The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)

The α2 glycine receptor (GlyR) subunit, abundant in embryonic neurons, is replaced by α1 in the adult nervous system. The single-channel activity of homomeric α2 channels differs from that of α1-containing GlyRs, as even at the lowest glycine concentration (20 µM), openings occurred in long (>300...

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Autores principales: Krashia, Paraskevi, Lape, Remigijus, Lodesani, Francesco, Colquhoun, David, Sivilotti, Lucia G.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2011
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3032374/
https://www.ncbi.nlm.nih.gov/pubmed/21282399
http://dx.doi.org/10.1085/jgp.201010521
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author Krashia, Paraskevi
Lape, Remigijus
Lodesani, Francesco
Colquhoun, David
Sivilotti, Lucia G.
author_facet Krashia, Paraskevi
Lape, Remigijus
Lodesani, Francesco
Colquhoun, David
Sivilotti, Lucia G.
author_sort Krashia, Paraskevi
collection PubMed
description The α2 glycine receptor (GlyR) subunit, abundant in embryonic neurons, is replaced by α1 in the adult nervous system. The single-channel activity of homomeric α2 channels differs from that of α1-containing GlyRs, as even at the lowest glycine concentration (20 µM), openings occurred in long (>300-ms) groups with high open probability (P(open); 0.96; cell-attached recordings, HEK-expressed channels). Shut-time intervals within groups of openings were dominated by short shuttings of 5–10 µs. The lack of concentration dependence in the groups of openings suggests that they represent single activations, separated by very long shut times at low concentrations. Several putative mechanisms were fitted by maximizing the likelihood of the entire sequence of open and shut times, with exact missed-events allowance (program hjcfit). Records obtained at several glycine concentrations were fitted simultaneously. The adequacy of the different schemes was judged by the accuracy with which they predicted not only single-channel data but also the time course and concentration dependence of macroscopic responses elicited by rapid glycine applications to outside-out patches. The data were adequately described only with schemes incorporating a reaction intermediate in the activation, and the best was a flip mechanism with two binding sites and one open state. Fits with this mechanism showed that for α2 channels, the opening rate constant is very fast, ∼130,000 s(−1), much as for α1β GlyRs (the receptor in mature synapses), but the estimated true mean open time is 20 times longer (around 3 ms). The efficacy for the flipping step and the binding affinity were lower for α2 than for α1β channels, but the overall efficacies were similar. As we previously showed for α1 homomeric receptors, in α2 glycine channels, maximum P(open) is achieved when fewer than all five of the putative binding sites in the pentamer are occupied by glycine.
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spelling pubmed-30323742011-08-01 The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”) Krashia, Paraskevi Lape, Remigijus Lodesani, Francesco Colquhoun, David Sivilotti, Lucia G. J Gen Physiol Article The α2 glycine receptor (GlyR) subunit, abundant in embryonic neurons, is replaced by α1 in the adult nervous system. The single-channel activity of homomeric α2 channels differs from that of α1-containing GlyRs, as even at the lowest glycine concentration (20 µM), openings occurred in long (>300-ms) groups with high open probability (P(open); 0.96; cell-attached recordings, HEK-expressed channels). Shut-time intervals within groups of openings were dominated by short shuttings of 5–10 µs. The lack of concentration dependence in the groups of openings suggests that they represent single activations, separated by very long shut times at low concentrations. Several putative mechanisms were fitted by maximizing the likelihood of the entire sequence of open and shut times, with exact missed-events allowance (program hjcfit). Records obtained at several glycine concentrations were fitted simultaneously. The adequacy of the different schemes was judged by the accuracy with which they predicted not only single-channel data but also the time course and concentration dependence of macroscopic responses elicited by rapid glycine applications to outside-out patches. The data were adequately described only with schemes incorporating a reaction intermediate in the activation, and the best was a flip mechanism with two binding sites and one open state. Fits with this mechanism showed that for α2 channels, the opening rate constant is very fast, ∼130,000 s(−1), much as for α1β GlyRs (the receptor in mature synapses), but the estimated true mean open time is 20 times longer (around 3 ms). The efficacy for the flipping step and the binding affinity were lower for α2 than for α1β channels, but the overall efficacies were similar. As we previously showed for α1 homomeric receptors, in α2 glycine channels, maximum P(open) is achieved when fewer than all five of the putative binding sites in the pentamer are occupied by glycine. The Rockefeller University Press 2011-02 /pmc/articles/PMC3032374/ /pubmed/21282399 http://dx.doi.org/10.1085/jgp.201010521 Text en © 2011 Krashia et al. This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 3.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/3.0/).
spellingShingle Article
Krashia, Paraskevi
Lape, Remigijus
Lodesani, Francesco
Colquhoun, David
Sivilotti, Lucia G.
The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)
title The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)
title_full The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)
title_fullStr The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)
title_full_unstemmed The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)
title_short The long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)
title_sort long activations of α2 glycine channels can be described by a mechanism with reaction intermediates (“flip”)
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3032374/
https://www.ncbi.nlm.nih.gov/pubmed/21282399
http://dx.doi.org/10.1085/jgp.201010521
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