Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation

BACKGROUND: ATP-sensitive potassium (K(ATP)) channels in neurons regulate excitability, neurotransmitter release and mediate protection from cell-death. Furthermore, activation of K(ATP )channels is suppressed in DRG neurons after painful-like nerve injury. NO-dependent mechanisms modulate both K(AT...

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Autores principales: Kawano, Takashi, Zoga, Vasiliki, Kimura, Masakazu, Liang, Mei-Ying, Wu, Hsiang-En, Gemes, Geza, McCallum, J Bruce, Kwok, Wai-Meng, Hogan, Quinn H, Sarantopoulos, Constantine D
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2009
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2673211/
https://www.ncbi.nlm.nih.gov/pubmed/19284878
http://dx.doi.org/10.1186/1744-8069-5-12
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author Kawano, Takashi
Zoga, Vasiliki
Kimura, Masakazu
Liang, Mei-Ying
Wu, Hsiang-En
Gemes, Geza
McCallum, J Bruce
Kwok, Wai-Meng
Hogan, Quinn H
Sarantopoulos, Constantine D
author_facet Kawano, Takashi
Zoga, Vasiliki
Kimura, Masakazu
Liang, Mei-Ying
Wu, Hsiang-En
Gemes, Geza
McCallum, J Bruce
Kwok, Wai-Meng
Hogan, Quinn H
Sarantopoulos, Constantine D
author_sort Kawano, Takashi
collection PubMed
description BACKGROUND: ATP-sensitive potassium (K(ATP)) channels in neurons regulate excitability, neurotransmitter release and mediate protection from cell-death. Furthermore, activation of K(ATP )channels is suppressed in DRG neurons after painful-like nerve injury. NO-dependent mechanisms modulate both K(ATP )channels and participate in the pathophysiology and pharmacology of neuropathic pain. Therefore, we investigated NO modulation of K(ATP )channels in control and axotomized DRG neurons. RESULTS: Cell-attached and cell-free recordings of K(ATP )currents in large DRG neurons from control rats (sham surgery, SS) revealed activation of K(ATP )channels by NO exogenously released by the NO donor SNAP, through decreased sensitivity to [ATP]i. This NO-induced K(ATP )channel activation was not altered in ganglia from animals that demonstrated sustained hyperalgesia-type response to nociceptive stimulation following spinal nerve ligation. However, baseline opening of K(ATP )channels and their activation induced by metabolic inhibition was suppressed by axotomy. Failure to block the NO-mediated amplification of K(ATP )currents with specific inhibitors of sGC and PKG indicated that the classical sGC/cGMP/PKG signaling pathway was not involved in the activation by SNAP. NO-induced activation of K(ATP )channels remained intact in cell-free patches, was reversed by DTT, a thiol-reducing agent, and prevented by NEM, a thiol-alkylating agent. Other findings indicated that the mechanisms by which NO activates K(ATP )channels involve direct S-nitrosylation of cysteine residues in the SUR1 subunit. Specifically, current through recombinant wild-type SUR1/Kir6.2 channels expressed in COS7 cells was activated by NO, but channels formed only from truncated isoform Kir6.2 subunits without SUR1 subunits were insensitive to NO. Further, mutagenesis of SUR1 indicated that NO-induced K(ATP )channel activation involves interaction of NO with residues in the NBD1 of the SUR1 subunit. CONCLUSION: NO activates K(ATP )channels in large DRG neurons via direct S-nitrosylation of cysteine residues in the SUR1 subunit. The capacity of NO to activate K(ATP )channels via this mechanism remains intact even after spinal nerve ligation, thus providing opportunities for selective pharmacological enhancement of K(ATP )current even after decrease of this current by painful-like nerve injury.
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spelling pubmed-26732112009-04-25 Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation Kawano, Takashi Zoga, Vasiliki Kimura, Masakazu Liang, Mei-Ying Wu, Hsiang-En Gemes, Geza McCallum, J Bruce Kwok, Wai-Meng Hogan, Quinn H Sarantopoulos, Constantine D Mol Pain Research BACKGROUND: ATP-sensitive potassium (K(ATP)) channels in neurons regulate excitability, neurotransmitter release and mediate protection from cell-death. Furthermore, activation of K(ATP )channels is suppressed in DRG neurons after painful-like nerve injury. NO-dependent mechanisms modulate both K(ATP )channels and participate in the pathophysiology and pharmacology of neuropathic pain. Therefore, we investigated NO modulation of K(ATP )channels in control and axotomized DRG neurons. RESULTS: Cell-attached and cell-free recordings of K(ATP )currents in large DRG neurons from control rats (sham surgery, SS) revealed activation of K(ATP )channels by NO exogenously released by the NO donor SNAP, through decreased sensitivity to [ATP]i. This NO-induced K(ATP )channel activation was not altered in ganglia from animals that demonstrated sustained hyperalgesia-type response to nociceptive stimulation following spinal nerve ligation. However, baseline opening of K(ATP )channels and their activation induced by metabolic inhibition was suppressed by axotomy. Failure to block the NO-mediated amplification of K(ATP )currents with specific inhibitors of sGC and PKG indicated that the classical sGC/cGMP/PKG signaling pathway was not involved in the activation by SNAP. NO-induced activation of K(ATP )channels remained intact in cell-free patches, was reversed by DTT, a thiol-reducing agent, and prevented by NEM, a thiol-alkylating agent. Other findings indicated that the mechanisms by which NO activates K(ATP )channels involve direct S-nitrosylation of cysteine residues in the SUR1 subunit. Specifically, current through recombinant wild-type SUR1/Kir6.2 channels expressed in COS7 cells was activated by NO, but channels formed only from truncated isoform Kir6.2 subunits without SUR1 subunits were insensitive to NO. Further, mutagenesis of SUR1 indicated that NO-induced K(ATP )channel activation involves interaction of NO with residues in the NBD1 of the SUR1 subunit. CONCLUSION: NO activates K(ATP )channels in large DRG neurons via direct S-nitrosylation of cysteine residues in the SUR1 subunit. The capacity of NO to activate K(ATP )channels via this mechanism remains intact even after spinal nerve ligation, thus providing opportunities for selective pharmacological enhancement of K(ATP )current even after decrease of this current by painful-like nerve injury. BioMed Central 2009-03-14 /pmc/articles/PMC2673211/ /pubmed/19284878 http://dx.doi.org/10.1186/1744-8069-5-12 Text en Copyright © 2009 Kawano et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Kawano, Takashi
Zoga, Vasiliki
Kimura, Masakazu
Liang, Mei-Ying
Wu, Hsiang-En
Gemes, Geza
McCallum, J Bruce
Kwok, Wai-Meng
Hogan, Quinn H
Sarantopoulos, Constantine D
Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation
title Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation
title_full Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation
title_fullStr Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation
title_full_unstemmed Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation
title_short Nitric oxide activates ATP-sensitive potassium channels in mammalian sensory neurons: action by direct S-nitrosylation
title_sort nitric oxide activates atp-sensitive potassium channels in mammalian sensory neurons: action by direct s-nitrosylation
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2673211/
https://www.ncbi.nlm.nih.gov/pubmed/19284878
http://dx.doi.org/10.1186/1744-8069-5-12
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