It has recently been proposed that post-translational modification of not only the M3-M4 linker but also the M1-M2 linker of pentameric ligand-gated ion channels modulates function in vivo. To estimate the involvement of the M1-M2 linker in gating and desensitization, we engineered a series of mutations to this linker of the human adult-muscle acetylcholine receptor (AChR), the alpha 3 beta 4 AChR and the homomeric alpha 1 glycine receptor (GlyR). All tested M1-M2 linker mutations had little effect on the kinetics of deactivation or desensitization compared with the effects of mutations to the M2 alpha-helix or the extracellular M2-M3 linker. However, when the effects of mutations were assessed with 50 Hz trains of similar to 1ms pulses of saturating neurotransmitter, some mutations led to much more, and others to much less, peak-current depression than observed for the wild-type channels, suggesting that these mutations could affect the fidelity of fast synaptic transmission. Nevertheless, no mutation to this linker could mimic the irreversible loss of responsiveness reported to result from the oxidation of the M1-M2 linker cysteines of the alpha 3 AChR subunit. We also replaced the M3-M4 linker of the alpha 1 GlyR with much shorter peptides and found that none of these extensive changes affects channel deactivation strongly or reduces the marked variability in desensitization kinetics that characterizes the wild-type channel. However, we found that these large mutations to the M3-M4 linker can have pronounced effects on desensitization kinetics, supporting the notion that its post-translational modification could indeed modulate alpha 1 GlyR behavior.
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Inst Pasteur, Channel Receptors Unit, F-75015 Paris, France
CNRS, UMR 3571, F-75015 Paris, FranceInst Pasteur, Channel Receptors Unit, F-75015 Paris, France
Nemecz, Akos
Prevost, Marie S.
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Univ Coll London & Birkbeck, Inst Struct & Mol Biol, Malet St, London WC1E 7HX, EnglandInst Pasteur, Channel Receptors Unit, F-75015 Paris, France
Prevost, Marie S.
Menny, Anais
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Inst Pasteur, Channel Receptors Unit, F-75015 Paris, France
CNRS, UMR 3571, F-75015 Paris, France
Univ Paris 06, Cellule Pasteur, F-75005 Paris, FranceInst Pasteur, Channel Receptors Unit, F-75015 Paris, France
Menny, Anais
Corringer, Pierre-Jean
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Inst Pasteur, Channel Receptors Unit, F-75015 Paris, France
CNRS, UMR 3571, F-75015 Paris, FranceInst Pasteur, Channel Receptors Unit, F-75015 Paris, France
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Inst Pasteur, CNRS, UMR 3528, Unite Dynam Struct Macromol, F-75015 Paris, FranceInst Pasteur, CNRS, UMR 3528, Unite Dynam Struct Macromol, F-75015 Paris, France
Shahsavar, Azadeh
Delarue, Marc
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Inst Pasteur, CNRS, UMR 3528, Unite Dynam Struct Macromol, F-75015 Paris, FranceInst Pasteur, CNRS, UMR 3528, Unite Dynam Struct Macromol, F-75015 Paris, France
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Univ Pittsburgh, Dept Neurosci, Pittsburgh, PA 15260 USA
Univ Pittsburgh, Ctr Neurosci, Pittsburgh, PA 15260 USAUniv Pittsburgh, Dept Neurosci, Pittsburgh, PA 15260 USA
Phillips, Matthew B.
Nigam, Aparna
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Univ Pittsburgh, Dept Neurosci, Pittsburgh, PA 15260 USAUniv Pittsburgh, Dept Neurosci, Pittsburgh, PA 15260 USA
Nigam, Aparna
Johnson, Jon W.
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Univ Pittsburgh, Dept Neurosci, Pittsburgh, PA 15260 USA
Univ Pittsburgh, Ctr Neurosci, Pittsburgh, PA 15260 USAUniv Pittsburgh, Dept Neurosci, Pittsburgh, PA 15260 USA