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Entry
- #610743 - SPINOCEREBELLAR ATAXIA, AUTOSOMAL RECESSIVE 8; SCAR8
- OMIM
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<span class="h4">#610743</span>
<br />
<strong>Table of Contents</strong>
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<a href="#phenotypeMap"><strong>Phenotype-Gene Relationships</strong></a>
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<a href="/clinicalSynopsis/610743"><strong>Clinical Synopsis</strong></a>
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<a href="/phenotypicSeries/PS213200"> <strong>Phenotypic Series</strong> </a>
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<a href="#description">Description</a>
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<a href="#clinicalFeatures">Clinical Features</a>
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<a href="#inheritance">Inheritance</a>
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<a href="#mapping">Mapping</a>
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<a href="#molecularGenetics">Molecular Genetics</a>
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<a href="#references"><strong>References</strong></a>
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<div><a href="https://clinicaltrials.gov/search?cond=SPINOCEREBELLAR ATAXIA, AUTOSOMAL RECESSIVE" class="mim-tip-hint" title="A registry of federally and privately supported clinical trials conducted in the United States and around the world." target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'Clinical Trials', 'domain': 'clinicaltrials.gov'})">Clinical Trials</a></div>
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<div style="display: table-cell;">Animal Models</div>
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</div>
<div id="mimAnimalModelsLinksFold" class="panel-collapse collapse mimLinksFold" role="tabpanel">
<div class="panel-body small mim-panel-body">
<div><a href="https://www.alliancegenome.org/disease/DOID:0111618" 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>
<div><a href="http://www.informatics.jax.org/disease/610743" 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>
<div><a href="https://wormbase.org/resources/disease/DOID:0111618" 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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</div>
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<span>
<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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<div class="col-lg-8 col-lg-pull-2 col-md-8 col-md-pull-2 col-sm-8 col-sm-pull-2 col-xs-12">
<div>
<a id="title" class="mim-anchor"></a>
<div>
<a id="number" class="mim-anchor"></a>
<div class="text-right">
<a href="#" class="mim-tip-icd" qtip_title="<strong>ICD+</strong>" qtip_text="
<strong>ORPHA:</strong> 88644<br />
<strong>DO:</strong> 0111618<br />
">ICD+</a>
</div>
<div>
<span class="h3">
<span class="mim-font mim-tip-hint" title="Phenotype description, molecular basis known">
<span class="text-danger"><strong>#</strong></span>
610743
</span>
</span>
</div>
</div>
<div>
<a id="preferredTitle" class="mim-anchor"></a>
<h3>
<span class="mim-font">
SPINOCEREBELLAR ATAXIA, AUTOSOMAL RECESSIVE 8; SCAR8
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</h3>
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<div>
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<div>
<a id="alternativeTitles" class="mim-anchor"></a>
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<p>
<span class="mim-font">
<em>Alternative titles; symbols</em>
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</p>
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<div>
<h4>
<span class="mim-font">
ATAXIA, RECESSIVE, OF BEAUCE<br />
CEREBELLAR ATAXIA, AUTOSOMAL RECESSIVE, TYPE 1; ARCA1
</span>
</h4>
</div>
</div>
<div>
<br />
</div>
</div>
<div>
<a id="phenotypeMap" class="mim-anchor"></a>
<h4>
<span class="mim-font">
<strong>Phenotype-Gene Relationships</strong>
</span>
</h4>
<div>
<table class="table table-bordered table-condensed table-hover small mim-table-padding">
<thead>
<tr class="active">
<th>
Location
</th>
<th>
Phenotype
</th>
<th>
Phenotype <br /> MIM number
</th>
<th>
Inheritance
</th>
<th>
Phenotype <br /> mapping key
</th>
<th>
Gene/Locus
</th>
<th>
Gene/Locus <br /> MIM number
</th>
</tr>
</thead>
<tbody>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/6/963?start=-3&limit=10&highlight=963">
6q25.2
</a>
</span>
</td>
<td>
<span class="mim-font">
Spinocerebellar ataxia, autosomal recessive 8
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/610743"> 610743 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
SYNE1
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608441"> 608441 </a>
</span>
</td>
</tr>
</tbody>
</table>
</div>
</div>
<div>
<div class="btn-group ">
<a href="/clinicalSynopsis/610743" class="btn btn-warning" role="button"> Clinical Synopsis </a>
<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="sr-only">Toggle Dropdown</span>
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<a href="/phenotypicSeries/PS213200" class="btn btn-info" role="button"> Phenotypic Series </a>
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&nbsp;
<div class="btn-group">
<button type="button" class="btn btn-success dropdown-toggle" data-toggle="dropdown" aria-haspopup="true" aria-expanded="false">
PheneGene Graphics <span class="caret"></span>
</button>
<ul class="dropdown-menu" style="width: 17em;">
<li><a href="/graph/linear/610743" target="_blank" onclick="gtag('event', 'mim_graph', {'destination': 'Linear'})"> Linear </a></li>
<li><a href="/graph/radial/610743" target="_blank" onclick="gtag('event', 'mim_graph', {'destination': 'Radial'})"> Radial </a></li>
</ul>
</div>
<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>
<div>
<p />
</div>
<div id="mimClinicalSynopsisFold" class="well well-sm collapse mimSingletonToggleFold">
<div class="small" style="margin: 5px">
<div>
<div>
<span class="h5 mim-font">
<strong> INHERITANCE </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<span class="mim-font">
- Autosomal recessive <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/258211005" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">258211005</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0441748&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0441748</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000007" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000007</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000007" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000007</a>]</span><br />
</span>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> HEAD & NECK </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<div>
<span class="h5 mim-font">
<em> Eyes </em>
</span>
</div>
<div style="margin-left: 2em;">
<span class="mim-font">
- Abnormal saccades <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1856499&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1856499</a>]</span><br /> -
Abnormal smooth pursuit <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1836393&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1836393</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000617" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000617</a>]</span><br /> -
Nystagmus <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/563001" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">563001</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/H55.0" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">H55.0</a>, <a href="https://purl.bioontology.org/ontology/ICD10CM/H55.00" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">H55.00</a>]</span> <span class="mim-feature-ids hidden">[ICD9CM: <a href="https://purl.bioontology.org/ontology/ICD9CM/379.50" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">379.50</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0028738&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0028738</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000639" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000639</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000639" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000639</a>]</span><br /> -
Strabismus <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/22066006" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">22066006</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/H50.9" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">H50.9</a>, <a href="https://purl.bioontology.org/ontology/ICD10CM/H50.40" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">H50.40</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0038379&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0038379</a>, <a href="https://bioportal.bioontology.org/search?q=C2020541&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C2020541</a>, <a href="https://bioportal.bioontology.org/search?q=C1423541&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1423541</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000486" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000486</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000486" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000486</a>]</span><br /> -
Ptosis <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/11934000" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">11934000</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/29696001" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">29696001</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/H02.409" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">H02.409</a>, <a href="https://purl.bioontology.org/ontology/ICD10CM/H02.40" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">H02.40</a>, <a href="https://purl.bioontology.org/ontology/ICD10CM/H02.4" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">H02.4</a>]</span> <span class="mim-feature-ids hidden">[ICD9CM: <a href="https://purl.bioontology.org/ontology/ICD9CM/374.3" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">374.3</a>, <a href="https://purl.bioontology.org/ontology/ICD9CM/374.30" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">374.30</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0005745&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0005745</a>, <a href="https://bioportal.bioontology.org/search?q=C0033377&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0033377</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000508" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000508</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000508" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000508</a>]</span> <a href="https://elementsofmorphology.nih.gov/index.cgi?tid=76abf29563d4adc64d21da86221224b1" target="_blank" class="small mim-tip-eom" title="&lt;img src=&quot;https://elementsofmorphology.nih.gov/images/terms/Ptosis-small.jpg&quot;&gt; &lt;br/&gt;Further Information: &lt;a href=&quot;https://elementsofmorphology.nih.gov/index.cgi?tid=76abf29563d4adc64d21da86221224b1&quot target=&quot;_blank&quot onclick=&quot;gtag(\'event\', \'mim_outbound\', {\'name\': \'EOM\', \'domain\': \'elementsofmorphology.nih.gov\'})&quot;&gt;Elements of Morphology&lt;/a&gt;"><span class="glyphicon glyphicon-user" aria-hidden="true"></span></a><br />
</span>
</div>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> RESPIRATORY </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<span class="mim-font">
- Restrictive respiratory insufficiency (in some patients) <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C3277226&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C3277226</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002091" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002091</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002091" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002091</a>]</span><br />
</span>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> GENITOURINARY </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<div>
<span class="h5 mim-font">
<em> Bladder </em>
</span>
</div>
<div style="margin-left: 2em;">
<span class="mim-font">
- Urinary urgency (in some patients) <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/75088002" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">75088002</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/R39.15" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">R39.15</a>]</span> <span class="mim-feature-ids hidden">[ICD9CM: <a href="https://purl.bioontology.org/ontology/ICD9CM/788.63" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">788.63</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0085606&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0085606</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000012" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000012</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0000012" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0000012</a>]</span><br />
</span>
</div>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> SKELETAL </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<div>
<span class="h5 mim-font">
<em> Spine </em>
</span>
</div>
<div style="margin-left: 2em;">
<span class="mim-font">
- Kyphosis <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/71311003" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">71311003</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/414564002" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">414564002</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/413428007" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">413428007</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/M40.20" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">M40.20</a>, <a href="https://purl.bioontology.org/ontology/ICD10CM/Q76.41" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">Q76.41</a>]</span> <span class="mim-feature-ids hidden">[ICD9CM: <a href="https://purl.bioontology.org/ontology/ICD9CM/737.1" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">737.1</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0265673&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0265673</a>, <a href="https://bioportal.bioontology.org/search?q=C0022821&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0022821</a>, <a href="https://bioportal.bioontology.org/search?q=C2115817&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C2115817</a>, <a href="https://bioportal.bioontology.org/search?q=C0022822&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0022822</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002808" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002808</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002808" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002808</a>]</span><br /> -
Scoliosis <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/298382003" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">298382003</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/20944008" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">20944008</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/111266001" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">111266001</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/M41.9" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">M41.9</a>, <a href="https://purl.bioontology.org/ontology/ICD10CM/M41" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">M41</a>, <a href="https://purl.bioontology.org/ontology/ICD10CM/Q67.5" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">Q67.5</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0559260&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0559260</a>, <a href="https://bioportal.bioontology.org/search?q=C0036439&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0036439</a>, <a href="https://bioportal.bioontology.org/search?q=C0700208&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0700208</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002650" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002650</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002650" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002650</a>]</span><br />
</span>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<em> Feet </em>
</span>
</div>
<div style="margin-left: 2em;">
<span class="mim-font">
- Pes cavus <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/205091006" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">205091006</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/36755004" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">36755004</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/86900005" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">86900005</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/Q66.7" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">Q66.7</a>]</span> <span class="mim-feature-ids hidden">[ICD9CM: <a href="https://purl.bioontology.org/ontology/ICD9CM/736.73" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">736.73</a>, <a href="https://purl.bioontology.org/ontology/ICD9CM/754.71" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">754.71</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0728829&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0728829</a>, <a href="https://bioportal.bioontology.org/search?q=C0039273&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0039273</a>, <a href="https://bioportal.bioontology.org/search?q=C2239098&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C2239098</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001761" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001761</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001761" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001761</a>]</span> <a href="https://elementsofmorphology.nih.gov/index.cgi?tid=2ad12e53b20f47e5685234fa29da6610" target="_blank" class="small mim-tip-eom" title="&lt;img src=&quot;https://elementsofmorphology.nih.gov/images/terms/Pes_Cavus-small.jpg&quot;&gt; &lt;br/&gt;Further Information: &lt;a href=&quot;https://elementsofmorphology.nih.gov/index.cgi?tid=2ad12e53b20f47e5685234fa29da6610&quot target=&quot;_blank&quot onclick=&quot;gtag(\'event\', \'mim_outbound\', {\'name\': \'EOM\', \'domain\': \'elementsofmorphology.nih.gov\'})&quot;&gt;Elements of Morphology&lt;/a&gt;"><span class="glyphicon glyphicon-user" aria-hidden="true"></span></a><br />
</span>
</div>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> MUSCLE, SOFT TISSUES </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<span class="mim-font">
- Neurogenic changes seen on EMG <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C3808564&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C3808564</a>]</span><br />
</span>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> NEUROLOGIC </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<div>
<span class="h5 mim-font">
<em> Central Nervous System </em>
</span>
</div>
<div style="margin-left: 2em;">
<span class="mim-font">
- Cerebellar ataxia <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/85102008" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">85102008</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0007758&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0007758</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001251" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001251</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001251" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001251</a>]</span><br /> -
Gait ataxia <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/25136009" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">25136009</a>]</span> <span class="mim-feature-ids hidden">[ICD10CM: <a href="https://purl.bioontology.org/ontology/ICD10CM/R26.0" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD10CM\', \'domain\': \'bioontology.org\'})">R26.0</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0751837&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0751837</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002066" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002066</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002066" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002066</a>]</span><br /> -
Limb ataxia <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0750937&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0750937</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002070" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002070</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0002070" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0002070</a>]</span><br /> -
Dysarthria <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/8011004" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">8011004</a>]</span> <span class="mim-feature-ids hidden">[ICD9CM: <a href="https://purl.bioontology.org/ontology/ICD9CM/438.13" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">438.13</a>, <a href="https://purl.bioontology.org/ontology/ICD9CM/784.51" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'ICD9CM\', \'domain\': \'bioontology.org\'})">784.51</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0013362&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0013362</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001260" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001260</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001260" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001260</a>]</span><br /> -
Dysmetria <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/32566006" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">32566006</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0234162&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0234162</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001310" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001310</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001310" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001310</a>]</span><br /> -
Brisk lower limb reflexes (in some patients) <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C4013420&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C4013420</a>]</span><br /> -
Spasticity (in some patients) <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/221360009" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">221360009</a>, <a href="https://purl.bioontology.org/ontology/SNOMEDCT/397790002" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">397790002</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0026838&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0026838</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001257" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001257</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001257" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001257</a>]</span><br /> -
Impaired cognition (in some patients) <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/386806002" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">386806002</a>]</span> <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0338656&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0338656</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0100543" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0100543</a>]</span><br /> -
Cerebellar atrophy <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C0740279&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C0740279</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001272" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001272</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0001272" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0001272</a>]</span><br /> -
Pontine atrophy (in some patients) <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C4013621&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C4013621</a>]</span><br />
</span>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<em> Peripheral Nervous System </em>
</span>
</div>
<div style="margin-left: 2em;">
<span class="mim-font">
- Axonal peripheral neuropathy, mild (in some patients) <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C4538409&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C4538409</a>]</span> <span class="mim-feature-ids hidden">[SNOMEDCT: <a href="https://purl.bioontology.org/ontology/SNOMEDCT/128208007" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'SNOMEDCT\', \'domain\': \'bioontology.org\'})">128208007</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0003477" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0003477</a>]</span><br /> -
Impaired vibration sense (in some patients) <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C4229246&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C4229246</a>]</span><br />
</span>
</div>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> MISCELLANEOUS </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<span class="mim-font">
- Variable age at onset, usually in second decade (range 6 to 40 years)<br /> -
Highly variable phenotype <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1839039&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1839039</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 /> -
Some patients have pure cerebellar ataxia<br /> -
Some patients have more a more complicated phenotype with spasticity, respiratory insufficiency, or cognitive impairment<br /> -
Slowly progressive <span class="mim-feature-ids hidden">[UMLS: <a href="https://bioportal.bioontology.org/search?q=C1854494&searchproperties=true" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'UMLS\', \'domain\': \'bioontology.org\'})">C1854494</a> HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0003677" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0003677</a>]</span> <span class="mim-feature-ids hidden">[HPO: <a href="https://hpo.jax.org/app/browse/term/HP:0003677" target="_blank" onclick="gtag(\'event\', \'mim_outbound\', {\'name\': \'HPO\', \'domain\': \'hpo.jax.org\'})">HP:0003677</a>]</span><br />
</span>
</div>
</div>
</div>
<div>
<div>
<span class="h5 mim-font">
<strong> MOLECULAR BASIS </strong>
</span>
</div>
<div style="margin-left: 2em;">
<div>
<span class="mim-font">
- Caused by mutation in the synaptic nuclear envelope protein-1 gene (SYNE1, <a href="/entry/608441#0001">608441.0001</a>)<br />
</span>
</div>
</div>
</div>
<div class="text-right">
<a href="#mimClinicalSynopsisFold" data-toggle="collapse">&#9650;&nbsp;Close</a>
</div>
</div>
</div>
<div id="mimPhenotypicSeriesFold" class="well well-sm collapse mimSingletonToggleFold">
<div class="small">
<div class="row">
<div class="col-lg-12 col-md-12 col-sm-12 col-xs-12">
<h5>
Spinocerebellar ataxia, autosomal recessive
- <a href="/phenotypicSeries/PS213200">PS213200</a>
- 32 Entries
</h5>
</div>
</div>
<div class="row" style="margin-left: 0.125em; margin-right: 0.125em;">
<table class="table table-bordered table-condensed table-hover mim-table-padding">
<thead>
<tr>
<th class="col-lg-1 col-md-1 col-sm-1 col-xs-1 text-nowrap">
<strong>Location</strong>
</th>
<th class="col-lg-5 col-md-5 col-sm-5 col-xs-6 text-nowrap">
<strong>Phenotype</strong>
</th>
<th class="col-lg-1 col-md-1 col-sm-1 col-xs-1 text-nowrap">
<strong>Inheritance</strong>
</th>
<th class="col-lg-1 col-md-1 col-sm-1 col-xs-1 text-nowrap">
<strong>Phenotype<br />mapping key</strong>
</th>
<th class="col-lg-1 col-md-1 col-sm-1 col-xs-1 text-nowrap">
<strong>Phenotype<br />MIM number</strong>
</th>
<th class="col-lg-1 col-md-1 col-sm-1 col-xs-1 text-nowrap">
<strong>Gene/Locus</strong>
</th>
<th class="col-lg-1 col-md-1 col-sm-1 col-xs-1 text-nowrap">
<strong>Gene/Locus<br />MIM number</strong>
</th>
</tr>
</thead>
<tbody>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/1/167?start=-3&limit=10&highlight=167"> 1p36.22-p36.21 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607317"> Spinocerebellar ataxia, autosomal recessive 4 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607317"> 607317 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608877"> VPS13D </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608877"> 608877 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/1/336?start=-3&limit=10&highlight=336"> 1p36.11 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616291"> Lichtenstein-Knorr syndrome </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616291"> 616291 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/107310"> SLC9A1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/107310"> 107310 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/1/967?start=-3&limit=10&highlight=967"> 1p12 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618369"> Spinocerebellar ataxia, autosomal recessive 27 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618369"> 618369 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618128"> GDAP2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618128"> 618128 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/1/1672?start=-3&limit=10&highlight=1672"> 1q32.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614229"> ?Spinocerebellar ataxia, autosomal recessive 11 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614229"> 614229 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/610949"> SYT14 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/610949"> 610949 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/1/1764?start=-3&limit=10&highlight=1764"> 1q42.13 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/612016"> Coenzyme Q10 deficiency, primary, 4 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/612016"> 612016 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/606980"> COQ8 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/606980"> 606980 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/2/493?start=-3&limit=10&highlight=493"> 2q11.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616948"> ?Spinocerebellar ataxia, autosomal recessive 22 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616948"> 616948 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614884"> VWA3B </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614884"> 614884 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/3/62?start=-3&limit=10&highlight=62"> 3p25.3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619422"> Spinocerebellar ataxia, autosomal recessive 31 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619422"> 619422 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608760"> ATG7 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608760"> 608760 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/3/216?start=-3&limit=10&highlight=216"> 3p22.1-p21.33 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613728"> Spinocerebellar ataxia, autosomal recessive 10 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613728"> 613728 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613726"> ANO10 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613726"> 613726 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/3/688?start=-3&limit=10&highlight=688"> 3q22.1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/617133"> ?Spinocerebellar ataxia, autosomal recessive 24 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/617133"> 617133 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/610552"> UBA5 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/610552"> 610552 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/3/1010?start=-3&limit=10&highlight=1010"> 3q29 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/615705"> Spinocerebellar ataxia, autosomal recessive 15 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/615705"> 615705 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613516"> RUBCN </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613516"> 613516 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/4/414?start=-3&limit=10&highlight=414"> 4q22.1-q22.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616204"> Spinocerebellar ataxia, autosomal recessive 18 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616204"> 616204 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/602368"> GRID2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/602368"> 602368 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/5/715?start=-3&limit=10&highlight=715"> 5q33.3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618800"> Spinocerebellar ataxia, autosomal recessive 28 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618800"> 618800 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618802"> THG1L </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618802"> 618802 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/6/70?start=-3&limit=10&highlight=70"> 6p23-p21 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/271250"> Spinocerebellar ataxia, autosomal recessive 3 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="2 - The disorder was placed on the map by statistical methods"> 2 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/271250"> 271250 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/271250"> SCAR3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/271250"> 271250 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/6/116?start=-3&limit=10&highlight=116"> 6p22.3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616949"> Spinocerebellar ataxia, autosomal recessive 23 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616949"> 616949 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/605764"> TDP2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/605764"> 605764 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/6/684?start=-3&limit=10&highlight=684"> 6q14.3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616354"> Spinocerebellar ataxia, autosomal recessive 20 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616354"> 616354 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616105"> SNX14 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616105"> 616105 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/6/747?start=-3&limit=10&highlight=747"> 6q21 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/617584"> ?Spinocerebellar ataxia, autosomal recessive 25 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/617584"> 617584 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604261"> ATG5 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604261"> 604261 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/6/928?start=-3&limit=10&highlight=928"> 6q24.3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614831"> Spinocerebellar ataxia, autosomal recessive 13 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614831"> 614831 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604473"> GRM1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604473"> 604473 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/6/963?start=-3&limit=10&highlight=963"> 6q25.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/610743"> Spinocerebellar ataxia, autosomal recessive 8 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/610743"> 610743 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608441"> SYNE1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608441"> 608441 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/7/204?start=-3&limit=10&highlight=204"> 7p14.1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619389"> Spinocerebellar ataxia, autosomal recessive 29 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619389"> 619389 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/605485"> VPS41 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/605485"> 605485 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/8/291?start=-3&limit=10&highlight=291"> 8q12.1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613227"> Spinocerebellar ataxia, autosomal recessive 34 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613227"> 613227 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/114815"> CA8 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/114815"> 114815 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/9/653?start=-3&limit=10&highlight=653"> 9q34.3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/213200"> Spinocerebellar ataxia, autosomal recessive 2 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/213200"> 213200 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613036"> PMPCA </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/613036"> 613036 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/10/16?start=-3&limit=10&highlight=16"> 10p15.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619405"> Spinocerebellar ataxia, autosomal recessive 30 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619405"> 619405 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618211"> PITRM1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/618211"> 618211 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/10/475?start=-3&limit=10&highlight=475"> 10q24.31 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616127"> Spinocerebellar ataxia, autosomal recessive 17 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616127"> 616127 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616120"> CWF19L1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616120"> 616120 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/10/609?start=-3&limit=10&highlight=609"> 10q26.11 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619862"> Spinocerebellar ataxia, autosomal recessive 32 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/619862"> 619862 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604769"> PRDX3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604769"> 604769 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/11/136?start=-3&limit=10&highlight=136"> 11p15.4 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/609270"> Spinocerebellar ataxia, autosomal recessive 7 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/609270"> 609270 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607998"> TPP1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607998"> 607998 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/11/594?start=-3&limit=10&highlight=594"> 11q13.1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616719"> Spinocerebellar ataxia, autosomal recessive 21 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/616719"> 616719 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607982"> SCYL1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607982"> 607982 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/11/646?start=-3&limit=10&highlight=646"> 11q13.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/615386"> Spinocerebellar ataxia, autosomal recessive 14 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/615386"> 615386 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604985"> SPTBN2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/604985"> 604985 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/16/37?start=-3&limit=10&highlight=37"> 16p13.3 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/615768"> Spinocerebellar ataxia, autosomal recessive 16 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/615768"> 615768 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607207"> STUB1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/607207"> 607207 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/16/666?start=-3&limit=10&highlight=666"> 16q23.1-q23.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614322"> Spinocerebellar ataxia, autosomal recessive 12 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/614322"> 614322 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/605131"> WWOX </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/605131"> 605131 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/19/777?start=-3&limit=10&highlight=777"> 19q13.31 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/617633"> ?Spinocerebellar ataxia, autosomal recessive 26 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/617633"> 617633 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/194360"> XRCC1 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/194360"> 194360 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/20/175?start=-3&limit=10&highlight=175"> 20q11-q13 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608029"> Spinocerebellar ataxia, autosomal recessive 6 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="2 - The disorder was placed on the map by statistical methods"> 2 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608029"> 608029 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608029"> SCAR6 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/608029"> 608029 </a>
</span>
</td>
</tr>
<tr>
<td>
<span class="mim-font">
<a href="/geneMap/22/350?start=-3&limit=10&highlight=350"> 22q13.2 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/620208"> ?Spinocerebellar ataxia, autosomal recessive 33 </a>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="Autosomal recessive">AR</abbr>
</span>
</td>
<td>
<span class="mim-font">
<abbr class="mim-tip-hint" title="3 - The molecular basis of the disorder is known"> 3 </abbr>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/620208"> 620208 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/620204"> RNU12 </a>
</span>
</td>
<td>
<span class="mim-font">
<a href="/entry/620204"> 620204 </a>
</span>
</td>
</tr>
</tbody>
</table>
</div>
<div class="text-right small">
<a href="#mimPhenotypicSeriesFold" data-toggle="collapse">&#9650;&nbsp;Close</a>
</div>
</div>
</div>
</div>
<div>
<br />
</div>
<div>
<a id="text" class="mim-anchor"></a>
<h4 href="#mimTextFold" id="mimTextToggle" class="mimTriangleToggle" style="cursor: pointer;" data-toggle="collapse">
<span id="mimTextToggleTriangle" class="small mimTextToggleTriangle">&#9660;</span>
<span class="mim-font">
<span class="mim-tip-floating" qtip_title="<strong>Looking For More References?</strong>" qtip_text="Click the 'reference plus' icon &lt;span class='glyphicon glyphicon-plus-sign'&gt;&lt;/span&gt at the end of each OMIM text paragraph to see more references related to the content of the preceding paragraph.">
<strong>TEXT</strong>
</span>
</span>
</h4>
<div id="mimTextFold" class="collapse in ">
<span class="mim-text-font">
<p>A number sign (#) is used with this entry because of evidence that autosomal recessive spinocerebellar ataxia-8 (SCAR8) is caused by homozygous or compound heterozygous mutation in the SYNE1 gene (<a href="/entry/608441">608441</a>) on chromosome 6q25.</p>
</span>
<div>
<br />
</div>
</div>
<div>
<a id="description" class="mim-anchor"></a>
<h4 href="#mimDescriptionFold" id="mimDescriptionToggle" class="mimTriangleToggle" style="cursor: pointer;" data-toggle="collapse">
<span id="mimDescriptionToggleTriangle" class="small mimTextToggleTriangle">&#9660;</span>
<span class="mim-font">
<strong>Description</strong>
</span>
</h4>
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<div id="mimDescriptionFold" class="collapse in ">
<span class="mim-text-font">
<p>Autosomal recessive spinocerebellar ataxia-8 (SCAR8) is a slowly progressive neurodegenerative disorder characterized by gait ataxia and other cerebellar signs, such as nystagmus and dysarthria. The age at onset is highly variable, and but most often is in the second or third decades. The disorder was initially identified in patients of French Canadian descent, most of whom have a relatively 'pure' form of the disorder. However, subsequent studies have shown that SCAR8 occurs worldwide and most commonly manifests with additional features, including spasticity, secondary musculoskeletal abnormalities, and ocular movement anomalies, consistent with a 'complicated' phenotype. Brain imaging typically shows cerebellar atrophy, sometimes with pontine involvement. Rare patients may have an early-onset multisystemic disorder with impaired intellectual development and respiratory dysfunction (summary by <a href="#4" class="mim-tip-reference" title="Synofzik, M., Smets, K., Mallaret, M., Di Bella, D., Gallenmuller, C., Baets, J., Schulze, M., Magri, S., Sarto, E., Mustafa, M., Deconinck, T., Haack, T., and 18 others. &lt;strong&gt;SYNE1 ataxia is a common recessive ataxia with major non-cerebellar features: a large multi-centre study.&lt;/strong&gt; Brain 139: 1378-1393, 2016.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/27086870/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;27086870&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1093/brain/aww079&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="27086870">Synofzik et al., 2016</a>). <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=27086870" 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>
</span>
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<br />
</div>
</div>
<div>
<a id="clinicalFeatures" class="mim-anchor"></a>
<h4 href="#mimClinicalFeaturesFold" id="mimClinicalFeaturesToggle" class="mimTriangleToggle" style="cursor: pointer;" data-toggle="collapse">
<span id="mimClinicalFeaturesToggleTriangle" class="small mimTextToggleTriangle">&#9660;</span>
<span class="mim-font">
<strong>Clinical Features</strong>
</span>
</h4>
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<div id="mimClinicalFeaturesFold" class="collapse in mimTextToggleFold">
<span class="mim-text-font">
<p><a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> identified a geographically defined group of 26 French Canadian families, including 53 affected family members, most of which originated from the Beauce and Bas-St-Laurent regions of the province of Quebec, Canada. All of the affected family members had a similar phenotype, which consisted of late-onset cerebellar ataxia with slow progression accompanied by dysarthria, with few associated features other than dysmetria, occasional brisk lower-extremity tendon reflexes, and minor abnormalities in saccades and smooth pursuit. <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> remarked that none of the subjects showed optic atrophy, auditory loss, sensory abnormalities, autonomic disturbances, or extrapyramidal signs. Nerve conduction studies carried out in 18 affected individuals were all within normal limits. Imaging by computed tomography (CT) or magnetic resonance imaging (MRI) invariably showed diffuse pure cerebellar atrophy. Therefore this disorder represented the first 'pure' autosomal recessive cerebellar ataxia mapped to that time. <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> designated this phenotype autosomal recessive cerebellar ataxia type 1 (ARCA1), also known as recessive ataxia of Beauce. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17159980" 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="Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H. &lt;strong&gt;Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.&lt;/strong&gt; Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/23325900/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;23325900&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1212/WNL.0b013e3182815529&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="23325900">Izumi et al. (2013)</a> reported 2 unrelated Japanese patients, each born of consanguineous parents, with onset of pure cerebellar ataxia at ages 36 and 27 years, respectively. Brain imaging in both patients showed cerebellar atrophy. The phenotype was similar to that reported by <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a>. <a href="#3" class="mim-tip-reference" title="Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H. &lt;strong&gt;Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.&lt;/strong&gt; Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/23325900/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;23325900&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1212/WNL.0b013e3182815529&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="23325900">Izumi et al. (2013)</a> noted that these were the first published patients with genetically confirmed SCAR8 outside of the French Canadian population. <a href="https://pubmed.ncbi.nlm.nih.gov/?term=17159980+23325900" 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><strong><em>Clinical Variability</em></strong></p><p>
<a href="#3" class="mim-tip-reference" title="Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H. &lt;strong&gt;Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.&lt;/strong&gt; Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/23325900/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;23325900&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1212/WNL.0b013e3182815529&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="23325900">Izumi et al. (2013)</a> reported a Japanese woman, born of consanguineous parents, with a severe variant of SCAR8. She presented at age 8 years with difficulty running, followed by distal dominant limb weakness and muscular atrophy, hyperreflexia, spastic ataxia, pes cavus, decreased Achilles tendon reflex, and decreased vibration sense. Brain MRI at age 19 showed cerebellar and brainstem atrophy. Other features included tongue fasciculation, tongue atrophy, and dysarthria. As an adult, her respiratory function was compromised, necessitating a tracheotomy. She died suddenly at age 44. The diagnosis was SCA with motor neuron disease; autopsy was not performed. Genetic analysis identified a homozygous truncating mutation in the SYNE1 gene and a homozygous missense variant (G185R) in the N-terminal region of SYNE1. Functional studies were not performed, but <a href="#3" class="mim-tip-reference" title="Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H. &lt;strong&gt;Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.&lt;/strong&gt; Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/23325900/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;23325900&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1212/WNL.0b013e3182815529&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="23325900">Izumi et al. (2013)</a> suggested that both mutations contributed to the more complex motor neuron phenotype in this patient. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=23325900" 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="#4" class="mim-tip-reference" title="Synofzik, M., Smets, K., Mallaret, M., Di Bella, D., Gallenmuller, C., Baets, J., Schulze, M., Magri, S., Sarto, E., Mustafa, M., Deconinck, T., Haack, T., and 18 others. &lt;strong&gt;SYNE1 ataxia is a common recessive ataxia with major non-cerebellar features: a large multi-centre study.&lt;/strong&gt; Brain 139: 1378-1393, 2016.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/27086870/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;27086870&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1093/brain/aww079&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="27086870">Synofzik et al. (2016)</a> reported 23 probands of European descent, none of whom were French Canadian, with SCAR8. Twenty-two of the patients had biallelic truncating alleles, and 1 was compound heterozygous for a missense and a truncating allele. Five probands were from multiplex families, whereas 18 were simplex cases with no family history of the disorder. Most patients had onset in the second or third decades, although a few had onset as early as 6 years or as late as 40. All had cerebellar ataxia with gait disturbances, and most (81%) had additional upper motor neuron signs, most often spasticity of the lower limbs and/or lower limb weakness and muscle atrophy. Additional common features included urinary urge incontinence, scoliosis, kyphosis, pes cavus, and ocular anomalies such as slow saccades, ophthalmoparesis, ptosis, and strabismus. A few patients had mild axonal sensory or motor peripheral neuropathy, and some had dystonia of the upper limbs. Three patients, including 2 sibs, had a multisystem disorder with impaired intellectual development (IQ of 49 in 1 patient) and respiratory dysfunction, which resulted in death at age 36 years in 1. EMG, when performed, showed neurogenic changes, and muscle biopsy showed neurogenic atrophy without evidence of a primary muscle disorder. Brain imaging showed cerebellar atrophy in all patients, and PET imaging in 2 patients showed decreased metabolism in the pontine brainstem. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=27086870" 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 id="inheritance" class="mim-anchor"></a>
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<p>The transmission pattern of SCAR8 in the families reported by <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> and <a href="#3" class="mim-tip-reference" title="Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H. &lt;strong&gt;Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.&lt;/strong&gt; Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/23325900/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;23325900&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1212/WNL.0b013e3182815529&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="23325900">Izumi et al. (2013)</a> was consistent with autosomal recessive inheritance. <a href="https://pubmed.ncbi.nlm.nih.gov/?term=17159980+23325900" 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 id="mapping" class="mim-anchor"></a>
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<p><a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> performed genomewide linkage analysis of selected families, which showed only 1 marker, D6S476, with a maximum lod score above 3.0. Mapping studies established a minimum candidate interval of about 0.5 Mb on chromosome 6q. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17159980" 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 id="molecularGenetics" class="mim-anchor"></a>
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<p>The candidate interval established by <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> in French Canadian families with pure cerebellar ataxia contained only 1 gene, SYNE1 (<a href="/entry/608441">608441</a>), which spans over 0.5 Mb of genomic DNA. Screening of all exons and flanking intronic sequences of SYNE1 led to the identification of 2 disease-segregating SNPs that were not detected among 380 age- and ethnicity-matched control chromosomes. <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> concluded that these 2 variants may be causative mutations for ARCA1: 310067A-G (<a href="/entry/608441#0001">608441.0001</a>) and 306434A-G (<a href="/entry/608441#0002">608441.0002</a>). Both of these were intronic mutations shown to have functional consequences on the proper splicing of the gene and resulting in premature termination of the protein. Based on haplotype reconstructions of affected individuals from all of the other families, <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> identified 3 other different disease haplotypes, suggesting that other mutations could be associated with the disease. A second mutational screen by direct sequencing uncovered 3 additional mutations that segregated with their respective haplotypes and were all predicted to lead to premature termination of the protein: R2906X (<a href="/entry/608441#0003">608441.0003</a>), a 5-bp del (<a href="/entry/608441#0004">608441.0004</a>), and Q7640X (<a href="/entry/608441#0005">608441.0005</a>). These additional mutations were likewise not detected among 380 age- and ethnicity-matched control chromosomes. The finding of 5 different mutations in a relatively homogeneous population led <a href="#2" class="mim-tip-reference" title="Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.&lt;/strong&gt; Nature Genet. 39: 80-85, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17159980/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17159980&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1038/ng1927&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17159980">Gros-Louis et al. (2007)</a> to predict that mutations in the SYNE1 gene may be responsible for a substantial fraction of all adult-onset autosomal recessive ataxia syndromes with cerebellar atrophy. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17159980" 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="#1" class="mim-tip-reference" title="Dupre, N., Gros-Louis, F., Chrestian, N., Verreault, S., Brunet, D., de Verteuil, D., Brais, B., Bouchard, J.-P., Rouleau, G. A. &lt;strong&gt;Clinical and genetic study of autosomal recessive cerebellar ataxia type 1.&lt;/strong&gt; Ann. Neurol. 62: 93-98, 2007.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/17503513/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;17503513&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1002/ana.21143&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="17503513">Dupre et al. (2007)</a> identified 2 additional SYNE1 mutations (<a href="/entry/608441#0006">608441.0006</a>; <a href="/entry/608441#0007">608441.0007</a>) in French Canadian patients with SCAR8. A splice site mutation (<a href="/entry/608441#0002">608441.0002</a>) was the most common mutation, occurring at a frequency of 50.8% among 124 patients. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17503513" 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 2 unrelated Japanese patients with adult-onset SCAR8, <a href="#3" class="mim-tip-reference" title="Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H. &lt;strong&gt;Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.&lt;/strong&gt; Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/23325900/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;23325900&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1212/WNL.0b013e3182815529&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="23325900">Izumi et al. (2013)</a> identified different homozygous truncating mutations in the SYNE1 gene (see, e.g., <a href="/entry/608441#0015">608441.0015</a>). <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=23325900" 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>Among 23 non-French-Canadian probands with SCAR8, <a href="#4" class="mim-tip-reference" title="Synofzik, M., Smets, K., Mallaret, M., Di Bella, D., Gallenmuller, C., Baets, J., Schulze, M., Magri, S., Sarto, E., Mustafa, M., Deconinck, T., Haack, T., and 18 others. &lt;strong&gt;SYNE1 ataxia is a common recessive ataxia with major non-cerebellar features: a large multi-centre study.&lt;/strong&gt; Brain 139: 1378-1393, 2016.[PubMed: &lt;a href=&quot;https://pubmed.ncbi.nlm.nih.gov/27086870/&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;name&#x27;: &#x27;PubMed&#x27;, &#x27;domain&#x27;: &#x27;pubmed.ncbi.nlm.nih.gov&#x27;})&quot;&gt;27086870&lt;/a&gt;] [&lt;a href=&quot;https://doi.org/10.1093/brain/aww079&quot; target=&quot;_blank&quot; onclick=&quot;gtag(&#x27;event&#x27;, &#x27;mim_outbound&#x27;, {&#x27;destination&#x27;: &#x27;Publisher&#x27;})&quot;&gt;Full Text&lt;/a&gt;]" pmid="27086870">Synofzik et al. (2016)</a> identified 35 different homozygous or compound heterozygous mutations in the SYNE1 gene (see, e.g., <a href="/entry/608441#0016">608441.0016</a>-<a href="/entry/608441#0017">608441.0017</a>). There were 20 nonsense, 7 frameshift, and 7 splice site mutations, and only 1 missense mutation; mutations occurred throughout the gene. Twenty-two of the patients had biallelic truncating alleles, and 1 was compound heterozygous for a missense and a truncating allele. Five probands were from multiplex families, whereas 18 were simplex cases with no family history of the disorder. All mutations were confirmed by Sanger sequencing, and the mutations segregated with the disorder in families from whom DNA was available. Most of the mutations were absent in the dbSNP, 1000 Genomes Project, Exome Variant Server, and ExAC databases, although a few were observed at low frequencies. The missense variant (F220S) occurred at a highly conserved residue in the actin-binding domain and was absent from public databases. Analysis of patient cells from 1 family with a truncating and a frameshift mutation showed that the mutations resulted in nonsense-mediated mRNA decay, consistent with a loss of function. Muscle biopsy samples from 3 unrelated patients showed severely decreased or absent SYNE1 immunostaining, also consistent with a loss of protein. Functional studies of the variants and additional studies of patient cells were not performed, but all of the variants were predicted to result in a loss of function. The patients were ascertained from a cohort of 434 index patients from 36 different countries with autosomal recessive ataxia compiled from 7 different European ataxia centers. Those with genetically confirmed SCAR8 accounted for almost 5%, indicating that SCAR8 is more common than previously thought. The findings also indicated that the phenotype of SCAR8 more often than not includes additional complicating features. <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=27086870" 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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<strong>REFERENCES</strong>
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<a id="Dupre2007" class="mim-anchor"></a>
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Dupre, N., Gros-Louis, F., Chrestian, N., Verreault, S., Brunet, D., de Verteuil, D., Brais, B., Bouchard, J.-P., Rouleau, G. A.
<strong>Clinical and genetic study of autosomal recessive cerebellar ataxia type 1.</strong>
Ann. Neurol. 62: 93-98, 2007.
[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17503513/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17503513</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17503513" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
[<a href="https://doi.org/10.1002/ana.21143" target="_blank">Full Text</a>]
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<a id="2" class="mim-anchor"></a>
<a id="Gros-Louis2007" class="mim-anchor"></a>
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Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A.
<strong>Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.</strong>
Nature Genet. 39: 80-85, 2007.
[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/17159980/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">17159980</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=17159980" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
[<a href="https://doi.org/10.1038/ng1927" target="_blank">Full Text</a>]
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<a id="Izumi2013" class="mim-anchor"></a>
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Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H.
<strong>Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.</strong>
Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.
[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/23325900/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">23325900</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=23325900" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
[<a href="https://doi.org/10.1212/WNL.0b013e3182815529" target="_blank">Full Text</a>]
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<a id="Synofzik2016" class="mim-anchor"></a>
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Synofzik, M., Smets, K., Mallaret, M., Di Bella, D., Gallenmuller, C., Baets, J., Schulze, M., Magri, S., Sarto, E., Mustafa, M., Deconinck, T., Haack, T., and 18 others.
<strong>SYNE1 ataxia is a common recessive ataxia with major non-cerebellar features: a large multi-centre study.</strong>
Brain 139: 1378-1393, 2016.
[PubMed: <a href="https://pubmed.ncbi.nlm.nih.gov/27086870/" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">27086870</a>, <a href="https://pubmed.ncbi.nlm.nih.gov/?cmd=link&linkname=pubmed_pubmed&from_uid=27086870" target="_blank" onclick="gtag('event', 'mim_outbound', {'name': 'PubMed Related', 'domain': 'pubmed.ncbi.nlm.nih.gov'})">related citations</a>]
[<a href="https://doi.org/10.1093/brain/aww079" target="_blank">Full Text</a>]
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Cassandra L. Kniffin - updated : 07/01/2019
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Cassandra L. Kniffin - updated : 11/3/2014<br>Cassandra L. Kniffin - updated : 1/7/2008
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Victor A. McKusick : 2/2/2007
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carol : 07/12/2019
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carol : 07/11/2019<br>ckniffin : 07/01/2019<br>carol : 06/07/2017<br>carol : 11/13/2014<br>mcolton : 11/3/2014<br>mcolton : 11/3/2014<br>ckniffin : 11/3/2014<br>joanna : 10/4/2013<br>ckniffin : 11/1/2011<br>wwang : 1/22/2008<br>ckniffin : 1/7/2008<br>alopez : 2/2/2007
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<strong>#</strong> 610743
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SPINOCEREBELLAR ATAXIA, AUTOSOMAL RECESSIVE 8; SCAR8
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<em>Alternative titles; symbols</em>
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ATAXIA, RECESSIVE, OF BEAUCE<br />
CEREBELLAR ATAXIA, AUTOSOMAL RECESSIVE, TYPE 1; ARCA1
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<strong>ORPHA:</strong> 88644; &nbsp;
<strong>DO:</strong> 0111618; &nbsp;
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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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6q25.2
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Spinocerebellar ataxia, autosomal recessive 8
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610743
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Autosomal recessive
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3
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SYNE1
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608441
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<strong>TEXT</strong>
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<p>A number sign (#) is used with this entry because of evidence that autosomal recessive spinocerebellar ataxia-8 (SCAR8) is caused by homozygous or compound heterozygous mutation in the SYNE1 gene (608441) on chromosome 6q25.</p>
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<strong>Description</strong>
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<p>Autosomal recessive spinocerebellar ataxia-8 (SCAR8) is a slowly progressive neurodegenerative disorder characterized by gait ataxia and other cerebellar signs, such as nystagmus and dysarthria. The age at onset is highly variable, and but most often is in the second or third decades. The disorder was initially identified in patients of French Canadian descent, most of whom have a relatively 'pure' form of the disorder. However, subsequent studies have shown that SCAR8 occurs worldwide and most commonly manifests with additional features, including spasticity, secondary musculoskeletal abnormalities, and ocular movement anomalies, consistent with a 'complicated' phenotype. Brain imaging typically shows cerebellar atrophy, sometimes with pontine involvement. Rare patients may have an early-onset multisystemic disorder with impaired intellectual development and respiratory dysfunction (summary by Synofzik et al., 2016). </p>
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<strong>Clinical Features</strong>
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<p>Gros-Louis et al. (2007) identified a geographically defined group of 26 French Canadian families, including 53 affected family members, most of which originated from the Beauce and Bas-St-Laurent regions of the province of Quebec, Canada. All of the affected family members had a similar phenotype, which consisted of late-onset cerebellar ataxia with slow progression accompanied by dysarthria, with few associated features other than dysmetria, occasional brisk lower-extremity tendon reflexes, and minor abnormalities in saccades and smooth pursuit. Gros-Louis et al. (2007) remarked that none of the subjects showed optic atrophy, auditory loss, sensory abnormalities, autonomic disturbances, or extrapyramidal signs. Nerve conduction studies carried out in 18 affected individuals were all within normal limits. Imaging by computed tomography (CT) or magnetic resonance imaging (MRI) invariably showed diffuse pure cerebellar atrophy. Therefore this disorder represented the first 'pure' autosomal recessive cerebellar ataxia mapped to that time. Gros-Louis et al. (2007) designated this phenotype autosomal recessive cerebellar ataxia type 1 (ARCA1), also known as recessive ataxia of Beauce. </p><p>Izumi et al. (2013) reported 2 unrelated Japanese patients, each born of consanguineous parents, with onset of pure cerebellar ataxia at ages 36 and 27 years, respectively. Brain imaging in both patients showed cerebellar atrophy. The phenotype was similar to that reported by Gros-Louis et al. (2007). Izumi et al. (2013) noted that these were the first published patients with genetically confirmed SCAR8 outside of the French Canadian population. </p><p><strong><em>Clinical Variability</em></strong></p><p>
Izumi et al. (2013) reported a Japanese woman, born of consanguineous parents, with a severe variant of SCAR8. She presented at age 8 years with difficulty running, followed by distal dominant limb weakness and muscular atrophy, hyperreflexia, spastic ataxia, pes cavus, decreased Achilles tendon reflex, and decreased vibration sense. Brain MRI at age 19 showed cerebellar and brainstem atrophy. Other features included tongue fasciculation, tongue atrophy, and dysarthria. As an adult, her respiratory function was compromised, necessitating a tracheotomy. She died suddenly at age 44. The diagnosis was SCA with motor neuron disease; autopsy was not performed. Genetic analysis identified a homozygous truncating mutation in the SYNE1 gene and a homozygous missense variant (G185R) in the N-terminal region of SYNE1. Functional studies were not performed, but Izumi et al. (2013) suggested that both mutations contributed to the more complex motor neuron phenotype in this patient. </p><p>Synofzik et al. (2016) reported 23 probands of European descent, none of whom were French Canadian, with SCAR8. Twenty-two of the patients had biallelic truncating alleles, and 1 was compound heterozygous for a missense and a truncating allele. Five probands were from multiplex families, whereas 18 were simplex cases with no family history of the disorder. Most patients had onset in the second or third decades, although a few had onset as early as 6 years or as late as 40. All had cerebellar ataxia with gait disturbances, and most (81%) had additional upper motor neuron signs, most often spasticity of the lower limbs and/or lower limb weakness and muscle atrophy. Additional common features included urinary urge incontinence, scoliosis, kyphosis, pes cavus, and ocular anomalies such as slow saccades, ophthalmoparesis, ptosis, and strabismus. A few patients had mild axonal sensory or motor peripheral neuropathy, and some had dystonia of the upper limbs. Three patients, including 2 sibs, had a multisystem disorder with impaired intellectual development (IQ of 49 in 1 patient) and respiratory dysfunction, which resulted in death at age 36 years in 1. EMG, when performed, showed neurogenic changes, and muscle biopsy showed neurogenic atrophy without evidence of a primary muscle disorder. Brain imaging showed cerebellar atrophy in all patients, and PET imaging in 2 patients showed decreased metabolism in the pontine brainstem. </p>
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<strong>Inheritance</strong>
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<p>The transmission pattern of SCAR8 in the families reported by Gros-Louis et al. (2007) and Izumi et al. (2013) was consistent with autosomal recessive inheritance. </p>
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<strong>Mapping</strong>
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<p>Gros-Louis et al. (2007) performed genomewide linkage analysis of selected families, which showed only 1 marker, D6S476, with a maximum lod score above 3.0. Mapping studies established a minimum candidate interval of about 0.5 Mb on chromosome 6q. </p>
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<strong>Molecular Genetics</strong>
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<p>The candidate interval established by Gros-Louis et al. (2007) in French Canadian families with pure cerebellar ataxia contained only 1 gene, SYNE1 (608441), which spans over 0.5 Mb of genomic DNA. Screening of all exons and flanking intronic sequences of SYNE1 led to the identification of 2 disease-segregating SNPs that were not detected among 380 age- and ethnicity-matched control chromosomes. Gros-Louis et al. (2007) concluded that these 2 variants may be causative mutations for ARCA1: 310067A-G (608441.0001) and 306434A-G (608441.0002). Both of these were intronic mutations shown to have functional consequences on the proper splicing of the gene and resulting in premature termination of the protein. Based on haplotype reconstructions of affected individuals from all of the other families, Gros-Louis et al. (2007) identified 3 other different disease haplotypes, suggesting that other mutations could be associated with the disease. A second mutational screen by direct sequencing uncovered 3 additional mutations that segregated with their respective haplotypes and were all predicted to lead to premature termination of the protein: R2906X (608441.0003), a 5-bp del (608441.0004), and Q7640X (608441.0005). These additional mutations were likewise not detected among 380 age- and ethnicity-matched control chromosomes. The finding of 5 different mutations in a relatively homogeneous population led Gros-Louis et al. (2007) to predict that mutations in the SYNE1 gene may be responsible for a substantial fraction of all adult-onset autosomal recessive ataxia syndromes with cerebellar atrophy. </p><p>Dupre et al. (2007) identified 2 additional SYNE1 mutations (608441.0006; 608441.0007) in French Canadian patients with SCAR8. A splice site mutation (608441.0002) was the most common mutation, occurring at a frequency of 50.8% among 124 patients. </p><p>In 2 unrelated Japanese patients with adult-onset SCAR8, Izumi et al. (2013) identified different homozygous truncating mutations in the SYNE1 gene (see, e.g., 608441.0015). </p><p>Among 23 non-French-Canadian probands with SCAR8, Synofzik et al. (2016) identified 35 different homozygous or compound heterozygous mutations in the SYNE1 gene (see, e.g., 608441.0016-608441.0017). There were 20 nonsense, 7 frameshift, and 7 splice site mutations, and only 1 missense mutation; mutations occurred throughout the gene. Twenty-two of the patients had biallelic truncating alleles, and 1 was compound heterozygous for a missense and a truncating allele. Five probands were from multiplex families, whereas 18 were simplex cases with no family history of the disorder. All mutations were confirmed by Sanger sequencing, and the mutations segregated with the disorder in families from whom DNA was available. Most of the mutations were absent in the dbSNP, 1000 Genomes Project, Exome Variant Server, and ExAC databases, although a few were observed at low frequencies. The missense variant (F220S) occurred at a highly conserved residue in the actin-binding domain and was absent from public databases. Analysis of patient cells from 1 family with a truncating and a frameshift mutation showed that the mutations resulted in nonsense-mediated mRNA decay, consistent with a loss of function. Muscle biopsy samples from 3 unrelated patients showed severely decreased or absent SYNE1 immunostaining, also consistent with a loss of protein. Functional studies of the variants and additional studies of patient cells were not performed, but all of the variants were predicted to result in a loss of function. The patients were ascertained from a cohort of 434 index patients from 36 different countries with autosomal recessive ataxia compiled from 7 different European ataxia centers. Those with genetically confirmed SCAR8 accounted for almost 5%, indicating that SCAR8 is more common than previously thought. The findings also indicated that the phenotype of SCAR8 more often than not includes additional complicating features. </p>
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<strong>REFERENCES</strong>
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Dupre, N., Gros-Louis, F., Chrestian, N., Verreault, S., Brunet, D., de Verteuil, D., Brais, B., Bouchard, J.-P., Rouleau, G. A.
<strong>Clinical and genetic study of autosomal recessive cerebellar ataxia type 1.</strong>
Ann. Neurol. 62: 93-98, 2007.
[PubMed: 17503513]
[Full Text: https://doi.org/10.1002/ana.21143]
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Gros-Louis, F., Dupre, N., Dion, P., Fox, M. A., Laurent, S., Verreault, S., Sanes, J. R., Bouchard, J.-P., Rouleau, G. A.
<strong>Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia.</strong>
Nature Genet. 39: 80-85, 2007.
[PubMed: 17159980]
[Full Text: https://doi.org/10.1038/ng1927]
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Izumi, Y., Miyamoto, R., Morino, H., Yoshizawa, A., Nishinaka, K., Udaka, F., Kameyama, M., Maruyama, H., Kawakami, H.
<strong>Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease.</strong>
Neurology 80: 600-601, 2013. Note: Erratum: Neurology 80: 1267 only, 2013.
[PubMed: 23325900]
[Full Text: https://doi.org/10.1212/WNL.0b013e3182815529]
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Synofzik, M., Smets, K., Mallaret, M., Di Bella, D., Gallenmuller, C., Baets, J., Schulze, M., Magri, S., Sarto, E., Mustafa, M., Deconinck, T., Haack, T., and 18 others.
<strong>SYNE1 ataxia is a common recessive ataxia with major non-cerebellar features: a large multi-centre study.</strong>
Brain 139: 1378-1393, 2016.
[PubMed: 27086870]
[Full Text: https://doi.org/10.1093/brain/aww079]
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