9UC4 image
Deposition Date 2025-04-03
Release Date 2026-02-18
Last Version Date 2026-03-04
Entry Detail
PDB ID:
9UC4
Title:
Crystal structure of voltage-gated sodium channel NavAb N49K/S178T/T206A mutant
Biological Source:
Source Organism(s):
Expression System(s):
Method Details:
Experimental Method:
Resolution:
3.40 Å
R-Value Free:
0.31
R-Value Work:
0.27
R-Value Observed:
0.28
Space Group:
I 4 2 2
Macromolecular Entities
Structures with similar UniProt ID
Protein Blast
Polymer Type:polypeptide(L)
Molecule:Ion transport protein
Gene (Uniprot):Abu_1752
Mutagens:N49K, S178T, T206A
Chain IDs:A
Chain Length:271
Number of Molecules:1
Biological Source:Aliarcobacter butzleri
Primary Citation
Structure-function analysis of the lithium-ion selectivity of the voltage-gated sodium channel.
J. Gen. Physiol. 158 ? ? (2026)
PMID: 41711638 DOI: 10.1085/jgp.202513855

Abstact

Voltage-gated sodium channels (Navs) selectively conduct Na+ to generate action potentials. Na+ permeates Navs with significantly higher efficiency than many other cations, but Li+ can also permeate Navs to an extent comparable with Na+. Li+ in the blood is known to enter cells via Navs and to have a beneficial effect on various neuropathies. However, the molecular basis of the high Li+ selectivity of Navs was unclear. In this study, using a prokaryotic Nav, we successfully created the first Nav mutant to be more selective for Li+ than for Na+. Electrophysiological and crystallographic analyses suggested the critical determinants of high Li+ selectivity: the strong electrostatic interaction between the ion pathway and hydrated ions, and the smaller number of hydration water exchanges within the ion pathway. Additionally, the extensive interactions around the ion pathway were shown to support monovalent cation selectivity. New drug directions based on the molecular basis for Li+ permeation may target various neurological disorders and could clarify the broader biological effects of lithium.

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