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P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels

HCN channels are thought to be structurally similar to K(v) channels, but show much lower selectivity for K(+). The ∼3.3 Å selectivity filter of K(+) channels is formed by the pore-lining sequence XT(V/I)GYG, with X usually T, and is held stable by key residues in the P-loop. Differences in the P-lo...

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Autores principales: D'Avanzo, Nazzareno, Pekhletski, Roman, Backx, Peter H.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2766643/
https://www.ncbi.nlm.nih.gov/pubmed/19890386
http://dx.doi.org/10.1371/journal.pone.0007712
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author D'Avanzo, Nazzareno
Pekhletski, Roman
Backx, Peter H.
author_facet D'Avanzo, Nazzareno
Pekhletski, Roman
Backx, Peter H.
author_sort D'Avanzo, Nazzareno
collection PubMed
description HCN channels are thought to be structurally similar to K(v) channels, but show much lower selectivity for K(+). The ∼3.3 Å selectivity filter of K(+) channels is formed by the pore-lining sequence XT(V/I)GYG, with X usually T, and is held stable by key residues in the P-loop. Differences in the P-loop sequence of HCN channels (eg. the pore-lining sequence L(478)C(479)IGYG) suggest these residues could account for differences in selectivity between these channel families. Despite being expressed, L478T/C479T HCN4 channels did not produce current. Since threonine in the second position is highly conserved in K(+) channels, we also studied C479T channels. Based on permeability ratios (P(X)/P(K)), C479T HCN4 channels (K(+)(1)>Rb(+)(0.85)>Cs(+)(0.59)>Li(+)(0.50)≥Na(+)(0.49)) were less selective than WT rabbit HCN4 (K(+)(1)>Rb(+)(0.48)>Cs(+)(0.31)≥Na(+)(0.29)>Li(+)(0.03)), indicating that the TIGYG sequence is insufficient to confer K(+) selectivity to HCN channels. C479T HCN4 channels had an increased permeability to large organic cations than WT HCN4 channels, as well as increased unitary K(+) conductance, and altered channel gating. Collectively, these results suggest that HCN4 channels have larger pores than K(+) channels and replacement of the cysteine at position 479 with threonine further increases pore size. Furthermore, selected mutations in other regions linked previously to pore stability in K(+) channels (ie. S475D, S475E and F471W/K472W) were also unable to confer K(+) selectivity to C479T HCN4 channels. Our findings establish the presence of the TIGYG pore-lining sequence does not confer K(+) selectivity to rabbit HCN4 channels, and suggests that differences in selectivity of HCN4 versus K(+) channels originate from differences outside the P-loop region.
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spelling pubmed-27666432009-11-05 P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels D'Avanzo, Nazzareno Pekhletski, Roman Backx, Peter H. PLoS One Research Article HCN channels are thought to be structurally similar to K(v) channels, but show much lower selectivity for K(+). The ∼3.3 Å selectivity filter of K(+) channels is formed by the pore-lining sequence XT(V/I)GYG, with X usually T, and is held stable by key residues in the P-loop. Differences in the P-loop sequence of HCN channels (eg. the pore-lining sequence L(478)C(479)IGYG) suggest these residues could account for differences in selectivity between these channel families. Despite being expressed, L478T/C479T HCN4 channels did not produce current. Since threonine in the second position is highly conserved in K(+) channels, we also studied C479T channels. Based on permeability ratios (P(X)/P(K)), C479T HCN4 channels (K(+)(1)>Rb(+)(0.85)>Cs(+)(0.59)>Li(+)(0.50)≥Na(+)(0.49)) were less selective than WT rabbit HCN4 (K(+)(1)>Rb(+)(0.48)>Cs(+)(0.31)≥Na(+)(0.29)>Li(+)(0.03)), indicating that the TIGYG sequence is insufficient to confer K(+) selectivity to HCN channels. C479T HCN4 channels had an increased permeability to large organic cations than WT HCN4 channels, as well as increased unitary K(+) conductance, and altered channel gating. Collectively, these results suggest that HCN4 channels have larger pores than K(+) channels and replacement of the cysteine at position 479 with threonine further increases pore size. Furthermore, selected mutations in other regions linked previously to pore stability in K(+) channels (ie. S475D, S475E and F471W/K472W) were also unable to confer K(+) selectivity to C479T HCN4 channels. Our findings establish the presence of the TIGYG pore-lining sequence does not confer K(+) selectivity to rabbit HCN4 channels, and suggests that differences in selectivity of HCN4 versus K(+) channels originate from differences outside the P-loop region. Public Library of Science 2009-11-05 /pmc/articles/PMC2766643/ /pubmed/19890386 http://dx.doi.org/10.1371/journal.pone.0007712 Text en D'Avanzo et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
D'Avanzo, Nazzareno
Pekhletski, Roman
Backx, Peter H.
P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels
title P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels
title_full P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels
title_fullStr P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels
title_full_unstemmed P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels
title_short P-Loop Residues Critical for Selectivity in K(+) Channels Fail to Confer Selectivity to Rabbit HCN4 Channels
title_sort p-loop residues critical for selectivity in k(+) channels fail to confer selectivity to rabbit hcn4 channels
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2766643/
https://www.ncbi.nlm.nih.gov/pubmed/19890386
http://dx.doi.org/10.1371/journal.pone.0007712
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