Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7

BACKGROUND: Sodium channel Na(V)1.7 is preferentially expressed within dorsal root ganglia (DRG), trigeminal ganglia and sympathetic ganglion neurons and their fine-diamter axons, where it acts as a threshold channel, amplifying stimuli such as generator potentials in nociceptors. Gain-of-function m...

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Autores principales: Estacion, Mark, Han, Chongyang, Choi, Jin-Sung, Hoeijmakers, Janneke GJ, Lauria, Giuseppe, Drenth, Joost PH, Gerrits, Monique M, Dib-Hajj, Sulayman D, Faber, Catharina G, Merkies, Ingemar SJ, Waxman, Stephen G
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3248882/
https://www.ncbi.nlm.nih.gov/pubmed/22136189
http://dx.doi.org/10.1186/1744-8069-7-92
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author Estacion, Mark
Han, Chongyang
Choi, Jin-Sung
Hoeijmakers, Janneke GJ
Lauria, Giuseppe
Drenth, Joost PH
Gerrits, Monique M
Dib-Hajj, Sulayman D
Faber, Catharina G
Merkies, Ingemar SJ
Waxman, Stephen G
author_facet Estacion, Mark
Han, Chongyang
Choi, Jin-Sung
Hoeijmakers, Janneke GJ
Lauria, Giuseppe
Drenth, Joost PH
Gerrits, Monique M
Dib-Hajj, Sulayman D
Faber, Catharina G
Merkies, Ingemar SJ
Waxman, Stephen G
author_sort Estacion, Mark
collection PubMed
description BACKGROUND: Sodium channel Na(V)1.7 is preferentially expressed within dorsal root ganglia (DRG), trigeminal ganglia and sympathetic ganglion neurons and their fine-diamter axons, where it acts as a threshold channel, amplifying stimuli such as generator potentials in nociceptors. Gain-of-function mutations and variants (single amino acid substitutions) of Na(V)1.7 have been linked to three pain syndromes: Inherited Erythromelalgia (IEM), Paroxysmal Extreme Pain Disorder (PEPD), and Small Fiber Neuropathy (SFN). IEM is characterized clinically by burning pain and redness that is usually focused on the distal extremities, precipitated by mild warmth and relieved by cooling, and is caused by mutations that hyperpolarize activation, slow deactivation, and enhance the channel ramp response. PEPD is characterized by perirectal, periocular or perimandibular pain, often triggered by defecation or lower body stimulation, and is caused by mutations that severely impair fast-inactivation. SFN presents a clinical picture dominated by neuropathic pain and autonomic symptoms; gain-of-function variants have been reported to be present in approximately 30% of patients with biopsy-confirmed idiopathic SFN, and functional testing has shown altered fast-inactivation, slow-inactivation or resurgent current. In this paper we describe three patients who house the Na(V)1.7/I228M variant. METHODS: We have used clinical assessment of patients, quantitative sensory testing and skin biopsy to study these patients, including two siblings in one family, in whom genomic screening demonstrated the I228M Na(V)1.7 variant. Electrophysiology (voltage-clamp and current-clamp) was used to test functional effects of the variant channel. RESULTS: We report three different clinical presentations of the I228M Na(V)1.7 variant: presentation with severe facial pain, presentation with distal (feet, hands) pain, and presentation with scalp discomfort in three patients housing this Na(V)1.7 variant, two of which are from a single family. We also demonstrate that the Na(V)1.7/I228M variant impairs slow-inactivation, and produces hyperexcitability in both trigeminal ganglion and DRG neurons. CONCLUSION: Our results demonstrate intra- and interfamily phenotypic diversity in pain syndromes produced by a gain-of-function variant of Na(V)1.7.
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spelling pubmed-32488822011-12-31 Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7 Estacion, Mark Han, Chongyang Choi, Jin-Sung Hoeijmakers, Janneke GJ Lauria, Giuseppe Drenth, Joost PH Gerrits, Monique M Dib-Hajj, Sulayman D Faber, Catharina G Merkies, Ingemar SJ Waxman, Stephen G Mol Pain Research BACKGROUND: Sodium channel Na(V)1.7 is preferentially expressed within dorsal root ganglia (DRG), trigeminal ganglia and sympathetic ganglion neurons and their fine-diamter axons, where it acts as a threshold channel, amplifying stimuli such as generator potentials in nociceptors. Gain-of-function mutations and variants (single amino acid substitutions) of Na(V)1.7 have been linked to three pain syndromes: Inherited Erythromelalgia (IEM), Paroxysmal Extreme Pain Disorder (PEPD), and Small Fiber Neuropathy (SFN). IEM is characterized clinically by burning pain and redness that is usually focused on the distal extremities, precipitated by mild warmth and relieved by cooling, and is caused by mutations that hyperpolarize activation, slow deactivation, and enhance the channel ramp response. PEPD is characterized by perirectal, periocular or perimandibular pain, often triggered by defecation or lower body stimulation, and is caused by mutations that severely impair fast-inactivation. SFN presents a clinical picture dominated by neuropathic pain and autonomic symptoms; gain-of-function variants have been reported to be present in approximately 30% of patients with biopsy-confirmed idiopathic SFN, and functional testing has shown altered fast-inactivation, slow-inactivation or resurgent current. In this paper we describe three patients who house the Na(V)1.7/I228M variant. METHODS: We have used clinical assessment of patients, quantitative sensory testing and skin biopsy to study these patients, including two siblings in one family, in whom genomic screening demonstrated the I228M Na(V)1.7 variant. Electrophysiology (voltage-clamp and current-clamp) was used to test functional effects of the variant channel. RESULTS: We report three different clinical presentations of the I228M Na(V)1.7 variant: presentation with severe facial pain, presentation with distal (feet, hands) pain, and presentation with scalp discomfort in three patients housing this Na(V)1.7 variant, two of which are from a single family. We also demonstrate that the Na(V)1.7/I228M variant impairs slow-inactivation, and produces hyperexcitability in both trigeminal ganglion and DRG neurons. CONCLUSION: Our results demonstrate intra- and interfamily phenotypic diversity in pain syndromes produced by a gain-of-function variant of Na(V)1.7. BioMed Central 2011-12-02 /pmc/articles/PMC3248882/ /pubmed/22136189 http://dx.doi.org/10.1186/1744-8069-7-92 Text en Copyright ©2011 Estacion 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
Estacion, Mark
Han, Chongyang
Choi, Jin-Sung
Hoeijmakers, Janneke GJ
Lauria, Giuseppe
Drenth, Joost PH
Gerrits, Monique M
Dib-Hajj, Sulayman D
Faber, Catharina G
Merkies, Ingemar SJ
Waxman, Stephen G
Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7
title Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7
title_full Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7
title_fullStr Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7
title_full_unstemmed Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7
title_short Intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of Na(V)1.7
title_sort intra- and interfamily phenotypic diversity in pain syndromes associated with a gain-of-function variant of na(v)1.7
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3248882/
https://www.ncbi.nlm.nih.gov/pubmed/22136189
http://dx.doi.org/10.1186/1744-8069-7-92
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