Modulation of the Erwinia ligand-gated ion channel (ELIC) and the 5-HT3 receptor via a common vestibule site

Brams, Marijke; Govaerts, Cédric; Kambara, Kumiko; Price, Kerry L.; Spurný, Radovan; Gharpure, Anant; Pardon, Els; Evans, G.L.; Bertrand, Daniel; Lummis, Sarah S.C.R.; Hibbs, Ryan; Steyaert, Jan; Ulens, Chris

doi:10.7554/elife.51511

Cited by 21 publications

(45 citation statements)

References 66 publications

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“…The first, an exterior site just below the orthosteric pocket, structurally resolved on GABA A [28, 29] and a nAChR [30] and the second, an exterior binding site directly overlapping and slightly above that of α-Btx, found with the 5-HT 3 receptor [20]. A third site on the complementary subunit to the right of and slightly above the orthosteric pocket, visualized on ELIC [22] and GABA A [31] respectively, is likely occluded in the α7-nAChR due to a unique glycosylation site. This site in the prokaryotic ELIC was found to have PAM effects.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, nanobodies have a number of advantages over small molecules, notably: they usually have a high affinity, typically in the nanomolar range, as well as a high specificity conferred by the large surface of the nanobody-antigen interaction. As an example: within the pentameric ligand-gated ion channel family, nanobodies acting as PAMs and NAMs were reported on the serotonin type 3 (5-HT 3 ) receptor [20], the GABA A receptor [21], and the bacterial ELIC [22]. The generation and functional characterization of two nanobodies specifically targeting the α7-nAChR is presented herein.…”

Section: Introductionmentioning

confidence: 99%

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Generation of nanobodies acting as silent and positive allosteric modulators of the α7 nicotinic acetylcholine receptor

Nemecz

Aymé

et al. 2023

Preprint

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The α7 nicotinic acetylcholine receptor (nAChR), a potential drug target for treating cognitive disorders, mediates communication between neuronal and non-neuronal cells. Although many competitive antagonists, agonists, and partial-agonists have been found and synthesized, they have not led to effective therapeutic treatments. In this context, small molecules acting as positive allosteric modulators binding outside the orthosteric, acetylcholine, site have attracted considerable interest. Two single-domain antibody fragments, C4 and E3, generated through alpaca immunization with cells expressing the extracellular domain of the human α7-nAChR, are herein described. They bind to the α7-nAChR but not to the other major nAChR subtypes, α4β2 and α3β4. E3 acts as a slowly associating type I positive allosteric modulator, strongly potentiating the acetylcholine-elicited currents, while not significantly altering the desensitization of the receptor. An E3-E3 bivalent construct shows similar potentiating properties but displays very slow dissociation kinetics conferring quasi-irreversible properties. Whereas, C4 does not alter the receptor function, but fully inhibits the E3-evoked potentiation, showing it is a silent allosteric modulator competing with E3 binding. Both nanobodies do not compete with α-bungarotoxin, localizing at an allosteric extracellular binding site away from the orthosteric site. The functional differences of each nanobody, as well as the alteration of functional properties through nanobody modifications indicate the importance of this extracellular site. The nanobodies will be useful for pharmacological and structural investigations; moreover, they, along with the extracellular site, have a direct potential for clinical applications.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Generation of nanobodies acting as silent and positive allosteric modulators of the α7 nicotinic acetylcholine receptor

Nemecz

Aymé

et al. 2023

Preprint

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“…In the pLGIC family, nanobodies were previously generated and used mainly to assist structural determination. Most bind at the ortho- or pseudo-ortho-steric site in the 5HT 3 R 20 , GABA A R 21,22 and prokaryotic homolog ELIC 23 , except for a single NAM nanobody binding in the vestibule of ELIC 23 . It is noteworthy that E3 and C4 were generated through immunization of alpacas with cells expressing the fully glycosylated α7-nAChR ECD, while previous nanobodies involved immunization with purified proteins partly depleted from N-linked glycosylation by enzymatic cleavage (5HT 3 R) or production in GntI-cells (GABA A R).…”

Section: Discussionmentioning

confidence: 99%

An original potentiating mechanism revealed by the cryoEM structures of the human α7 nicotinic receptor in complex with nanobodies

Prevost

Barilone

Bâtie

et al. 2023

Preprint

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The human α7 nicotinic receptor is a pentameric channel mediating cellular and neuronal communication. It has attracted considerable interest to design ligands for the treatment of neurological and psychiatric disorders. To develop a novel class of α7 ligands, we recently generated two nanobodies named E3 and C4 acting as positive and silent allosteric modulators respectively. Here, we solved the cryo-EM structures of the nanobody-receptor complexes. E3 and C4 bind to a common epitope involving two subunits at the apex of the receptor. They form by themselves a symmetric pentameric assembly that extends the extracellular domain. Unlike C4, the binding of E3 drives an active or desensitized conformation in the absence of orthosteric agonist, and mutational analysis shows a key contribution of a N-linked sugar moiety in mediating E3 potentiation. The nanobody E3, by remotely controlling the global allosteric conformation of the receptor, implements an original mechanism of regulation which opens new avenues for drug design.

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“…Second, amino acid substitutions at the position corresponding to K104 in GlyR-1 with residues that annihilate (23) or revert the charge (21,22) strongly affect the unitary conductance in both anionic and cationic pLGICs [i.e., -aminobutyric acid type A receptor (GABA A R) K105, 5-HT 3 R D132, and muscle nAChR D97] without altering the charge selectivity (39). Third, lateral fenestrations have been already detected in GABA A R (40,41), 5HT 3 R (42), STeLIC (endosymbiont of Tevnia jerichonana pentameric ligand gated ion channel) (43), and ELIC (Erwinia chrysanthemi pentameric ligand gated ion channel) (44), and these observations are now extended to a larger set of pLGICs (table S8). Fourth, the existence of lateral fenestrations for ion conductance appears to overcome the problem of glycans in recent cryo-EM structures of GlyR 2 (45) and GABAR 112 (46) or 132 (47), where sugar moieties located at the apex of the receptor clearly hinder and possibly occlude the apical pathway.…”

Section: Discussionmentioning

confidence: 99%

Lateral fenestrations in the extracellular domain of the glycine receptor contribute to the main chloride permeation pathway

et al. 2022

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Glycine receptors (GlyRs) are ligand-gated ion channels mediating signal transduction at chemical synapses. Since the early patch-clamp electrophysiology studies, the details of the ion permeation mechanism have remained elusive. Here, we combine molecular dynamics simulations of a zebrafish GlyR-α1 model devoid of the intracellular domain with mutagenesis and single-channel electrophysiology of the full-length human GlyR-α1. We show that lateral fenestrations between subunits in the extracellular domain provide the main translocation pathway for chloride ions to enter/exit a central water-filled vestibule at the entrance of the transmembrane channel. In addition, we provide evidence that these fenestrations are at the origin of current rectification in known anomalous mutants and design de novo two inward-rectifying channels by introducing mutations within them. These results demonstrate the central role of lateral fenestrations on synaptic neurotransmission.

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Modulation of the Erwinia ligand-gated ion channel (ELIC) and the 5-HT3 receptor via a common vestibule site

Cited by 21 publications

References 66 publications

Generation of nanobodies acting as silent and positive allosteric modulators of the α7 nicotinic acetylcholine receptor

Generation of nanobodies acting as silent and positive allosteric modulators of the α7 nicotinic acetylcholine receptor

An original potentiating mechanism revealed by the cryoEM structures of the human α7 nicotinic receptor in complex with nanobodies

Lateral fenestrations in the extracellular domain of the glycine receptor contribute to the main chloride permeation pathway

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