2019
DOI: 10.1016/j.neuron.2019.07.030
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Agonist Selectivity and Ion Permeation in the α3β4 Ganglionic Nicotinic Receptor

Abstract: Highlights d The a3b4 ganglionic nicotinic receptor is a target for antiaddiction therapeutics d Receptor structures were determined in a functionally supportive lipidic environment d Comparisons with the a4b2 subtype suggest principles underlying ligand selectivity d Lateral portals in the intracellular domain facilitate ion permeation

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Cited by 161 publications
(162 citation statements)
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“…Further rearrangement to the open state contracts both the β1-β2/M2 and F/M2-M3 clefts (Fig 5C, Appendix Fig S5A). The same pattern is evident in agonist-bound versus apo structures of ELIC, GluCl, glycine and nicotinic receptors (Appendix Fig S5B-E) [49]–[54], and in open/desensitized versus inhibitor-bound structures of DeCLIC and GABA A receptors (Appendix Fig S5F-G) [55], [56]. A noted exception is the 5-HT 3A receptor, in which loop F instead translocates outward and the M2-M3 loop inward (Appendix Fig S5H), suggesting that apparent open states reported for 5-HT 3A may sample a divergent mechanism of gating [57]–[59].…”
Section: Discussionmentioning
confidence: 60%
“…Further rearrangement to the open state contracts both the β1-β2/M2 and F/M2-M3 clefts (Fig 5C, Appendix Fig S5A). The same pattern is evident in agonist-bound versus apo structures of ELIC, GluCl, glycine and nicotinic receptors (Appendix Fig S5B-E) [49]–[54], and in open/desensitized versus inhibitor-bound structures of DeCLIC and GABA A receptors (Appendix Fig S5F-G) [55], [56]. A noted exception is the 5-HT 3A receptor, in which loop F instead translocates outward and the M2-M3 loop inward (Appendix Fig S5H), suggesting that apparent open states reported for 5-HT 3A may sample a divergent mechanism of gating [57]–[59].…”
Section: Discussionmentioning
confidence: 60%
“…Three enzymes were selected for the construction of homology models: AChE, ACh, and Cht. The template enzymes were: AChE from Anopheles gambiae (PDB ID: 5YDH) [ 116 ], ACh from Homo sapiens (PDB ID: 6PV7) [ 117 ], and ChtII from Ostrinia furnicalis (PDB ID: 6JAV) [ 107 ]. The enzyme models were built using the molecular homology modeling method in the MODELLER 9.20 software [ 118 ].…”
Section: Methodsmentioning
confidence: 99%
“…To determine the effects of inter-subunit contacts between residues on the binding interfaces, we employed a network interaction analysis implemented in the software Cytoscape [57]. Differences in inter-subunit contacts help reveal changes in the relative orientations of the subunits at toxin-bound interfaces, which may be related to the capacity of the toxins to inhibit nAChR function [36,[58][59][60].…”
Section: Inter-subunit Contacts At the α3(+)β2(−) And β2(+)α3(−) Intementioning
confidence: 99%