contain a β roll followed by two α helices, designated the B and C helices. To examine the quaternary structure of CNG channels and how it changes during ion channel gating, we introduced single cysteines along the C helix of each subunit in an otherwise cysteineless channel. We found that cysteines on the C helices could form intersubunit disulfide bonds, even between diagonal subunits. Disulfide bond formation occurred primarily in closed channels and inhibited channel opening. These data suggest that the C helices from all four channel subunits are in close proximity in the closed state and move apart during channel opening.
Summary | Full Text | PDF (438 kb) - Molecular Rearrangements in the Ligand-Binding Domain of Cyc...Molecular Rearrangements in the Ligand-Binding Domain of Cyclic Nucleotide–Gated Channels
Neuron, Volume 24, Issue 2, 1 October 1999, Pages 443-452
Kimberly Matulef, Galen E Flynn and William N Zagotta
SummaryCyclic nucleotide–gated (CNG) channels are activated in response to the direct binding of cyclic nucleotides to an intracellular domain. This domain is thought to contain a β roll and two α helices, designated the B and C helices. To probe the conformational changes occurring in the ligand-binding domain during channel activation, we used the substituted cysteine accessibility method (SCAM). We found that a residue in the β roll, C505, is more accessible in unliganded channels than in liganded channels, whereas a residue in the C helix, G597C, is more accessible in closed channels than in open channels. These results support a molecular mechanism for channel activation in which the ligand initially binds to the β roll, followed by an opening allosteric transition involving the relative movement of the C helix toward the β roll.
Summary | Full Text | PDF (267 kb) - …more
Copyright © 1996 The Biophysical Society. All rights reserved.
Biophysical Journal, Volume 70, Issue 6, 2667-2679, 1 June 1996
doi:10.1016/S0006-3495(96)79836-3
Research Article
Subunit interactions in the activation of cyclic nucleotide-gated ion channels
M.D. Varnum and W.N. Zagotta
Abstract
Cyclic nucleotide-gated (CNG) ion channels of retinal photoreceptors and olfactory neurons are multimeric proteins of unknown stoichiometry. To investigate the subunit interactions that occur during CNG channel activation, we have used tandem cDNA constructs of the rod CNG channel to generate heteromultimeric channels composed of wild-type and mutant subunits. We introduced point mutations that affect channel activation: 1) D604M, which alters the relative ability of agonists to promote the allosteric conformational change(s) associated with channel opening, and 2) T560A, which primarily affects the initial binding affinity for cGMP, and to a lesser extent, the allosteric transition. At saturating concentrations of agonist, heteromultimeric channels were intermediate between wild-type and mutant homomultimers in agonist efficacy and apparent affinity for cGMP, cIMP, and cAMP, consistent with a model for the allosteric transition involving a concerted conformational change in all of the channel subunits. Results were also consistent with a model involving independent transitions in two or three, but not one or four, of the channel subunits. The behavior of the heterodimers implies that the channel stoichiometry is some multiple of 2 and is consistent with a tetrameric quaternary structure for the functional channel complex. Steady-state dose-response relations for homomultimeric and heteromultimeric channels were well fit by a Monod, Wyman, and Changeux model with a concerted allosteric opening transition stabilized by binding of agonist.
