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<title>
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Entry
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- #613345 - HYPOKALEMIC PERIODIC PARALYSIS, TYPE 2; HOKPP2
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- OMIM
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<span class="h4">#613345</span>
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<a href="#phenotypeMap"><strong>Phenotype-Gene Relationships</strong></a>
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<a href="/clinicalSynopsis/613345"><strong>Clinical Synopsis</strong></a>
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<a href="#clinicalFeatures">Clinical Features</a>
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<a href="#molecularGenetics">Molecular Genetics</a>
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<a href="#pathogenesis">Pathogenesis</a>
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<a href="#references"><strong>References</strong></a>
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<a href="#creationDate"><strong>Creation Date</strong></a>
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<div><a href="https://clinicaltrials.gov/search?cond=(HYPOKALEMIC PERIODIC PARALYSIS, TYPE) OR (SCN4A)" class="mim-tip-hint" title="Clinical Trials" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'Clinical Trials', 'domain': 'clinicaltrials.gov'})">Clinical Trials</a></div>
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<div><a href="https://www.orpha.net/consor/cgi-bin/ClinicalLabs_Search_Simple.php?lng=EN&LnkId=211&Typ=Pat" class="mim-tip-hint" title="A list of European laboratories that offer genetic testing." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'EuroGentest', 'domain': 'orpha.net'})">EuroGentest</a></div>
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<div><a href="https://www.diseaseinfosearch.org/x/8612" class="mim-tip-hint" title="Network of disease-specific advocacy organizations, universities, private companies, government agencies, and public policy organizations." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'Genetic Alliance', 'domain': 'diseaseinfosearch.org'})">Genetic Alliance</a></div>
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<div><a href="https://medlineplus.gov/genetics/condition/hypokalemic-periodic-paralysis" class="mim-tip-hint" title="Consumer-friendly information about the effects of genetic variation on human health." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'MedlinePlus Genetics', 'domain': 'medlineplus.gov'})">MedlinePlus Genetics</a></div>
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<div><a href="https://www.ncbi.nlm.nih.gov/gtr/all/tests/?term=613345[mim]" class="mim-tip-hint" title="Genetic Testing Registry." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'GTR', 'domain': 'ncbi.nlm.nih.gov'})">GTR</a></div>
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<div><a href="https://www.orpha.net/consor/cgi-bin/OC_Exp.php?lng=EN&Expert=681" class="mim-tip-hint" title="European reference portal for information on rare diseases and orphan drugs." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'OrphaNet', 'domain': 'orpha.net'})">OrphaNet</a></div>
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<div><a href="https://www.alliancegenome.org/disease/DOID:14452" class="mim-tip-hint" title="Search Across Species; explore model organism and human comparative genomics." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'Alliance Genome', 'domain': 'alliancegenome.org'})">Alliance Genome</a></div>
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<div><a href="http://www.informatics.jax.org/disease/613345" class="mim-tip-hint" title="Phenotypes, alleles, and disease models from Mouse Genome Informatics." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'MGI Mouse Phenotype', 'domain': 'informatics.jax.org'})">MGI Mouse Phenotype</a></div>
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<div><a href="https://omia.org/OMIA000785/" class="mim-tip-hint" title="Online Mendelian Inheritance in Animals (OMIA) is a database of genes, inherited disorders and traits in 191 animal species (other than human and mouse.)" target="_blank">OMIA</a></div>
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<div><a href="https://wormbase.org/resources/disease/DOID:14452" class="mim-tip-hint" title="Database of the biology and genome of Caenorhabditis elegans and related nematodes." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'Wormbase Disease Ontology', 'domain': 'wormbase.org'})">Wormbase Disease Ontology</a></div>
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<span>
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<span class="mim-tip-bottom" qtip_title="<strong>Looking for this gene or this phenotype in other resources?</strong>" qtip_text="Select a related resource from the dropdown menu and click for a targeted link to information directly relevant.">
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<a id="title" class="mim-anchor"></a>
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<a id="number" class="mim-anchor"></a>
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<div class="text-right">
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<a href="#" class="mim-tip-icd" qtip_title="<strong>ICD+</strong>" qtip_text="
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<strong>ORPHA:</strong> 681<br />
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<strong>DO:</strong> 14452<br />
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">ICD+</a>
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<div>
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<span class="h3">
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<span class="mim-font mim-tip-hint" title="Phenotype description, molecular basis known">
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<span class="text-danger"><strong>#</strong></span>
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613345
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</span>
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</span>
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</div>
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</div>
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<div>
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<a id="preferredTitle" class="mim-anchor"></a>
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<h3>
|
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<span class="mim-font">
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HYPOKALEMIC PERIODIC PARALYSIS, TYPE 2; HOKPP2
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</span>
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</h3>
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</div>
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<div>
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<br />
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</div>
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<a id="phenotypeMap" class="mim-anchor"></a>
|
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<h4>
|
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<span class="mim-font">
|
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<strong>Phenotype-Gene Relationships</strong>
|
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</span>
|
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</h4>
|
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<div>
|
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<table class="table table-bordered table-condensed table-hover small mim-table-padding">
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<thead>
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<tr class="active">
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<th>
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Location
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</th>
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<th>
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Phenotype
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</th>
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<th>
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Phenotype <br /> MIM number
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Inheritance
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Phenotype <br /> mapping key
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Gene/Locus
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Gene/Locus <br /> MIM number
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<tbody>
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<span class="mim-font">
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<a href="/geneMap/17/852?start=-3&limit=10&highlight=852">
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17q23.3
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</a>
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</span>
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</td>
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<td>
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<span class="mim-font">
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Hypokalemic periodic paralysis, type 2
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</span>
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</td>
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<td>
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<span class="mim-font">
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<a href="/entry/613345"> 613345 </a>
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</span>
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</td>
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<td>
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<span class="mim-font">
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<abbr class="mim-tip-hint" title="Autosomal dominant">AD</abbr>
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</span>
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</td>
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<td>
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<span class="mim-font">
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<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
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</span>
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</td>
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<td>
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<span class="mim-font">
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SCN4A
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</span>
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</td>
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<td>
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<span class="mim-font">
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<a href="/entry/603967"> 603967 </a>
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</span>
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</td>
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</tr>
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</tbody>
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</table>
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<div>
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<div class="btn-group ">
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<a href="/clinicalSynopsis/613345" class="btn btn-warning" role="button"> Clinical Synopsis </a>
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<button type="button" id="mimPhenotypicSeriesToggle" class="btn btn-warning dropdown-toggle mimSingletonFoldToggle" data-toggle="collapse" href="#mimClinicalSynopsisFold" onclick="ga('send', 'event', 'Unfurl', 'ClinicalSynopsis', 'omim.org')">
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<span class="caret"></span>
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<span class="sr-only">Toggle Dropdown</span>
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</button>
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<div class="btn-group">
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<button type="button" class="btn btn-success dropdown-toggle" data-toggle="dropdown" aria-haspopup="true" aria-expanded="false">
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PheneGene Graphics <span class="caret"></span>
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</button>
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<ul class="dropdown-menu" style="width: 17em;">
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<li><a href="/graph/linear/613345" target="_blank" onclick="gtag('event', 'mim_graph', {'destination': 'Linear'})"> Linear </a></li>
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<li><a href="/graph/radial/613345" target="_blank" onclick="gtag('event', 'mim_graph', {'destination': 'Radial'})"> Radial </a></li>
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</ul>
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</div>
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<span class="glyphicon glyphicon-question-sign mim-tip-hint" title="OMIM PheneGene graphics depict relationships between phenotypes, groups of related phenotypes (Phenotypic Series), and genes.<br /><a href='/static/omim/pdf/OMIM_Graphics.pdf' target='_blank'>A quick reference overview and guide (PDF)</a>"></span>
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<p />
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<div id="mimClinicalSynopsisFold" class="well well-sm collapse mimSingletonToggleFold">
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<div class="small" style="margin: 5px">
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<div>
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<div>
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<span class="h5 mim-font">
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<strong> INHERITANCE </strong>
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</span>
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</div>
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<div style="margin-left: 2em;">
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<div>
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<span class="mim-font">
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- Autosomal dominant <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/263681008" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">263681008</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/771269000" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">771269000</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0443147&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0443147</a>, <a href="https://bioportal.bioontology.org/search?q=C1867440&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1867440</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000006" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000006</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000006" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000006</a>]</span><br />
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</span>
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</div>
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</div>
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</div>
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<div>
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<div>
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<span class="h5 mim-font">
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<strong> MUSCLE, SOFT TISSUES </strong>
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</span>
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</div>
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<div style="margin-left: 2em;">
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<div>
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<span class="mim-font">
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- Flaccid weakness or paralysis, episodic attacks <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868434&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868434</a>]</span><br /> -
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Attacks last 4 to 24 hours <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868447&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868447</a>]</span><br /> -
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Attacks precipitated by hypokalemia, administration of glucose or insulin, heavy carbohydrate consumption, stress, fatigue, rest after exercise <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868448&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868448</a>]</span><br /> -
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Attacks may present during or after sleep <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868449&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868449</a>]</span><br /> -
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Attacks relieved by potassium administration <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868450&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868450</a>]</span><br /> -
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Attacks usually decrease or disappear after age 40 years <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868451&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868451</a>]</span><br /> -
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Progressive interictal weakness is common <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868452&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868452</a>]</span><br /> -
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Myotonia is usually not seen <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868453&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868453</a>]</span><br /> -
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Vacuolar myopathy may occur <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868454&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868454</a>]</span> <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/719815005" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">719815005</a>]</span><br /> -
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Tubular aggregates in muscle fibers may occur <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868455&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868455</a>]</span><br /> -
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Acetazolamide may worsen symptoms <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868456&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868456</a>]</span><br />
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</span>
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</div>
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</div>
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</div>
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<div>
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<div>
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<span class="h5 mim-font">
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<strong> LABORATORY ABNORMALITIES </strong>
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</span>
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</div>
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<div style="margin-left: 2em;">
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<div>
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<span class="mim-font">
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- Hypokalemia occurs during paralytic attacks <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1868457&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1868457</a>]</span><br />
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</span>
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</div>
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</div>
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</div>
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<div>
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<div>
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<span class="h5 mim-font">
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<strong> MISCELLANEOUS </strong>
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</span>
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</div>
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<div style="margin-left: 2em;">
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<div>
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<span class="mim-font">
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- Onset usually in second decade (may occur earlier)<br /> -
|
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One-third of cases are sporadic<br /> -
|
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Variable phenotype <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1837514&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1837514</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0003812" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0003812</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0003812" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0003812</a>]</span><br /> -
|
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Reduced penetrance in females<br /> -
|
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Allelic disorder to hyperkalemic periodic paralysis (HYPP, <a href="/entry/170500">170500</a>)<br />
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</span>
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</div>
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</div>
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</div>
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<div>
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<div>
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<span class="h5 mim-font">
|
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<strong> MOLECULAR BASIS </strong>
|
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</span>
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</div>
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<div style="margin-left: 2em;">
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<div>
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<span class="mim-font">
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- Caused by mutation in the alpha subunit of the type IV voltage-gated sodium channel gene (SCN4A, <a href="/entry/603967#0015">603967.0015</a>).<br />
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</span>
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</div>
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</div>
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</div>
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<div class="text-right">
|
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<a href="#mimClinicalSynopsisFold" data-toggle="collapse">▲ Close</a>
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</div>
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</div>
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</div>
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</div>
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<div>
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<br />
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</div>
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<div>
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<a id="text" class="mim-anchor"></a>
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<h4 href="#mimTextFold" id="mimTextToggle" class="mimTriangleToggle" style="cursor: pointer;" data-toggle="collapse">
|
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<span id="mimTextToggleTriangle" class="small mimTextToggleTriangle">▼</span>
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<span class="mim-font">
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<span class="mim-tip-floating" qtip_title="<strong>Looking For More References?</strong>" qtip_text="Click the 'reference plus' icon <span class='glyphicon glyphicon-plus-sign'></span> at the end of each OMIM text paragraph to see more references related to the content of the preceding paragraph.">
|
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<strong>TEXT</strong>
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</span>
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</span>
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</h4>
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<div id="mimTextFold" class="collapse in ">
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<span class="mim-text-font">
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<p>A number sign (#) is used with this entry because hypokalemic periodic paralysis type 2 (HOKPP2) is caused by heterozygous mutation in the SCN4A gene (<a href="/entry/603967">603967</a>).</p><p>Mutations in the SCN4A gene can also cause hyperkalemic periodic paralysis (HYPP; <a href="/entry/170500">170500</a>).</p><p>For a general phenotypic description and a discussion of genetic heterogeneity of HOKPP, see HOKPP1 (<a href="/entry/170400">170400</a>), which is caused by mutation in the CACNL1A3 gene (CACNA1S; <a href="/entry/114208">114208</a>).</p>
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</span>
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<div>
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<br />
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</div>
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<div>
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<a id="clinicalFeatures" class="mim-anchor"></a>
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<h4 href="#mimClinicalFeaturesFold" id="mimClinicalFeaturesToggle" class="mimTriangleToggle" style="cursor: pointer;" data-toggle="collapse">
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<span id="mimClinicalFeaturesToggleTriangle" class="small mimTextToggleTriangle">▼</span>
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<span class="mim-font">
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<strong>Clinical Features</strong>
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</span>
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</h4>
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</div>
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<div id="mimClinicalFeaturesFold" class="collapse in mimTextToggleFold">
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<span class="mim-text-font">
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<p><a href="#1" class="mim-tip-reference" title="Bulman, D. E., Scoggan, K. A., van Oene, M. D., Nicolle, M. W., Hahn, A. F., Tollar, L. L., Ebers, G. C. <strong>A novel sodium channel mutation in a family with hypokalemic periodic paralysis.</strong> Neurology 53: 1932-1936, 1999.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10599760/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10599760</a>] [<a href="https://doi.org/10.1212/wnl.53.9.1932" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="10599760">Bulman et al. (1999)</a> reported 2 cousins with HOKPP. The proband experienced a first paralytic attack at age 14 on awakening in the morning, and was found to have a serum potassium of 2.2 mmol/L. Myotonia was not present. Similar paralytic episodes involving either his legs or all 4 limbs recurred with variable frequency, ranging from 1 to 2 times per week to once every 2 months. Potassium supplementation was effective. His cousin had a similar phenotype. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=10599760" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p><a href="#12" class="mim-tip-reference" title="Sugiura, Y., Aoki, T., Sugiyama, Y., Hida, C., Ogata, M., Yamamoto, T. <strong>Temperature-sensitive sodium channelopathy with heat-induced myotonia and cold-induced paralysis.</strong> Neurology 54: 2179-2181, 2000.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10851391/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10851391</a>] [<a href="https://doi.org/10.1212/wnl.54.11.2179" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="10851391">Sugiura et al. (2000)</a> reported an unusual HOKPP phenotype in a Japanese family. Affected members showed heat-induced myotonia and cold-induced paralysis with hypokalemia. Myotonia lessened with exercise and was alleviated by cold, which distinguished the disorder from paramyotonia congenita (PMC; <a href="/entry/168300">168300</a>). Treatment with acetazolamide alleviated the myotonia, but slightly worsened the paralysis. Patients showed seasonal swings with myotonia in the summer and paralysis in the winter, with hypokalemia during the paralytic attacks. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=10851391" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p><a href="#13" class="mim-tip-reference" title="Venance, S. L., Jurkat-Rott, K., Lehmann-Horn, F., Tawil, R. <strong>SCN4A-associated hypokalemic periodic paralysis merits a trial of acetazolamide.</strong> Neurology 63: 1977 only, 2004.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/15557532/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">15557532</a>] [<a href="https://doi.org/10.1212/01.wnl.0000143068.99794.5b" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="15557532">Venance et al. (2004)</a> reported a sporadic patient with HOKPP2, confirmed by mutation in the SCN4A gene (<a href="/entry/603967#0020">603967.0020</a>), who responded well to acetazolamide. The authors noted the variability in response to the drug in HOKPP, and suggested that carbonic anhydrase inhibitors should be considered in patients with SCN4A-associated HOKPP. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=15557532" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p>In a review of 71 patients from 56 kindreds with HOKPP, <a href="#7" class="mim-tip-reference" title="Miller, T. M., Dias da Silva, M. R., Miller, H. A., Kwiecinski, H., Mendell, J. R., Tawil, R., McManis, P., Griggs, R. C., Angelini, C., Servidei, S., Petajan, J., Dalakas, M. C., Ranum, L. P. W., Fu, Y. H., Ptacek, L. J. <strong>Correlating phenotype and genotype in the periodic paralyses.</strong> Neurology 63: 1647-1655, 2004.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/15534250/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">15534250</a>] [<a href="https://doi.org/10.1212/01.wnl.0000143383.91137.00" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="15534250">Miller et al. (2004)</a> found that 64% of kindreds had mutations in either the CACNA1S or SCN4A genes. The arg1239-to-his (R1239H; <a href="/entry/114208#0001">114208.0001</a>) and arg528-to-his (R528H; <a href="/entry/114208#0003">114208.0003</a>) mutations of the CACNA1S gene were the most common mutations, each found in 42% of kindreds. Five kindreds had SCN4A mutations. No mutations were identified in 20 kindreds. HOKPP patients with mutations had a significantly earlier age at disease onset (10 years) compared to those without mutations (22 years); however, 2 patients with mutations presented at ages 23 and 26 years, respectively. Among those with mutations, the disease was most severe during the teenage years, and 72% of patients had residual muscle weakness. Muscle biopsies showed vacuolar changes in 80% of patients with CACNA1S mutations; these changes were not seen in any patients without mutations. Treatment with acetazolamide was beneficial in 85% of those with mutations and 100% of those without mutations. In a diagnostic flow chart for the periodic paralyses, <a href="#7" class="mim-tip-reference" title="Miller, T. M., Dias da Silva, M. R., Miller, H. A., Kwiecinski, H., Mendell, J. R., Tawil, R., McManis, P., Griggs, R. C., Angelini, C., Servidei, S., Petajan, J., Dalakas, M. C., Ranum, L. P. W., Fu, Y. H., Ptacek, L. J. <strong>Correlating phenotype and genotype in the periodic paralyses.</strong> Neurology 63: 1647-1655, 2004.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/15534250/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">15534250</a>] [<a href="https://doi.org/10.1212/01.wnl.0000143383.91137.00" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="15534250">Miller et al. (2004)</a> indicated that HOKPP shows onset in childhood to adolescence and is characterized by infrequent but severe attacks, often lasting up to 24 hours, and decreased serum potassium. Myotonia is not a feature. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=15534250" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p>
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<p>Studying families in which linkage to the CACNL1A3 gene had been excluded, <a href="#1" class="mim-tip-reference" title="Bulman, D. E., Scoggan, K. A., van Oene, M. D., Nicolle, M. W., Hahn, A. F., Tollar, L. L., Ebers, G. C. <strong>A novel sodium channel mutation in a family with hypokalemic periodic paralysis.</strong> Neurology 53: 1932-1936, 1999.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10599760/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10599760</a>] [<a href="https://doi.org/10.1212/wnl.53.9.1932" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="10599760">Bulman et al. (1999)</a> identified a mutation in the SCN4A gene (<a href="/entry/603967#0015">603967.0015</a>), and <a href="#4" class="mim-tip-reference" title="Jurkat-Rott, K., Mitrovic, N., Hang, C., Kouzmekine, A., Iaizzo, P., Herzog, J., Lerche, H., Nicole, S., Vale-Santos, J., Chauveau, D., Fontaine, B., Lehmann-Horn, F. <strong>Voltage-sensor sodium channel mutations cause hypokalemic periodic paralysis type 2 by enhanced inactivation and reduced current.</strong> Proc. Nat. Acad. Sci. 97: 9549-9554, 2000.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10944223/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10944223</a>, <a href="https://www.ncbi.nlm.nih.gov/pmc/?term=10944223[PMID]&report=imagesdocsum" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Image', 'domain': 'ncbi.nlm.nih.gov'})">images</a>] [<a href="https://doi.org/10.1073/pnas.97.17.9549" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="10944223">Jurkat-Rott et al. (2000)</a> identified other mutations (<a href="/entry/603967#0016">603967.0016</a> and <a href="/entry/603967#0017">603967.0017</a>) in the same gene. The clinical picture did not differ from that of HOKPP caused by mutations in the CACNL1A3 gene. <a href="https://pubmed.ncbi.nlm.nih.gov/?term=10599760+10944223" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p>In a Japanese family with an unusual temperature-dependent HOKPP phenotype, <a href="#12" class="mim-tip-reference" title="Sugiura, Y., Aoki, T., Sugiyama, Y., Hida, C., Ogata, M., Yamamoto, T. <strong>Temperature-sensitive sodium channelopathy with heat-induced myotonia and cold-induced paralysis.</strong> Neurology 54: 2179-2181, 2000.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10851391/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10851391</a>] [<a href="https://doi.org/10.1212/wnl.54.11.2179" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="10851391">Sugiura et al. (2000)</a> identified a mutation in the SCN4A gene (P1158S; <a href="/entry/603967#0021">603967.0021</a>). <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=10851391" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p><a href="#2" class="mim-tip-reference" title="Davies, N. P., Eunson, L. H., Samuel, M., Hanna, M. G. <strong>Sodium channel gene mutations in hypokalemic periodic paralysis: an uncommon cause in the UK.</strong> Neurology 57: 1323-1325, 2001.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/11591859/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">11591859</a>] [<a href="https://doi.org/10.1212/wnl.57.7.1323" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="11591859">Davies et al. (2001)</a> found that 11 of 36 families with HOKPP harbored mutations in the CACNA1S gene (<a href="/entry/114208#0001">114208.0001</a> and <a href="/entry/114208#0003">114208.0003</a>), whereas only 1 family had a mutation in the SCN4A gene (<a href="/entry/603967#0020">603967.0020</a>), suggesting that SCN4A mutations are an uncommon cause of HOKPP in the U.K. Among 58 independent index cases of HOKPP, <a href="#11" class="mim-tip-reference" title="Sternberg, D., Maisonabe, T., Jurkat-Rott, K., Nicole, S., Launay, E., Chauveau, D., Tabti, N., Lehmann-Horn, F., Hainque, B., Fontaine, B. <strong>Hypokalaemic periodic paralysis type 2 caused by mutation at codon 672 in the muscle sodium channel gene SCN4A.</strong> Brain 124: 1091-1099, 2001.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/11353725/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">11353725</a>] [<a href="https://doi.org/10.1093/brain/124.6.1091" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="11353725">Sternberg et al. (2001)</a> found that 40 were linked to the CACNA1S gene and 5 to the SCN4A gene, all of which were in the same codon (see, e.g., <a href="/entry/603967#0016">603967.0016</a>). Thirteen families remained without known mutations, indicating genetic heterogeneity. <a href="https://pubmed.ncbi.nlm.nih.gov/?term=11591859+11353725" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p><a href="#6" class="mim-tip-reference" title="Matthews, E., Labrum, R., Sweeney, M. G., Sud, R., Haworth, A., Chinnery, P. F., Meola, G., Schorge, S., Kullmann, D. M., Davis, M. B., Hanna, M. G. <strong>Voltage sensor charge loss accounts for most cases of hypokalemic periodic paralysis.</strong> Neurology 72: 1544-1547, 2009.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/19118277/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">19118277</a>, <a href="https://www.ncbi.nlm.nih.gov/pmc/?term=19118277[PMID]&report=imagesdocsum" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Image', 'domain': 'ncbi.nlm.nih.gov'})">images</a>] [<a href="https://doi.org/10.1212/01.wnl.0000342387.65477.46" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="19118277">Matthews et al. (2009)</a> identified mutations in the CACNA1S or SCN4A gene in 74 (almost 90%) of 83 patients with HOKPP. All of the mutations, including 3 novel mutations, affected arginine residues in the S4 voltage sensing region in 1 of the transmembrane domains of each gene. The most common mutations affected residues arg528 (25 cases) and arg1239 (39 cases) in CACNA1S (see, e.g., R1239H; <a href="/entry/114208#0001">114208.0001</a> and R528H; <a href="/entry/114208#0003">114208.0003</a>). The most common mutations in SCN4A affected residues arg672 (see, e.g., <a href="/entry/603967#0016">603967.0016</a>) and arg1132. The findings supported the hypothesis that loss of positive charge in S4 voltage sensors is important to the pathogenesis of this disorder. (<a href="#10" class="mim-tip-reference" title="Sokolov, S., Scheuer, T., Catterall, W. A. <strong>Gating pore current in an inherited ion channelopathy.</strong> Nature 446: 76-78, 2007.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17330043/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17330043</a>] [<a href="https://doi.org/10.1038/nature05598" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="17330043">Sokolov et al., 2007</a>). <a href="https://pubmed.ncbi.nlm.nih.gov/?term=19118277+17330043" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p>
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<p>In muscle fibers of patients with HOKPP, <a href="#8" class="mim-tip-reference" title="Rudel, R., Lehmann-Horn, F., Ricker, K., Kuther, G. <strong>Hypokalemia periodic paralysis: in vitro investigation of muscle fiber membrane parameters.</strong> Muscle Nerve 7: 110-120, 1984.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/6325904/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">6325904</a>] [<a href="https://doi.org/10.1002/mus.880070205" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="6325904">Rudel et al. (1984)</a> determined that the basic defects were a reduced excitability and an increased sodium conductance, and that these defects were aggravated by reduction of the extracellular potassium concentration. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=6325904" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p>In a commentary, <a href="#9" class="mim-tip-reference" title="Ruff, R. <strong>Skeletal muscle sodium current is reduced in hypokalemic periodic paralysis.</strong> Proc. Nat. Acad. Sci. 97: 9832-9833, 2000.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10954743/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10954743</a>] [<a href="https://doi.org/10.1073/pnas.170293197" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="10954743">Ruff (2000)</a> reviewed the evidence that HOKPP is caused by membrane depolarization triggering sodium channel inactivation, which renders the muscle membrane inexcitable. In addition, SCN4A mutations may also result in decreased density of membrane sodium channels, also decreasing overall current. HOKPP resulting from calcium channel mutations (CACNA1S) represent an 'indirect channelopathy': membrane depolarization results from hypokalemia activating a pathologic depolarizing current and from decreased inward rectifier potassium channel conductance. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=10954743" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p>By in vitro studies, <a href="#5" class="mim-tip-reference" title="Kuzmenkin, A., Muncan, V., Jurkat-Rott, K., Hang, C., Lerche, H., Lehmann-Horn, F., Mitrovic, N. <strong>Enhanced inactivation and pH sensitivity of Na+ channel mutations causing hypokalemic periodic paralysis type II.</strong> Brain 125: 835-843, 2002.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/11912116/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">11912116</a>] [<a href="https://doi.org/10.1093/brain/awf071" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="11912116">Kuzmenkin et al. (2002)</a> showed that 2 mutations in the voltage sensor region of the SCN4A gene (R669H <a href="/entry/603967#0015">603967.0015</a> and R672H; <a href="/entry/603967#0016">603967.0016</a>) showed enhanced inactivation. The inactivation defects could be alleviated by decreased pH, which may explain why some patients have relief by some physical exercise. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=11912116" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p><a href="#10" class="mim-tip-reference" title="Sokolov, S., Scheuer, T., Catterall, W. A. <strong>Gating pore current in an inherited ion channelopathy.</strong> Nature 446: 76-78, 2007.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17330043/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17330043</a>] [<a href="https://doi.org/10.1038/nature05598" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="17330043">Sokolov et al. (2007)</a> showed that 3 mutations in gating charge-carrying arginine residues in an S4 segment that cause HOKPP induced a hyperpolarization-activated cationic leak through the voltage sensor of the skeletal muscle Nav1.4 channel (SCN4A). This cation leak would substantially increase resting membrane conductance and sodium influx into HOKPP skeletal muscle fibers, resulting in a gain of function effect that contributes to the dominant inheritance, depolarization, reduced rate of rise and amplitude of the action potential, cytopathology, and episodic paralysis correlated with decreased serum potassium. The mutant channels showed similar permeability to sodium, potassium, and cesium ions, but the organic monovalent cations tetraethylammonium and N-methyl-D-glucamine were much less permeant. <a href="#10" class="mim-tip-reference" title="Sokolov, S., Scheuer, T., Catterall, W. A. <strong>Gating pore current in an inherited ion channelopathy.</strong> Nature 446: 76-78, 2007.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17330043/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17330043</a>] [<a href="https://doi.org/10.1038/nature05598" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="17330043">Sokolov et al. (2007)</a> concluded that their results revealed gating pore current in naturally occurring disease mutations of an ion channel and showed a clear correlation between mutations that cause gating pore current and HOKPP. In addition, the findings contrasted with the well-established paradigm in which alterations in control of ion conductance through the central pore of ion channels impair cell function. <a href="#10" class="mim-tip-reference" title="Sokolov, S., Scheuer, T., Catterall, W. A. <strong>Gating pore current in an inherited ion channelopathy.</strong> Nature 446: 76-78, 2007.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17330043/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17330043</a>] [<a href="https://doi.org/10.1038/nature05598" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="17330043">Sokolov et al. (2007)</a> postulated that their observations might be generalizable to other ion channelopathies. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17330043" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p><p><a href="#3" class="mim-tip-reference" title="Francis, D. G., Rybalchenko, V., Struyk, A., Cannon, S. C. <strong>Leaky sodium channels from voltage sensor mutations in periodic paralysis, but not paramyotonia.</strong> Neurology 76: 1635-1641, 2011.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/21490317/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">21490317</a>, <a href="https://www.ncbi.nlm.nih.gov/pmc/?term=21490317[PMID]&report=imagesdocsum" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Image', 'domain': 'ncbi.nlm.nih.gov'})">images</a>] [<a href="https://doi.org/10.1212/WNL.0b013e318219fb57" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="21490317">Francis et al. (2011)</a> demonstrated that an R1132Q mutation (<a href="/entry/603967#0030">603967.0030</a>) in the domain III voltage sensor domain of SCN4A found in a family with HOKPP created an anomalous gating pore current similar to that observed by <a href="#10" class="mim-tip-reference" title="Sokolov, S., Scheuer, T., Catterall, W. A. <strong>Gating pore current in an inherited ion channelopathy.</strong> Nature 446: 76-78, 2007.[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17330043/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17330043</a>] [<a href="https://doi.org/10.1038/nature05598" target="_blank" onclick="gtag('event', 'mim_outbound', {'destination': 'Publisher'})">Full Text</a>]" pmid="17330043">Sokolov et al. (2007)</a>. This current is sufficient to depolarize and render the muscle fiber inexcitable particularly during low external potassium. The findings suggested a mechanism for loss of sarcolemmal excitability during attacks of weakness in HOKPP. In contrast, the R1148C mutation (<a href="/entry/603967#0003">603967.0003</a>) causing PMC (<a href="/entry/168300">168300</a>) did not result in gating pore abnormalities. <a href="https://pubmed.ncbi.nlm.nih.gov/?term=17330043+21490317" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})"><span class="glyphicon glyphicon-plus-sign mim-tip-hint" title="Click this 'reference-plus' icon to see articles related to this paragraph in PubMed."></span></a></p>
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[<a href="https://doi.org/10.1212/wnl.53.9.1932" target="_blank">Full Text</a>]
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<a id="Davies2001" class="mim-anchor"></a>
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Davies, N. P., Eunson, L. H., Samuel, M., Hanna, M. G.
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<strong>Sodium channel gene mutations in hypokalemic periodic paralysis: an uncommon cause in the UK.</strong>
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/11591859/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">11591859</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=11591859" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1212/wnl.57.7.1323" target="_blank">Full Text</a>]
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<a id="Francis2011" class="mim-anchor"></a>
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Francis, D. G., Rybalchenko, V., Struyk, A., Cannon, S. C.
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<strong>Leaky sodium channels from voltage sensor mutations in periodic paralysis, but not paramyotonia.</strong>
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Neurology 76: 1635-1641, 2011.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/21490317/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">21490317</a>, <a href="https://www.ncbi.nlm.nih.gov/pmc/?term=21490317[PMID]&report=imagesdocsum" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Image', 'domain': 'ncbi.nlm.nih.gov'})">images</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=21490317" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1212/WNL.0b013e318219fb57" target="_blank">Full Text</a>]
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<a id="Jurkat-Rott2000" class="mim-anchor"></a>
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Jurkat-Rott, K., Mitrovic, N., Hang, C., Kouzmekine, A., Iaizzo, P., Herzog, J., Lerche, H., Nicole, S., Vale-Santos, J., Chauveau, D., Fontaine, B., Lehmann-Horn, F.
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<strong>Voltage-sensor sodium channel mutations cause hypokalemic periodic paralysis type 2 by enhanced inactivation and reduced current.</strong>
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Proc. Nat. Acad. Sci. 97: 9549-9554, 2000.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10944223/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10944223</a>, <a href="https://www.ncbi.nlm.nih.gov/pmc/?term=10944223[PMID]&report=imagesdocsum" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Image', 'domain': 'ncbi.nlm.nih.gov'})">images</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=10944223" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1073/pnas.97.17.9549" target="_blank">Full Text</a>]
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Kuzmenkin, A., Muncan, V., Jurkat-Rott, K., Hang, C., Lerche, H., Lehmann-Horn, F., Mitrovic, N.
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<strong>Enhanced inactivation and pH sensitivity of Na+ channel mutations causing hypokalemic periodic paralysis type II.</strong>
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Brain 125: 835-843, 2002.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/11912116/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">11912116</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=11912116" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1093/brain/awf071" target="_blank">Full Text</a>]
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Matthews, E., Labrum, R., Sweeney, M. G., Sud, R., Haworth, A., Chinnery, P. F., Meola, G., Schorge, S., Kullmann, D. M., Davis, M. B., Hanna, M. G.
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<strong>Voltage sensor charge loss accounts for most cases of hypokalemic periodic paralysis.</strong>
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Neurology 72: 1544-1547, 2009.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/19118277/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">19118277</a>, <a href="https://www.ncbi.nlm.nih.gov/pmc/?term=19118277[PMID]&report=imagesdocsum" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Image', 'domain': 'ncbi.nlm.nih.gov'})">images</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=19118277" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1212/01.wnl.0000342387.65477.46" target="_blank">Full Text</a>]
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<a id="Miller2004" class="mim-anchor"></a>
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Miller, T. M., Dias da Silva, M. R., Miller, H. A., Kwiecinski, H., Mendell, J. R., Tawil, R., McManis, P., Griggs, R. C., Angelini, C., Servidei, S., Petajan, J., Dalakas, M. C., Ranum, L. P. W., Fu, Y. H., Ptacek, L. J.
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Neurology 63: 1647-1655, 2004.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/15534250/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">15534250</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=15534250" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1212/01.wnl.0000143383.91137.00" target="_blank">Full Text</a>]
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<a id="8" class="mim-anchor"></a>
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<a id="Rudel1984" class="mim-anchor"></a>
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<div class="">
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<p class="mim-text-font">
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Rudel, R., Lehmann-Horn, F., Ricker, K., Kuther, G.
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<strong>Hypokalemia periodic paralysis: in vitro investigation of muscle fiber membrane parameters.</strong>
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Muscle Nerve 7: 110-120, 1984.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/6325904/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">6325904</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=6325904" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1002/mus.880070205" target="_blank">Full Text</a>]
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<a id="Ruff2000" class="mim-anchor"></a>
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<div class="">
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<p class="mim-text-font">
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Ruff, R.
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<strong>Skeletal muscle sodium current is reduced in hypokalemic periodic paralysis.</strong>
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Proc. Nat. Acad. Sci. 97: 9832-9833, 2000.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10954743/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10954743</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=10954743" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1073/pnas.170293197" target="_blank">Full Text</a>]
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<a id="Sokolov2007" class="mim-anchor"></a>
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<div class="">
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<p class="mim-text-font">
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Sokolov, S., Scheuer, T., Catterall, W. A.
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<strong>Gating pore current in an inherited ion channelopathy.</strong>
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Nature 446: 76-78, 2007.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17330043/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17330043</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17330043" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1038/nature05598" target="_blank">Full Text</a>]
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<a id="Sternberg2001" class="mim-anchor"></a>
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Sternberg, D., Maisonabe, T., Jurkat-Rott, K., Nicole, S., Launay, E., Chauveau, D., Tabti, N., Lehmann-Horn, F., Hainque, B., Fontaine, B.
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<strong>Hypokalaemic periodic paralysis type 2 caused by mutation at codon 672 in the muscle sodium channel gene SCN4A.</strong>
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Brain 124: 1091-1099, 2001.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/11353725/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">11353725</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=11353725" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1093/brain/124.6.1091" target="_blank">Full Text</a>]
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<a id="Sugiura2000" class="mim-anchor"></a>
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Sugiura, Y., Aoki, T., Sugiyama, Y., Hida, C., Ogata, M., Yamamoto, T.
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<strong>Temperature-sensitive sodium channelopathy with heat-induced myotonia and cold-induced paralysis.</strong>
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Neurology 54: 2179-2181, 2000.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/10851391/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">10851391</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=10851391" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1212/wnl.54.11.2179" target="_blank">Full Text</a>]
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<a id="Venance2004" class="mim-anchor"></a>
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Venance, S. L., Jurkat-Rott, K., Lehmann-Horn, F., Tawil, R.
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<strong>SCN4A-associated hypokalemic periodic paralysis merits a trial of acetazolamide.</strong>
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Neurology 63: 1977 only, 2004.
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[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/15557532/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">15557532</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=15557532" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
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[<a href="https://doi.org/10.1212/01.wnl.0000143068.99794.5b" target="_blank">Full Text</a>]
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<span class="mim-text-font">
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Cassandra L. Kniffin - updated : 5/8/2013
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Cassandra L. Kniffin : 4/7/2010
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carol : 02/16/2016
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alopez : 5/14/2013<br>ckniffin : 5/8/2013<br>ckniffin : 4/7/2010
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HYPOKALEMIC PERIODIC PARALYSIS, TYPE 2; HOKPP2
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<strong>ORPHA:</strong> 681;
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<strong>DO:</strong> 14452;
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<strong>Phenotype-Gene Relationships</strong>
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Location
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Phenotype
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Phenotype <br /> MIM number
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Inheritance
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Phenotype <br /> mapping key
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Gene/Locus <br /> MIM number
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17q23.3
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Hypokalemic periodic paralysis, type 2
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613345
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Autosomal dominant
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3
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SCN4A
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603967
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<p>A number sign (#) is used with this entry because hypokalemic periodic paralysis type 2 (HOKPP2) is caused by heterozygous mutation in the SCN4A gene (603967).</p><p>Mutations in the SCN4A gene can also cause hyperkalemic periodic paralysis (HYPP; 170500).</p><p>For a general phenotypic description and a discussion of genetic heterogeneity of HOKPP, see HOKPP1 (170400), which is caused by mutation in the CACNL1A3 gene (CACNA1S; 114208).</p>
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<strong>Clinical Features</strong>
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<p>Bulman et al. (1999) reported 2 cousins with HOKPP. The proband experienced a first paralytic attack at age 14 on awakening in the morning, and was found to have a serum potassium of 2.2 mmol/L. Myotonia was not present. Similar paralytic episodes involving either his legs or all 4 limbs recurred with variable frequency, ranging from 1 to 2 times per week to once every 2 months. Potassium supplementation was effective. His cousin had a similar phenotype. </p><p>Sugiura et al. (2000) reported an unusual HOKPP phenotype in a Japanese family. Affected members showed heat-induced myotonia and cold-induced paralysis with hypokalemia. Myotonia lessened with exercise and was alleviated by cold, which distinguished the disorder from paramyotonia congenita (PMC; 168300). Treatment with acetazolamide alleviated the myotonia, but slightly worsened the paralysis. Patients showed seasonal swings with myotonia in the summer and paralysis in the winter, with hypokalemia during the paralytic attacks. </p><p>Venance et al. (2004) reported a sporadic patient with HOKPP2, confirmed by mutation in the SCN4A gene (603967.0020), who responded well to acetazolamide. The authors noted the variability in response to the drug in HOKPP, and suggested that carbonic anhydrase inhibitors should be considered in patients with SCN4A-associated HOKPP. </p><p>In a review of 71 patients from 56 kindreds with HOKPP, Miller et al. (2004) found that 64% of kindreds had mutations in either the CACNA1S or SCN4A genes. The arg1239-to-his (R1239H; 114208.0001) and arg528-to-his (R528H; 114208.0003) mutations of the CACNA1S gene were the most common mutations, each found in 42% of kindreds. Five kindreds had SCN4A mutations. No mutations were identified in 20 kindreds. HOKPP patients with mutations had a significantly earlier age at disease onset (10 years) compared to those without mutations (22 years); however, 2 patients with mutations presented at ages 23 and 26 years, respectively. Among those with mutations, the disease was most severe during the teenage years, and 72% of patients had residual muscle weakness. Muscle biopsies showed vacuolar changes in 80% of patients with CACNA1S mutations; these changes were not seen in any patients without mutations. Treatment with acetazolamide was beneficial in 85% of those with mutations and 100% of those without mutations. In a diagnostic flow chart for the periodic paralyses, Miller et al. (2004) indicated that HOKPP shows onset in childhood to adolescence and is characterized by infrequent but severe attacks, often lasting up to 24 hours, and decreased serum potassium. Myotonia is not a feature. </p>
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<span class="mim-font">
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<strong>Molecular Genetics</strong>
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<p>Studying families in which linkage to the CACNL1A3 gene had been excluded, Bulman et al. (1999) identified a mutation in the SCN4A gene (603967.0015), and Jurkat-Rott et al. (2000) identified other mutations (603967.0016 and 603967.0017) in the same gene. The clinical picture did not differ from that of HOKPP caused by mutations in the CACNL1A3 gene. </p><p>In a Japanese family with an unusual temperature-dependent HOKPP phenotype, Sugiura et al. (2000) identified a mutation in the SCN4A gene (P1158S; 603967.0021). </p><p>Davies et al. (2001) found that 11 of 36 families with HOKPP harbored mutations in the CACNA1S gene (114208.0001 and 114208.0003), whereas only 1 family had a mutation in the SCN4A gene (603967.0020), suggesting that SCN4A mutations are an uncommon cause of HOKPP in the U.K. Among 58 independent index cases of HOKPP, Sternberg et al. (2001) found that 40 were linked to the CACNA1S gene and 5 to the SCN4A gene, all of which were in the same codon (see, e.g., 603967.0016). Thirteen families remained without known mutations, indicating genetic heterogeneity. </p><p>Matthews et al. (2009) identified mutations in the CACNA1S or SCN4A gene in 74 (almost 90%) of 83 patients with HOKPP. All of the mutations, including 3 novel mutations, affected arginine residues in the S4 voltage sensing region in 1 of the transmembrane domains of each gene. The most common mutations affected residues arg528 (25 cases) and arg1239 (39 cases) in CACNA1S (see, e.g., R1239H; 114208.0001 and R528H; 114208.0003). The most common mutations in SCN4A affected residues arg672 (see, e.g., 603967.0016) and arg1132. The findings supported the hypothesis that loss of positive charge in S4 voltage sensors is important to the pathogenesis of this disorder. (Sokolov et al., 2007). </p>
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<h4>
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<span class="mim-font">
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<strong>Pathogenesis</strong>
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<p>In muscle fibers of patients with HOKPP, Rudel et al. (1984) determined that the basic defects were a reduced excitability and an increased sodium conductance, and that these defects were aggravated by reduction of the extracellular potassium concentration. </p><p>In a commentary, Ruff (2000) reviewed the evidence that HOKPP is caused by membrane depolarization triggering sodium channel inactivation, which renders the muscle membrane inexcitable. In addition, SCN4A mutations may also result in decreased density of membrane sodium channels, also decreasing overall current. HOKPP resulting from calcium channel mutations (CACNA1S) represent an 'indirect channelopathy': membrane depolarization results from hypokalemia activating a pathologic depolarizing current and from decreased inward rectifier potassium channel conductance. </p><p>By in vitro studies, Kuzmenkin et al. (2002) showed that 2 mutations in the voltage sensor region of the SCN4A gene (R669H 603967.0015 and R672H; 603967.0016) showed enhanced inactivation. The inactivation defects could be alleviated by decreased pH, which may explain why some patients have relief by some physical exercise. </p><p>Sokolov et al. (2007) showed that 3 mutations in gating charge-carrying arginine residues in an S4 segment that cause HOKPP induced a hyperpolarization-activated cationic leak through the voltage sensor of the skeletal muscle Nav1.4 channel (SCN4A). This cation leak would substantially increase resting membrane conductance and sodium influx into HOKPP skeletal muscle fibers, resulting in a gain of function effect that contributes to the dominant inheritance, depolarization, reduced rate of rise and amplitude of the action potential, cytopathology, and episodic paralysis correlated with decreased serum potassium. The mutant channels showed similar permeability to sodium, potassium, and cesium ions, but the organic monovalent cations tetraethylammonium and N-methyl-D-glucamine were much less permeant. Sokolov et al. (2007) concluded that their results revealed gating pore current in naturally occurring disease mutations of an ion channel and showed a clear correlation between mutations that cause gating pore current and HOKPP. In addition, the findings contrasted with the well-established paradigm in which alterations in control of ion conductance through the central pore of ion channels impair cell function. Sokolov et al. (2007) postulated that their observations might be generalizable to other ion channelopathies. </p><p>Francis et al. (2011) demonstrated that an R1132Q mutation (603967.0030) in the domain III voltage sensor domain of SCN4A found in a family with HOKPP created an anomalous gating pore current similar to that observed by Sokolov et al. (2007). This current is sufficient to depolarize and render the muscle fiber inexcitable particularly during low external potassium. The findings suggested a mechanism for loss of sarcolemmal excitability during attacks of weakness in HOKPP. In contrast, the R1148C mutation (603967.0003) causing PMC (168300) did not result in gating pore abnormalities. </p>
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<h4>
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<span class="mim-font">
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<strong>REFERENCES</strong>
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</h4>
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<p />
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<ol>
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<p class="mim-text-font">
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Bulman, D. E., Scoggan, K. A., van Oene, M. D., Nicolle, M. W., Hahn, A. F., Tollar, L. L., Ebers, G. C.
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<strong>A novel sodium channel mutation in a family with hypokalemic periodic paralysis.</strong>
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Neurology 53: 1932-1936, 1999.
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[PubMed: 10599760]
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[Full Text: https://doi.org/10.1212/wnl.53.9.1932]
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<p class="mim-text-font">
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Davies, N. P., Eunson, L. H., Samuel, M., Hanna, M. G.
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<strong>Sodium channel gene mutations in hypokalemic periodic paralysis: an uncommon cause in the UK.</strong>
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Neurology 57: 1323-1325, 2001.
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[PubMed: 11591859]
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[Full Text: https://doi.org/10.1212/wnl.57.7.1323]
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<p class="mim-text-font">
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Francis, D. G., Rybalchenko, V., Struyk, A., Cannon, S. C.
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<strong>Leaky sodium channels from voltage sensor mutations in periodic paralysis, but not paramyotonia.</strong>
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Neurology 76: 1635-1641, 2011.
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[PubMed: 21490317]
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[Full Text: https://doi.org/10.1212/WNL.0b013e318219fb57]
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<li>
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<p class="mim-text-font">
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Jurkat-Rott, K., Mitrovic, N., Hang, C., Kouzmekine, A., Iaizzo, P., Herzog, J., Lerche, H., Nicole, S., Vale-Santos, J., Chauveau, D., Fontaine, B., Lehmann-Horn, F.
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<strong>Voltage-sensor sodium channel mutations cause hypokalemic periodic paralysis type 2 by enhanced inactivation and reduced current.</strong>
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Proc. Nat. Acad. Sci. 97: 9549-9554, 2000.
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[PubMed: 10944223]
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[Full Text: https://doi.org/10.1073/pnas.97.17.9549]
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</p>
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</li>
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<li>
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<p class="mim-text-font">
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Kuzmenkin, A., Muncan, V., Jurkat-Rott, K., Hang, C., Lerche, H., Lehmann-Horn, F., Mitrovic, N.
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<strong>Enhanced inactivation and pH sensitivity of Na+ channel mutations causing hypokalemic periodic paralysis type II.</strong>
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Brain 125: 835-843, 2002.
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[PubMed: 11912116]
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[Full Text: https://doi.org/10.1093/brain/awf071]
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</p>
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</li>
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<li>
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<p class="mim-text-font">
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Matthews, E., Labrum, R., Sweeney, M. G., Sud, R., Haworth, A., Chinnery, P. F., Meola, G., Schorge, S., Kullmann, D. M., Davis, M. B., Hanna, M. G.
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<strong>Voltage sensor charge loss accounts for most cases of hypokalemic periodic paralysis.</strong>
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Neurology 72: 1544-1547, 2009.
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[PubMed: 19118277]
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[Full Text: https://doi.org/10.1212/01.wnl.0000342387.65477.46]
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</p>
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</li>
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<li>
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<p class="mim-text-font">
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Miller, T. M., Dias da Silva, M. R., Miller, H. A., Kwiecinski, H., Mendell, J. R., Tawil, R., McManis, P., Griggs, R. C., Angelini, C., Servidei, S., Petajan, J., Dalakas, M. C., Ranum, L. P. W., Fu, Y. H., Ptacek, L. J.
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<strong>Correlating phenotype and genotype in the periodic paralyses.</strong>
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Neurology 63: 1647-1655, 2004.
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[PubMed: 15534250]
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[Full Text: https://doi.org/10.1212/01.wnl.0000143383.91137.00]
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</p>
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</li>
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<li>
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<p class="mim-text-font">
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Rudel, R., Lehmann-Horn, F., Ricker, K., Kuther, G.
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<strong>Hypokalemia periodic paralysis: in vitro investigation of muscle fiber membrane parameters.</strong>
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Muscle Nerve 7: 110-120, 1984.
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[PubMed: 6325904]
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[Full Text: https://doi.org/10.1002/mus.880070205]
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</p>
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</li>
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<li>
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<p class="mim-text-font">
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Ruff, R.
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<strong>Skeletal muscle sodium current is reduced in hypokalemic periodic paralysis.</strong>
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Proc. Nat. Acad. Sci. 97: 9832-9833, 2000.
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[PubMed: 10954743]
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[Full Text: https://doi.org/10.1073/pnas.170293197]
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</p>
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</li>
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<li>
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<p class="mim-text-font">
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Sokolov, S., Scheuer, T., Catterall, W. A.
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<strong>Gating pore current in an inherited ion channelopathy.</strong>
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Nature 446: 76-78, 2007.
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[PubMed: 17330043]
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[Full Text: https://doi.org/10.1038/nature05598]
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</p>
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</li>
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<li>
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<p class="mim-text-font">
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Sternberg, D., Maisonabe, T., Jurkat-Rott, K., Nicole, S., Launay, E., Chauveau, D., Tabti, N., Lehmann-Horn, F., Hainque, B., Fontaine, B.
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<strong>Hypokalaemic periodic paralysis type 2 caused by mutation at codon 672 in the muscle sodium channel gene SCN4A.</strong>
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Brain 124: 1091-1099, 2001.
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[PubMed: 11353725]
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[Full Text: https://doi.org/10.1093/brain/124.6.1091]
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Sugiura, Y., Aoki, T., Sugiyama, Y., Hida, C., Ogata, M., Yamamoto, T.
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<strong>Temperature-sensitive sodium channelopathy with heat-induced myotonia and cold-induced paralysis.</strong>
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Neurology 54: 2179-2181, 2000.
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[PubMed: 10851391]
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[Full Text: https://doi.org/10.1212/wnl.54.11.2179]
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Venance, S. L., Jurkat-Rott, K., Lehmann-Horn, F., Tawil, R.
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<strong>SCN4A-associated hypokalemic periodic paralysis merits a trial of acetazolamide.</strong>
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Neurology 63: 1977 only, 2004.
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[PubMed: 15557532]
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[Full Text: https://doi.org/10.1212/01.wnl.0000143068.99794.5b]
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Cassandra L. Kniffin - updated : 5/8/2013
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Cassandra L. Kniffin : 4/7/2010
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carol : 02/16/2016<br>alopez : 5/14/2013<br>ckniffin : 5/8/2013<br>ckniffin : 4/7/2010
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