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Conformational plasticity of NaK2K and TREK2 potassium channel selectivity filters.


ABSTRACT: The K+ channel selectivity filter (SF) is defined by TxGYG amino acid sequences that generate four identical K+ binding sites (S1-S4). Only two sites (S3, S4) are present in the non-selective bacterial NaK channel, but a four-site K+-selective SF is obtained by mutating the wild-type TVGDGN SF sequence to a canonical K+ channel TVGYGD sequence (NaK2K mutant). Using single molecule FRET (smFRET), we show that the SF of NaK2K, but not of non-selective NaK, is ion-dependent, with the constricted SF configuration stabilized in high K+ conditions. Patch-clamp electrophysiology and non-canonical fluorescent amino acid incorporation show that NaK2K selectivity is reduced by crosslinking to limit SF conformational movement. Finally, the eukaryotic K+ channel TREK2 SF exhibits essentially identical smFRET-reported ion-dependent conformations as in prokaryotic K+ channels. Our results establish the generality of K+-induced SF conformational stability across the K+ channel superfamily, and introduce an approach to study manipulation of channel selectivity.

SUBMITTER: Matamoros M 

PROVIDER: S-EPMC9822992 | biostudies-literature | 2023 Jan

REPOSITORIES: biostudies-literature

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Conformational plasticity of NaK2K and TREK2 potassium channel selectivity filters.

Matamoros Marcos M   Ng Xue Wen XW   Brettmann Joshua B JB   Piston David W DW   Nichols Colin G CG  

Nature communications 20230106 1


The K<sup>+</sup> channel selectivity filter (SF) is defined by TxGYG amino acid sequences that generate four identical K<sup>+</sup> binding sites (S1-S4). Only two sites (S3, S4) are present in the non-selective bacterial NaK channel, but a four-site K<sup>+</sup>-selective SF is obtained by mutating the wild-type TVGDGN SF sequence to a canonical K<sup>+</sup> channel TVGYGD sequence (NaK2K mutant). Using single molecule FRET (smFRET), we show that the SF of NaK2K, but not of non-selective Na  ...[more]

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