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<meta name="robots" content="INDEX,FOLLOW,NOARCHIVE" /><meta name="citation_inbook_title" content="GeneReviews® [Internet]" /><meta name="citation_title" content="Cerebrotendinous Xanthomatosis" /><meta name="citation_publisher" content="University of Washington, Seattle" /><meta name="citation_date" content="2024/11/14" /><meta name="citation_author" content="Antonio Federico" /><meta name="citation_author" content="Gian Nicola Gallus" /><meta name="citation_pmid" content="20301583" /><meta name="citation_fulltext_html_url" content="https://www.ncbi.nlm.nih.gov/books/NBK1409/" /><meta name="citation_keywords" content="Sterol 26-hydroxylase, mitochondrial" /><meta name="citation_keywords" content="CYP27A1" /><meta name="citation_keywords" content="Cerebrotendinous Xanthomatosis" /><link rel="schema.DC" href="http://purl.org/DC/elements/1.0/" /><meta name="DC.Title" content="Cerebrotendinous Xanthomatosis" /><meta name="DC.Type" content="Text" /><meta name="DC.Publisher" content="University of Washington, Seattle" /><meta name="DC.Contributor" content="Antonio Federico" /><meta name="DC.Contributor" content="Gian Nicola Gallus" /><meta name="DC.Date" content="2024/11/14" /><meta name="DC.Identifier" content="https://www.ncbi.nlm.nih.gov/books/NBK1409/" /><meta name="description" content="Cerebrotendinous xanthomatosis (CTX) is a lipid storage disease characterized by infantile-onset diarrhea, childhood-onset cataract, adolescent- to young adult-onset tendon xanthomas, and adult-onset progressive neurologic dysfunction (dementia, psychiatric disturbances, pyramidal and/or cerebellar signs, dystonia, atypical parkinsonism, peripheral neuropathy, and seizures). Chronic diarrhea from infancy and/or neonatal cholestasis may be the earliest clinical manifestation. In approximately 75% of affected individuals, cataracts are the first finding, often appearing in the first decade of life. Xanthomas appear in the second or third decade; they occur on the Achilles tendon, the extensor tendons of the elbow and hand, the patellar tendon, and the neck tendons. Xanthomas have been reported in the lung, bones, and central nervous system. Some individuals show cognitive impairment from early infancy, whereas the majority have normal or only slightly impaired intellectual function until puberty; dementia with slow deterioration in intellectual abilities occurs in the third decade in more than 50% of individuals. Neuropsychiatric symptoms such as behavioral changes, hallucinations, agitation, aggression, depression, and suicide attempts may be prominent. 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Xanthomas appear in the second or third decade; they occur on the Achilles tendon, the extensor tendons of the elbow and hand, the patellar tendon, and the neck tendons. Xanthomas have been reported in the lung, bones, and central nervous system. Some individuals show cognitive impairment from early infancy, whereas the majority have normal or only slightly impaired intellectual function until puberty; dementia with slow deterioration in intellectual abilities occurs in the third decade in more than 50% of individuals. Neuropsychiatric symptoms such as behavioral changes, hallucinations, agitation, aggression, depression, and suicide attempts may be prominent. 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<div class="pre-content"><div><div class="bk_prnt"><p class="small">NCBI Bookshelf. A service of the National Library of Medicine, National Institutes of Health.</p><p>Adam MP, Feldman J, Mirzaa GM, et al., editors. GeneReviews® [Internet]. Seattle (WA): University of Washington, Seattle; 1993-2025. </p></div><div class="iconblock clearfix whole_rhythm no_top_margin bk_noprnt"><a class="img_link icnblk_img" title="All GeneReviews" href="/books/n/gene/"><img class="source-thumb" src="/corehtml/pmc/pmcgifs/bookshelf/thumbs/th-gene-lrg.png" alt="Cover of GeneReviews®" height="100px" width="80px" /></a><div class="icnblk_cntnt eight_col"><h2>GeneReviews<sup>®</sup> [Internet].</h2><a data-jig="ncbitoggler" href="#__NBK1409_dtls__">Show details</a><div style="display:none" class="ui-widget" id="__NBK1409_dtls__"><div>Adam MP, Feldman J, Mirzaa GM, et al., editors.</div><div>Seattle (WA): <a href="http://www.washington.edu" ref="pagearea=page-banner&amp;targetsite=external&amp;targetcat=link&amp;targettype=publisher">University of Washington, Seattle</a>; 1993-2025.</div></div><div class="half_rhythm"><ul class="inline_list"><li style="margin-right:1em"><a class="bk_cntns" href="/books/n/gene/">GeneReviews by Title</a></li></ul></div><div class="bk_noprnt"><form method="get" action="/books/n/gene/" id="bk_srch"><div class="bk_search"><label for="bk_term" class="offscreen_noflow">Search term</label><input type="text" title="Search GeneReviews" id="bk_term" name="term" value="" data-jig="ncbiclearbutton" /> <input type="submit" class="jig-ncbibutton" value="Search GeneReviews" submit="false" style="padding: 0.1em 0.4em;" /></div></form><div><ul class="inline_list"><li><a href="/books/n/gene/advanced/">GeneReviews Advanced Search</a></li><li style="margin-left:.5em"><a href="/books/n/gene/helpadvsearch/">Help</a></li></ul></div></div></div><div class="icnblk_cntnt two_col"><div class="pagination bk_noprnt"><a class="active page_link prev" href="/books/n/gene/cco/" title="Previous page in this title">&lt; Prev</a><a class="active page_link next" href="/books/n/gene/char/" title="Next page in this title">Next &gt;</a></div></div></div></div></div>
<div class="main-content lit-style" itemscope="itemscope" itemtype="http://schema.org/CreativeWork"><div class="meta-content fm-sec"><h1 id="_NBK1409_"><span class="title" itemprop="name">Cerebrotendinous Xanthomatosis</span></h1><p class="contrib-group"><span itemprop="author">Antonio Federico</span>, MD and <span itemprop="author">Gian Nicola Gallus</span>, DSci.</p><a data-jig="ncbitoggler" href="#__NBK1409_ai__" style="border:0;text-decoration:none">Author Information and Affiliations</a><div style="display:none" class="ui-widget" id="__NBK1409_ai__"><div class="contrib half_rhythm"><span itemprop="author">Antonio Federico</span>, MD<div class="affiliation small">Department of Medicine, Surgery and NeurosciencesMedical SchoolUniversity of SienaSiena, Italy<div><span class="email-label">Email: </span><a href="mailto:dev@null" data-email="ti.isinu@ociredef" class="oemail">ti.isinu@ociredef</a></div></div></div><div class="contrib half_rhythm"><span itemprop="author">Gian Nicola Gallus</span>, DSci<div class="affiliation small">Department of Medicine, Surgery and NeurosciencesMedical SchoolUniversity of SienaSiena, Italy<div><span class="email-label">Email: </span><a href="mailto:dev@null" data-email="ti.isinu@2sullag" class="oemail">ti.isinu@2sullag</a></div></div></div></div><p class="small">Initial Posting: <span itemprop="datePublished">July 16, 2003</span>; Last Revision: <span itemprop="dateModified">November 14, 2024</span>.</p><p><em>Estimated reading time: 24 minutes</em></p></div><div class="jig-ncbiinpagenav body-content whole_rhythm" data-jigconfig="allHeadingLevels: ['h2'],smoothScroll: false" itemprop="text"><div id="ctx.Summary" itemprop="description"><h2 id="_ctx_Summary_">Summary</h2><div><h4 class="inline">Clinical characteristics.</h4><p>Cerebrotendinous xanthomatosis (CTX) is a lipid storage disease characterized by infantile-onset diarrhea, childhood-onset cataract, adolescent- to young adult-onset tendon xanthomas, and adult-onset progressive neurologic dysfunction (dementia, psychiatric disturbances, pyramidal and/or cerebellar signs, dystonia, atypical parkinsonism, peripheral neuropathy, and seizures). Chronic diarrhea from infancy and/or neonatal cholestasis may be the earliest clinical manifestation. In approximately 75% of affected individuals, cataracts are the first finding, often appearing in the first decade of life. Xanthomas appear in the second or third decade; they occur on the Achilles tendon, the extensor tendons of the elbow and hand, the patellar tendon, and the neck tendons. Xanthomas have been reported in the lung, bones, and central nervous system. Some individuals show cognitive impairment from early infancy, whereas the majority have normal or only slightly impaired intellectual function until puberty; dementia with slow deterioration in intellectual abilities occurs in the third decade in more than 50% of individuals. Neuropsychiatric symptoms such as behavioral changes, hallucinations, agitation, aggression, depression, and suicide attempts may be prominent. Pyramidal signs (i.e., spasticity) and/or cerebellar signs almost invariably become evident between ages 20 and 30 years.</p><p>The biochemical abnormalities that distinguish CTX from other conditions with xanthomas include high plasma and tissue cholestanol concentration, normal-to-low plasma cholesterol concentration, decreased chenodeoxycholic acid (CDCA), increased concentration of bile alcohols and their glyconjugates, and increased concentrations of cholestanol and apolipoprotein B in cerebrospinal fluid.</p></div><div><h4 class="inline">Diagnosis/testing.</h4><p>The diagnosis of CTX is established in a <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a> with suggestive findings and <a class="def" href="/books/n/gene/glossary/def-item/biallelic/">biallelic</a> pathogenic variants in <i>CYP27A1</i> identified by <a class="def" href="/books/n/gene/glossary/def-item/molecular-genetic-testing/">molecular genetic testing</a>.</p></div><div><h4 class="inline">Management.</h4><p><i>Targeted therapy:</i> Long-term treatment with chenodeoxycholic acid (CDCA) normalizes plasma and cerebrospinal fluid concentration of cholestanol and improves neurophysiologic findings.</p><p><i>Supportive treatment:</i> Inhibitors of 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase alone or in combination with CDCA are also effective in decreasing cholestanol concentration and improving clinical signs; however, they may induce muscle damage. Cholic acid treatment decreases cholestanol levels and improves neurologic symptoms in the few individuals in whom it has been tried and may be useful in those who experience side effects with CDCA treatments. Cataract extraction is typically required in at least one eye by age 50 years. Epilepsy, spasticity, and parkinsonism are treated symptomatically.</p><p><i>Surveillance:</i> Annual cholestanol plasma concentration, neurologic and neuropsychological evaluation, brain MRI, echocardiogram, and assessment of bone density.</p><p><i>Agents/circumstances to avoid:</i> Caution has been suggested with statins.</p><p><i>Evaluation of relatives at risk:</i> It is appropriate to clarify the genetic status of apparently asymptomatic older and younger at-risk relatives of an affected individual in order to identify as early as possible those who would benefit from prompt initiation of CDCA treatment and surveillance.</p><p><i>Pregnancy management:</i> Treatment with CDCA should not be interrupted during pregnancy.</p></div><div><h4 class="inline">Genetic counseling.</h4><p>CTX is inherited in an <a class="def" href="/books/n/gene/glossary/def-item/autosomal-recessive/">autosomal recessive</a> manner. If both parents are known to be <a class="def" href="/books/n/gene/glossary/def-item/heterozygous/">heterozygous</a> for a <i>CYP27A1</i> <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a>, each sib of an affected individual has at conception a 25% chance of being affected, a 50% chance of being a <a class="def" href="/books/n/gene/glossary/def-item/carrier/">carrier</a>, and a 25% chance of inheriting neither of the <a class="def" href="/books/n/gene/glossary/def-item/familial/">familial</a> pathogenic variants. Carrier testing for at-risk family members and prenatal and <a class="def" href="/books/n/gene/glossary/def-item/preimplantation-genetic-testing/">preimplantation genetic testing</a> are possible if both <i>CYP27A1</i> pathogenic variants in the family are known.</p></div></div><div id="ctx.Diagnosis"><h2 id="_ctx_Diagnosis_">Diagnosis</h2><p>A consensus paper on the diagnostic criteria and management of cerebrotendinous xanthomatosis (CTX) has been published [<a class="bk_pop" href="#ctx.REF.stelten.2021a.353">Stelten et al 2021a</a>] (<a href="https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8349076/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">full text</a>).</p><div id="ctx.Suggestive_Findings"><h3>Suggestive Findings</h3><p>CTX, a lipid storage disease, <b>should be suspected</b> in individuals with the following clinical, laboratory, imaging, and family history findings.</p><p>
<b>Clinical findings</b>
</p><ul><li class="half_rhythm"><div>Neonatal cholestasis</div></li><li class="half_rhythm"><div>Infantile-onset diarrhea</div></li><li class="half_rhythm"><div>Childhood-onset cataract</div></li><li class="half_rhythm"><div>Adolescent- to young adult-onset tendon xanthomas (<a class="figpopup" href="/books/NBK1409/figure/ctx.F1/?report=objectonly" target="object" rid-figpopup="figctxF1" rid-ob="figobctxF1">Figure 1</a>)</div></li><li class="half_rhythm"><div>Adult-onset progressive neurologic dysfunction (dementia, psychiatric disturbances, pyramidal and/or cerebellar signs, and seizures)</div></li></ul><div class="iconblock whole_rhythm clearfix ten_col fig" id="figctxF1" co-legend-rid="figlgndctxF1"><a href="/books/NBK1409/figure/ctx.F1/?report=objectonly" target="object" title="Figure 1. " class="img_link icnblk_img figpopup" rid-figpopup="figctxF1" rid-ob="figobctxF1"><img class="small-thumb" src="/books/NBK1409/bin/ctx-Image001.gif" src-large="/books/NBK1409/bin/ctx-Image001.jpg" alt="Figure 1. . Different localization and severity of tendon xanthomas in CTX." /></a><div class="icnblk_cntnt" id="figlgndctxF1"><h4 id="ctx.F1"><a href="/books/NBK1409/figure/ctx.F1/?report=objectonly" target="object" rid-ob="figobctxF1">Figure 1. </a></h4><p class="float-caption no_bottom_margin">Different localization and severity of tendon xanthomas in CTX. Besides the classic xanthomas of the Achilles tendon (A), xanthomas of the patellar tendon (B), the extensor tendons of the hand (C), and the extensor tendons of the elbow (D) have been observed. <a href="/books/NBK1409/figure/ctx.F1/?report=objectonly" target="object" rid-ob="figobctxF1">(more...)</a></p></div></div><p>
<b>Laboratory findings</b>
</p><ul><li class="half_rhythm"><div>High plasma and tissue cholestanol concentration (<a href="/books/NBK1409/table/ctx.T.biochemical_abnormalities_in_cereb/?report=objectonly" target="object" rid-ob="figobctxTbiochemicalabnormalitiesincereb">Table 1</a>)</div></li><li class="half_rhythm"><div>Normal-to-low plasma cholesterol concentration</div></li><li class="half_rhythm"><div>Markedly decreased formation of chenodeoxycholic acid as a result of impaired primary bile acid synthesis</div></li><li class="half_rhythm"><div>Increased concentration of bile alcohols and their glyconjugates in bile, urine, and plasma (<a href="/books/NBK1409/table/ctx.T.biochemical_abnormalities_in_cereb/?report=objectonly" target="object" rid-ob="figobctxTbiochemicalabnormalitiesincereb">Table 1</a>)</div></li><li class="half_rhythm"><div>Increased concentration of cholestanol and apolipoprotein B in cerebrospinal fluid</div></li><li class="half_rhythm"><div>Increased plasma lactate concentration</div></li></ul><div id="ctx.T.biochemical_abnormalities_in_cereb" class="table"><h3><span class="label">Table 1. </span></h3><div class="caption"><p>Biochemical Abnormalities in Cerebrotendinous Xanthomatosis</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.biochemical_abnormalities_in_cereb/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.biochemical_abnormalities_in_cereb_lrgtbl__"><table><thead><tr><th id="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_1" rowspan="2" scope="col" colspan="1" headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_1" style="text-align:left;vertical-align:middle;">Analyte</th><th id="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_2" rowspan="2" scope="col" colspan="1" headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_2" style="text-align:left;vertical-align:middle;">Source</th><th id="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3" colspan="2" scope="colgroup" rowspan="1" style="text-align:center;vertical-align:middle;">Concentration</th></tr><tr><th headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3" id="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_1" colspan="1" scope="colgroup" rowspan="1" style="text-align:left;vertical-align:middle;">In CTX</th><th headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3" id="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Normal</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Cholestanol</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Plasma &#x00026; tissue</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3 hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_1" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">&#x02264;5-10x normal</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3 hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">330&#x000b1;30 &#x000b5;g/dL</td></tr><tr><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_1" rowspan="2" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">Bile alcohols</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Urine</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3 hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_1" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">14,000&#x000b1;3500 nmol/L</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3 hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Not detectable</td></tr><tr><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Plasma</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3 hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_1" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">&#x02264;500-1000x normal</td><td headers="hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_1_3 hd_h_ctx.T.biochemical_abnormalities_in_cereb_1_1_2_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">8.48&#x000b1;3.67</td></tr></tbody></table></div></div><p>
<b>Brain imaging</b>
</p><ul><li class="half_rhythm"><div>Bilateral hyperintensity of the dentate nuclei and cerebral and cerebellar white matter (<a class="figpopup" href="/books/NBK1409/figure/ctx.F2/?report=objectonly" target="object" rid-figpopup="figctxF2" rid-ob="figobctxF2">Figure 2</a>) on brain MRI. Additional changes on brain CT and MRI include diffuse brain and cerebellar atrophy, white matter signal alterations, and bilateral focal cerebellar lesions.</div></li><li class="half_rhythm"><div>Increased brain lactate and decreased n-acetylaspartate concentration (by MR spectroscopy)</div></li></ul><div class="iconblock whole_rhythm clearfix ten_col fig" id="figctxF2" co-legend-rid="figlgndctxF2"><a href="/books/NBK1409/figure/ctx.F2/?report=objectonly" target="object" title="Figure 2. " class="img_link icnblk_img figpopup" rid-figpopup="figctxF2" rid-ob="figobctxF2"><img class="small-thumb" src="/books/NBK1409/bin/ctx-Image002.gif" src-large="/books/NBK1409/bin/ctx-Image002.jpg" alt="Figure 2. " /></a><div class="icnblk_cntnt" id="figlgndctxF2"><h4 id="ctx.F2"><a href="/books/NBK1409/figure/ctx.F2/?report=objectonly" target="object" rid-ob="figobctxF2">Figure 2. </a></h4><p class="float-caption no_bottom_margin">MRI findings in three persons with CTX A. Signal alterations of cerebral peduncle</p></div></div><p><b>Family history</b> is consistent with <a class="def" href="/books/n/gene/glossary/def-item/autosomal-recessive/">autosomal recessive</a> inheritance (e.g., affected sibs and/or parental <a class="def" href="/books/n/gene/glossary/def-item/consanguinity/">consanguinity</a>). Absence of a known family history does not preclude the diagnosis.</p></div><div id="ctx.Establishing_the_Diagnosis"><h3>Establishing the Diagnosis</h3><p>The diagnosis of CTX <b>is established</b> in a <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a> with suggestive findings and <a class="def" href="/books/n/gene/glossary/def-item/biallelic/">biallelic</a> pathogenic (or <a class="def" href="/books/n/gene/glossary/def-item/likely-pathogenic/">likely pathogenic</a>) variants in <i>CYP27A1</i> identified by <a class="def" href="/books/n/gene/glossary/def-item/molecular-genetic-testing/">molecular genetic testing</a> (see <a href="/books/NBK1409/table/ctx.T.molecular_genetic_testing_used_in/?report=objectonly" target="object" rid-ob="figobctxTmoleculargenetictestingusedin">Table 2</a>).</p><p>Note: (1) Per ACMG/AMP variant interpretation guidelines, the terms "<a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a>" and "<a class="def" href="/books/n/gene/glossary/def-item/likely-pathogenic/">likely pathogenic</a> variant" are synonymous in a clinical setting, meaning that both are considered diagnostic and can be used for clinical decision making [<a class="bk_pop" href="#ctx.REF.richards.2015.405">Richards et al 2015</a>]. Reference to "pathogenic variants" in this <i>GeneReview</i> is understood to include likely pathogenic variants. (2) Identification of <a class="def" href="/books/n/gene/glossary/def-item/biallelic/">biallelic</a> <i>CYP27A1</i> variants of <a class="def" href="/books/n/gene/glossary/def-item/uncertain-significance/">uncertain significance</a> (or of one known <i>CYP27A1</i> pathogenic variant and one <i>CYP27A1</i> variant of uncertain significance) does not establish or rule out the diagnosis.</p><p>Molecular genetic testing approaches can include a combination of <b><a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a>-targeted testing</b> (single-gene testing, <a class="def" href="/books/n/gene/glossary/def-item/multigene-panel/">multigene panel</a>) and <b>comprehensive</b>
<b><a class="def" href="/books/n/gene/glossary/def-item/genomic/">genomic</a> testing</b> (<a class="def" href="/books/n/gene/glossary/def-item/exome-sequencing/">exome sequencing</a>, <a class="def" href="/books/n/gene/glossary/def-item/genome-sequencing/">genome sequencing</a>) depending on the <a class="def" href="/books/n/gene/glossary/def-item/phenotype/">phenotype</a>.</p><p>Gene-targeted testing requires that the clinician determine which <a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a>(s) are likely involved, whereas <a class="def" href="/books/n/gene/glossary/def-item/genomic/">genomic</a> testing does not. Individuals with the distinctive findings described in <a href="#ctx.Suggestive_Findings">Suggestive Findings</a> are likely to be diagnosed using gene-targeted testing (see <a href="#ctx.Option_1">Option 1</a>), whereas those in whom the diagnosis of CTX has not been considered are more likely to be diagnosed using genomic testing (see <a href="#ctx.Option_2">Option 2</a>).</p><div id="ctx.Option_1"><h4>Option 1</h4><p><b>Single-<a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a> testing.</b> Sequence analysis of <i>CYP27A1</i> is performed first to detect <a class="def" href="/books/n/gene/glossary/def-item/missense/">missense</a>, <a class="def" href="/books/n/gene/glossary/def-item/nonsense-variant/">nonsense</a>, and <a class="def" href="/books/n/gene/glossary/def-item/splice-site/">splice site</a> variants and small intragenic deletions/insertions. Note: Depending on the sequencing method used, single-<a class="def" href="/books/n/gene/glossary/def-item/exon/">exon</a>, multiexon, or whole-gene deletions/duplications may not be detected. If only one or no variant is detected by the sequencing method used, the next step is to perform gene-targeted <a class="def" href="/books/n/gene/glossary/def-item/deletion-duplication-analysis/">deletion/duplication analysis</a> to detect exon and whole-gene deletions or duplications.</p><p><b>A <a class="def" href="/books/n/gene/glossary/def-item/multigene-panel/">multigene panel</a></b> that includes <i>CYP27A1</i> and other genes of interest (see <a href="#ctx.Differential_Diagnosis">Differential Diagnosis</a>) is most likely to identify the genetic cause of the condition while limiting identification of variants of <a class="def" href="/books/n/gene/glossary/def-item/uncertain-significance/">uncertain significance</a> and pathogenic variants in genes that do not explain the underlying <a class="def" href="/books/n/gene/glossary/def-item/phenotype/">phenotype</a>. Note: (1) The genes included in the panel and the diagnostic <a class="def" href="/books/n/gene/glossary/def-item/sensitivity/">sensitivity</a> of the testing used for each <a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a> vary by laboratory and are likely to change over time. (2) Some multigene panels may include genes not associated with the condition discussed in this <i>GeneReview</i>. (3) In some laboratories, panel options may include a custom laboratory-designed panel and/or custom phenotype-focused <a class="def" href="/books/n/gene/glossary/def-item/exome/">exome</a> analysis that includes genes specified by the clinician. (4) Methods used in a panel may include <a class="def" href="/books/n/gene/glossary/def-item/sequence-analysis/">sequence analysis</a>, <a class="def" href="/books/n/gene/glossary/def-item/deletion-duplication-analysis/">deletion/duplication analysis</a>, and/or other non-sequencing-based tests.</p><p>For an introduction to multigene panels click <a href="/books/n/gene/app5/#app5.Multigene_Panels">here</a>. More detailed information for clinicians ordering genetic tests can be found <a href="/books/n/gene/app5/#app5.Multigene_Panels_FAQs">here</a>.</p></div><div id="ctx.Option_2"><h4>Option 2</h4><p><b>Comprehensive</b>
<b><a class="def" href="/books/n/gene/glossary/def-item/genomic/">genomic</a> testing</b> does not require the clinician to determine which <a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a> is likely involved. <b>Exome sequencing</b> is most commonly used; <b><a class="def" href="/books/n/gene/glossary/def-item/genome-sequencing/">genome sequencing</a></b> is also possible.</p><p>For an introduction to comprehensive <a class="def" href="/books/n/gene/glossary/def-item/genomic/">genomic</a> testing click <a href="/books/n/gene/app5/#app5.Comprehensive_Genomic_Testing">here</a>. More detailed information for clinicians ordering genomic testing can be found <a href="/books/n/gene/app5/#app5.Comprehensive_Genomic_Testing_1">here</a>.</p><div id="ctx.T.molecular_genetic_testing_used_in" class="table"><h3><span class="label">Table 2. </span></h3><div class="caption"><p>Molecular Genetic Testing Used in Cerebrotendinous Xanthomatosis</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.molecular_genetic_testing_used_in/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.molecular_genetic_testing_used_in_lrgtbl__"><table class="no_bottom_margin"><thead><tr><th id="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Gene&#x000a0;<sup>1</sup></th><th id="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Method</th><th id="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_3" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Proportion of Pathogenic Variants&#x000a0;<sup>2</sup> Identified by Method</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_1" rowspan="2" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">
<i>CYP27A1</i>
</td><td headers="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Sequence analysis&#x000a0;<sup>3</sup></td><td headers="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">99%&#x000a0;<sup>4</sup></td></tr><tr><td headers="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Gene-targeted <a class="def" href="/books/n/gene/glossary/def-item/deletion-duplication-analysis/">deletion/duplication analysis</a>&#x000a0;<sup>5</sup></td><td headers="hd_h_ctx.T.molecular_genetic_testing_used_in_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">1%&#x000a0;<sup>4</sup></td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt>1. </dt><dd><div id="ctx.TF.2.1"><p class="no_margin">See <a href="/books/NBK1409/#ctx.molgen.TA">Table A. Genes and Databases</a> for <a class="def" href="/books/n/gene/glossary/def-item/chromosome/">chromosome</a> <a class="def" href="/books/n/gene/glossary/def-item/locus/">locus</a> and protein.</p></div></dd><dt>2. </dt><dd><div id="ctx.TF.2.2"><p class="no_margin">See <a href="#ctx.Molecular_Genetics">Molecular Genetics</a> for information on variants detected in this <a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a>.</p></div></dd><dt>3. </dt><dd><div id="ctx.TF.2.3"><p class="no_margin">Sequence analysis detects variants that are benign, <a class="def" href="/books/n/gene/glossary/def-item/likely-benign/">likely benign</a>, of <a class="def" href="/books/n/gene/glossary/def-item/uncertain-significance/">uncertain significance</a>, <a class="def" href="/books/n/gene/glossary/def-item/likely-pathogenic/">likely pathogenic</a>, or pathogenic. Variants may include <a class="def" href="/books/n/gene/glossary/def-item/missense/">missense</a>, <a class="def" href="/books/n/gene/glossary/def-item/nonsense-variant/">nonsense</a>, and <a class="def" href="/books/n/gene/glossary/def-item/splice-site/">splice site</a> variants and small intragenic deletions/insertions; typically, <a class="def" href="/books/n/gene/glossary/def-item/exon/">exon</a> or whole-<a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a> deletions/duplications are not detected. For issues to consider in interpretation of <a class="def" href="/books/n/gene/glossary/def-item/sequence-analysis/">sequence analysis</a> results, click <a href="/books/n/gene/app2/">here</a>.</p></div></dd><dt>4. </dt><dd><div id="ctx.TF.2.4"><p class="no_margin">Data derived from the subscription-based professional view of Human Gene Mutation Database and Ensembl 105: Dec 2021 [<a class="bk_pop" href="#ctx.REF.stenson.2020.1197">Stenson et al 2020</a>, <a class="bk_pop" href="#ctx.REF.howe.2021.d884">Howe et al 2021</a>]</p></div></dd><dt>5. </dt><dd><div id="ctx.TF.2.5"><p class="no_margin">Gene-targeted <a class="def" href="/books/n/gene/glossary/def-item/deletion-duplication-analysis/">deletion/duplication analysis</a> detects intragenic deletions or duplications. Methods used may include a range of techniques such as <a class="def" href="/books/n/gene/glossary/def-item/quantitative-pcr/">quantitative PCR</a>, long-range PCR, multiplex ligation-dependent probe amplification (MLPA), and a <a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a>-targeted microarray designed to detect single-<a class="def" href="/books/n/gene/glossary/def-item/exon/">exon</a> deletions or duplications.</p></div></dd></dl></div></div></div></div></div></div><div id="ctx.Clinical_Characteristics"><h2 id="_ctx_Clinical_Characteristics_">Clinical Characteristics</h2><div id="ctx.Clinical_Description"><h3>Clinical Description</h3><p>Cerebrotendinous xanthomatosis (CTX) is a lipid storage disease characterized by infantile-onset diarrhea, childhood-onset cataract, adolescent- to young adult-onset tendon xanthomas, and adult-onset progressive neurologic dysfunction (dementia, psychiatric disturbances, pyramidal and/or cerebellar signs, dystonia, atypical parkinsonism, peripheral neuropathy, and seizures). Intrafamilial variability is considerable. A suspicion index for diagnosis has been reported based on clinical and laboratory findings [<a class="bk_pop" href="#ctx.REF.mignarri.2014.421">Mignarri et al 2014</a>].</p><div id="ctx.T.cerebrotendinous_xanthomatosis_fre" class="table"><h3><span class="label">Table 3. </span></h3><div class="caption"><p>Cerebrotendinous Xanthomatosis: Frequency of Select Features</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_fre/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.cerebrotendinous_xanthomatosis_fre_lrgtbl__"><table class="no_bottom_margin"><thead><tr><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="2" scope="colgroup" rowspan="1" style="text-align:left;vertical-align:middle;">Feature</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">% of Persons w/Feature</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="2" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Infantile-onset diarrhea</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">40%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="2" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Childhood-onset cataract</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">89%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="2" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Adolescent- to young adult-onset tendon xanthomas</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">78%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="2" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Cardiovascular findings</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">25%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="2" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Osteopenia</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">67%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" rowspan="7" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">Adult-onset progressive neurologic dysfunction</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Intellectual disability</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">60%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Psychiatric disturbances</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">44%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Ataxia</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">36%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Spastic paraparesis</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">64%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Parkinsonism</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">9%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Peripheral neuropathy</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">70%</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_1" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Seizures</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_fre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">33%</td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt></dt><dd><div><p class="no_margin">Based on <a class="bk_pop" href="#ctx.REF.mignarri.2014.421">Mignarri et al [2014]</a></p></div></dd></dl></div></div></div><p><b>Gastrointestinal and hepatic findings.</b> Chronic diarrhea from infancy, even in the neonatal period, may be the earliest clinical manifestation of CTX [<a class="bk_pop" href="#ctx.REF.cruysberg.2002.1975">Cruysberg 2002</a>, <a class="bk_pop" href="#ctx.REF.gong.2017.561">Gong et al 2017</a>]. Gallstones have been reported on occasion. Neonatal cholestasis has been identified as a presenting manifestation of CTX [<a class="bk_pop" href="#ctx.REF.zhang.2021.116">Zhang et al 2021</a>]. Cases with fatal cholestasis [<a class="bk_pop" href="#ctx.REF.von_bahr.2005.481">von Bahr et al 2005</a>] and infantile hepatitis in infancy [<a class="bk_pop" href="#ctx.REF.clayton.2002.501">Clayton et al 2002</a>] have been also reported.</p><p><b>Eye.</b> In approximately 75% of affected individuals, cataracts are the first finding, often appearing in the first decade of life. In 25% of individuals, cataracts are first observed after age 40 years. Cataracts may be visually significant opacities requiring lensectomy or visually insignificant cortical opacities. The appearance can include irregular cortical opacities, anterior polar cataracts, and dense posterior subcapsular cataracts [<a class="bk_pop" href="#ctx.REF.cruysberg.1995.597">Cruysberg et al 1995</a>]. Among large study groups of individuals with juvenile-onset cataracts, CTX was diagnosed in 1.8% in the United States [<a class="bk_pop" href="#ctx.REF.freedman.2019.1312">Freedman et al 2019</a>] and 1.55% in Turkey [<a class="bk_pop" href="#ctx.REF.atilla.2021.269.e1">Atilla et al 2021</a>].</p><p>Other findings include palpebral xanthelasmas, optic nerve atrophy and proptosis, paleness of the optic disk, premature retinal senescence with retinal vessel sclerosis, cholesterol-like deposits along vascular arcades, and myelinated nerve fibers [<a class="bk_pop" href="#ctx.REF.dotti.2001.696">Dotti et al 2001</a>].</p><p><a class="bk_pop" href="#ctx.REF.khan.2013.956">Khan et al [2013]</a> reported the unique finding of fleck lenticular opacities in three children with CTX; these affected children also had capsular opacities (posterior only or posterior and anterior) that caused visual symptoms.</p><p><b>Xanthomas</b> appear in the second or third decade. In addition to the classic xanthomas of the Achilles tendon, xanthomas also occur on the extensor tendons of the elbow and hand, the patellar tendon (see <a class="figpopup" href="/books/NBK1409/figure/ctx.F1/?report=objectonly" target="object" rid-figpopup="figctxF1" rid-ob="figobctxF1">Figure 1</a>), and the neck tendons. Xanthomas have been reported in the lung, bones, and central nervous system [<a class="bk_pop" href="#ctx.REF.brienza.2015.981">Brienza et al 2015</a>].</p><p><b>Cardiovascular system.</b> Premature atherosclerosis and coronary artery disease have been reported [<a class="bk_pop" href="#ctx.REF.valdivielso.2004.680">Valdivielso et al 2004</a>, <a class="bk_pop" href="#ctx.REF.androdias.2012.364">Androdias et al 2012</a>], as has lipomatous hypertrophy of the atrial septum [<a class="bk_pop" href="#ctx.REF.dotti.1998.723">Dotti et al 1998</a>, <a class="bk_pop" href="#ctx.REF.frihayed.2005.992">Frih-Ayed et al 2005</a>].</p><p><b>Skeleton.</b> Bone involvement is characterized by granulomatous lesions in the lumbar vertebrae and femur, osteoporosis and increased risk of bone fractures, and impaired adsorption of radiocalcium, which improves with chenodeoxycholic acid treatment [<a class="bk_pop" href="#ctx.REF.martini.2013.282">Martini et al 2013</a>]. Osteoporosis is evident by total body densitometry in untreated individuals. Individuals may have marked thoracic kyphosis.</p><p><b>Premature aging.</b> Early-onset cataract, osteopenia with bone fractures and loss of teeth, atherosclerosis, and neurologic impairment with dementia and/or parkinsonism (associated with the characteristic facies) suggest a generalized premature aging process [<a class="bk_pop" href="#ctx.REF.dotti.1991.371">Dotti et al 1991</a>].</p><div id="ctx.Neurologic_Signs"><h4>Neurologic Signs</h4><p><b>Intellectual disability or dementia</b> following slow deterioration in intellectual abilities occurs in the third decade in more than 50% of individuals [<a class="bk_pop" href="#ctx.REF.verrips.2000a.407">Verrips et al 2000a</a>]. Some individuals show cognitive impairment from early infancy, whereas the majority have normal or only slightly impaired intellectual function until puberty. In the spinal form, mainly characterized by myelopathy and spastic paraparesis, intellect is almost always normal.</p><p><b>Neuropsychiatric symptoms</b> including behavioral changes, hallucinations, agitation, aggression, depression, and suicide attempts may be prominent [<a class="bk_pop" href="#ctx.REF.fraidakis.2013.e302">Fraidakis 2013</a>].</p><p><b>Pyramidal signs (i.e., spasticity) and/or cerebellar signs</b> are almost invariably present between ages 20 and 30 years. The clinical findings are related to the primary involvement of corticospinal tracts, subcortical white matter, dentate nuclei, and cerebellum cortex involvement that is evident on MRI [<a class="bk_pop" href="#ctx.REF.dotti.1994.1721">Dotti et al 1994</a>, <a class="bk_pop" href="#ctx.REF.inglese.2003.495">Inglese et al 2003</a>, <a class="bk_pop" href="#ctx.REF.mignarri.2017.862">Mignarri et al 2017</a>, <a class="bk_pop" href="#ctx.REF.rosini.2017.3607">Rosini et al 2017</a>, <a class="bk_pop" href="#ctx.REF.catarino.2018.388">Catarino et al 2018</a>, <a class="bk_pop" href="#ctx.REF.makary.2018.e637">Makary et al 2018</a>].</p><p>Some individuals present with a spinal form, in which progressive spastic paraparesis is the main clinical concern [<a class="bk_pop" href="#ctx.REF.nicholls.2015.280">Nicholls et al 2015</a>, <a class="bk_pop" href="#ctx.REF.catarino.2018.388">Catarino et al 2018</a>].</p><p><b>Extrapyramidal manifestations</b> can be considered a late disease manifestation, with parkinsonism the most frequently reported, followed by dystonia, myoclonus, and postural tremor. In a recent review of 79 individuals with CTX, the mean age at onset of a movement disorder was 40&#x000b1;12 years (median 40, range 13-62 years). Movement disorders were found to be mixed in 23% of individuals and were usually part of a complex clinical picture, rather than a prominent finding. Still, in 18% of individuals, a movement disorder was the presenting manifestation [<a class="bk_pop" href="#ctx.REF.stelten.2019.12">Stelten et al 2019</a>].</p><p><b>Seizures</b> are reported in approximately 50% of individuals with CTX [<a class="bk_pop" href="#ctx.REF.pedroso.2012.380">Pedroso et al 2012</a>].</p><p><b>Peripheral neuropathy</b> is evident on electrophysiologic studies [<a class="bk_pop" href="#ctx.REF.ginanneschi.2013.268">Ginanneschi et al 2013</a>, <a class="bk_pop" href="#ctx.REF.zhang.2020.1372">Zhang et al 2020</a>], which reveal decreased nerve conduction velocities and abnormalities in somatosensory, motor, brain stem, and visual evoked potentials. Clinical manifestations related to peripheral nerve involvement are distal muscle atrophy and pes cavus. Sensory abnormalities are rarely described.</p></div><div id="ctx.Heterozygotes"><h4>Heterozygotes</h4><p>Heterozygotes are generally asymptomatic; however, clinical findings have been reported in heterozygotes ranging from an increased incidence of cardiovascular disorders to gallstones [Author, personal observation].</p></div></div><div id="ctx.GenotypePhenotype_Correlations"><h3>Genotype-Phenotype Correlations</h3><p>No <a class="def" href="/books/n/gene/glossary/def-item/genotype-phenotype-correlations/">genotype-phenotype correlations</a> for <i>CYP27A1</i> have been identified.</p></div><div id="ctx.Nomenclature"><h3>Nomenclature</h3><p>Terms used in the past for CTX and no longer in use include the following:</p><ul><li class="half_rhythm"><div>Cerebral cholesterinosis</div></li><li class="half_rhythm"><div>Cerebrotendinous cholesterosis</div></li><li class="half_rhythm"><div>Van Bogaert-Scherer-Epstein syndrome</div></li></ul></div><div id="ctx.Prevalence"><h3>Prevalence</h3><p>More than 400 individuals with CTX have been reported worldwide [<a class="bk_pop" href="#ctx.REF.stelten.2021a.353">Stelten et al 2021a</a>], with larger groups of affected individuals being reported in the medical literature from Italy, the Netherlands, Germany, Japan, China, Turkey, Israel, and Spain.</p></div></div><div id="ctx.Genetically_Related_Allelic_Disorder"><h2 id="_ctx_Genetically_Related_Allelic_Disorder_">Genetically Related (Allelic) Disorders</h2><p>No phenotypes other than those discussed in this <i>GeneReview</i> are known to be associated with <a class="def" href="/books/n/gene/glossary/def-item/germline/">germline</a> pathogenic variants in <i>CYP27A1</i>.</p></div><div id="ctx.Differential_Diagnosis"><h2 id="_ctx_Differential_Diagnosis_">Differential Diagnosis</h2><p>Selected monogenic disorders that may present with clinical features similar to those of cerebrotendinous xanthomatosis are summarized in <a href="/books/NBK1409/table/ctx.T.selected_monogenic_disorders_in_th/?report=objectonly" target="object" rid-ob="figobctxTselectedmonogenicdisordersinth">Table 4</a>.</p><div id="ctx.T.selected_monogenic_disorders_in_th" class="table"><h3><span class="label">Table 4. </span></h3><div class="caption"><p>Selected Monogenic Disorders in the Differential Diagnosis of Cerebrotendinous Xanthomatosis</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.selected_monogenic_disorders_in_th/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.selected_monogenic_disorders_in_th_lrgtbl__"><table class="no_bottom_margin"><thead><tr><th id="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Feature</th><th id="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Genetic Disorder</th><th id="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Gene(s)</th><th id="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">MOI</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Chronic</b>
<br />
<b>diarrhea</b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Congenital diarrhea (OMIM <a href="https://omim.org/phenotypicSeries/PS214700" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">PS214700</a>)</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>DGAT1</i>
<br />
<i>EPCAM</i>
<br />
<i>GUCY2C</i>
<br />
<i>MYO5B</i>
<br />
<i>NEUROG3</i>
<br />
<i>PERCC1</i>
<br />
<i>PLVAP</i>
<br />
<i>SLC26A3</i>
<br />
<i>SLC9A3</i>
<br />
<i>SPINT2</i>
<br />
<i>STX3</i>
<br />
<i>WNT2B</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AR<br />AD&#x000a0;<sup>1</sup></td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" rowspan="4" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Neonatal</b>
<br />
<b>cholestasis&#x000a0;<sup>2</sup></b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<a href="/books/n/gene/alagille/">Alagille syndrome</a>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>JAG1</i>
<br />
<i>NOTCH2</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AD</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Dubin-Johnson syndrome (OMIM <a href="https://omim.org/entry/237500" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">237500</a>)</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>ABCC2</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AR</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Neonatal intrahepatic cholestasis caused by <a href="/books/n/gene/citrin/">citrin deficiency</a></td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>SLC25A13</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AR</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Progressive <a class="def" href="/books/n/gene/glossary/def-item/familial/">familial</a> intrahepatic cholestasis (see <a href="/books/n/gene/pfic/">ATP8B1 deficiency</a> &#x00026; OMIM <a href="https://omim.org/phenotypicSeries/PS211600" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">PS211600</a>)</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>ABCB4</i>
<br />
<i>ABCB11</i>
<br />
<i>ATP8B1</i>
<br />
<i>NR1H4</i>
<br />
<i>SLC51A</i>
<br />
<i>TJP2</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AR</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Juvenile</b>
<br />
<b>cataracts</b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<a href="/books/n/gene/myotonic-d/">Myotonic dystrophy type 1</a>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>DMPK</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AD</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" rowspan="2" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Xanthomas</b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"><a href="/books/n/gene/stsl/">Sitosterolemia</a>. Note: Tendon xanthomas or tuberous (i.e., planar) xanthomas can occur in childhood &#x00026; in unusual locations (heels, knees, elbows, &#x00026; buttocks).</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>ABCG5</i>
<br />
<i>ABCG8</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AR</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;"><a href="/books/n/gene/hyperchol/">Familial hypercholesterolemia</a> (FH). Note: Common locations of xanthomas incl around eyelids, tendons of elbows, hands, knees, &#x00026; feet, particularly Achilles tendon. Interdigital xanthomas occur in persons w/<a class="def" href="/books/n/gene/glossary/def-item/homozygous/">homozygous</a> FH.</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<i>APOB</i>
<br />
<i>LDLR</i>
<br />
<i>PCSK9</i>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AD</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Spastic</b>
<br />
<b>paraplegia</b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">See <a href="/books/n/gene/hsp/">Hereditary Spastic Paraplegia Overview</a>.</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">&#x0003e;80 genes</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AD<br />AR<br />XL<br />Mat</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Ataxia</b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">See <a href="/books/n/gene/ataxias/">Hereditary Ataxia Overview</a>.</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">&#x0003e;130 genes</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AD<br />AR<br />XL</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Intellectual</b>
<br />
<b>disability</b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">See <a href="https://www.omim.org/phenotypicSeries/PS156200" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">OMIM Autosomal Dominant</a>, <a href="https://omim.org/phenotypicSeries/PS249500" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">Autosomal Recessive</a>, <a href="https://omim.org/phenotypicSeries/PS309530" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">Nonsyndromic X-Linked</a>, &#x00026; <a href="https://omim.org/phenotypicSeries/PS309510" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">Syndromic X-Linked Intellectual Developmental Disorder Phenotypic Series</a>.</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">&#x0003e;200 genes</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AD<br />AR<br />XL</td></tr><tr><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Genetic</b>
<br />
<b>leukoenceph-</b>
<br />
<b>alopathies</b>
</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">See <a class="bk_pop" href="#ctx.REF.vanderver.2016.916">Vanderver [2016]</a>.</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">&#x0003e;100 genes</td><td headers="hd_h_ctx.T.selected_monogenic_disorders_in_th_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">AD<br />AR<br />XL<br />Mat</td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt></dt><dd><div><p class="no_margin">AD = <a class="def" href="/books/n/gene/glossary/def-item/autosomal-dominant/">autosomal dominant</a>; AR = <a class="def" href="/books/n/gene/glossary/def-item/autosomal-recessive/">autosomal recessive</a>; Mat = maternal; MOI = <a class="def" href="/books/n/gene/glossary/def-item/mode-of-inheritance/">mode of inheritance</a>; XL = <a class="def" href="/books/n/gene/glossary/def-item/x-linked/">X-linked</a></p></div></dd><dt>1. </dt><dd><div id="ctx.TF.4.1"><p class="no_margin">Inheritance is <a class="def" href="/books/n/gene/glossary/def-item/autosomal-recessive/">autosomal recessive</a> with the exception of <i>GUCY2C</i>-related diarrhea, which is inherited in an <a class="def" href="/books/n/gene/glossary/def-item/autosomal-dominant/">autosomal dominant</a> manner.</p></div></dd><dt>2. </dt><dd><div id="ctx.TF.4.2"><p class="no_margin">
<a class="bk_pop" href="#ctx.REF.lipi_ski.2020.414">Lipi&#x00144;ski et al [2020]</a>
</p></div></dd></dl></div></div></div></div><div id="ctx.Management"><h2 id="_ctx_Management_">Management</h2><p>A clinical practice guideline on the diagnosis, treatment, and management of cerebrotendinous xanthomatosis (CTX) has been published, based on expert opinion collected with the Delphi method [<a class="bk_pop" href="#ctx.REF.stelten.2021a.353">Stelten et al 2021a</a>] (<a href="https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8349076/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">full text</a>).</p><div id="ctx.Evaluations_Following_Initial_Diagno"><h3>Evaluations Following Initial Diagnosis</h3><p>To establish the extent of disease and needs in an individual diagnosed with CTX, the evaluations summarized in <a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_rec/?report=objectonly" target="object" rid-ob="figobctxTcerebrotendinousxanthomatosisrec">Table 5</a> (if not performed as part of the evaluation that led to the diagnosis) are recommended.</p><div id="ctx.T.cerebrotendinous_xanthomatosis_rec" class="table"><h3><span class="label">Table 5. </span></h3><div class="caption"><p>Cerebrotendinous Xanthomatosis: Recommended Evaluations Following Initial Diagnosis</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_rec/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.cerebrotendinous_xanthomatosis_rec_lrgtbl__"><table class="no_bottom_margin"><thead><tr><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">System/Concern</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Evaluation</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Comment</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>&#x02191; cholestanol level</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Lab testing of lipids incl plasma cholestanol level</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Peripheral neuropathy</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">EMG &#x00026; NCV studies as baseline</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Cardiologic concerns</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Cardiac eval incl EKG &#x00026; echocardiogram</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Osteoporosis</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Bone density study</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Cataracts</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Ophthalmologic eval</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Neurologic &#x00026;</b>
<br />
<b>behavioral concerns</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Baseline neurologic &#x00026; neuropsychiatric eval</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Genetic counseling</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">By genetics professionals&#x000a0;<sup>1</sup></td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">To obtain a <a class="def" href="/books/n/gene/glossary/def-item/pedigree/">pedigree</a> &#x00026; inform affected persons &#x00026; their families re nature, MOI, &#x00026; implications of CTX to facilitate medical &#x00026; personal decision making</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Family support</b>
<br />
<b>&#x00026; resources</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Assess need for:
<ul><li class="half_rhythm"><div>Community or <a href="#ctx.Resources">online resources</a> such as <a href="https://www.p2pusa.org/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">Parent to Parent</a>;</div></li><li class="half_rhythm"><div>Social work involvement for parental support;</div></li><li class="half_rhythm"><div>Home nursing referral.</div></li></ul>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt></dt><dd><div><p class="no_margin">MOI = <a class="def" href="/books/n/gene/glossary/def-item/mode-of-inheritance/">mode of inheritance</a>; NCV = nerve conduction velocity</p></div></dd><dt>1. </dt><dd><div id="ctx.TF.5.1"><p class="no_margin">Medical geneticist, certified genetic counselor, certified advanced genetic nurse</p></div></dd></dl></div></div></div></div><div id="ctx.Treatment_of_Manifestations"><h3>Treatment of Manifestations</h3><div id="ctx.Targeted_Therapy"><h4>Targeted Therapy</h4><p>
<i>In GeneReviews, a targeted therapy is one that addresses the specific underlying mechanism of disease causation (regardless of whether the therapy is significantly efficacious for one or more manifestation of the genetic condition); would otherwise not be considered without knowledge of the underlying genetic cause of the condition; or could lead to a cure</i>. &#x02014;ED</p><p>Early treatment with chenodeoxycholic acid (CDCA) in presymptomatic individuals appears to prevent clinical manifestations (see <a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_tar/?report=objectonly" target="object" rid-ob="figobctxTcerebrotendinousxanthomatosistar">Table 6</a>) [<a class="bk_pop" href="#ctx.REF.degrassi.2020.382">Degrassi et al 2020</a>].</p><div id="ctx.T.cerebrotendinous_xanthomatosis_tar" class="table"><h3><span class="label">Table 6. </span></h3><div class="caption"><p>Cerebrotendinous Xanthomatosis: Targeted Therapy</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_tar/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.cerebrotendinous_xanthomatosis_tar_lrgtbl__"><table class="no_bottom_margin"><thead><tr><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tar_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Manifestation/Concern</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tar_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Treatment</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tar_1_1_1_3" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Considerations/Other</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tar_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>&#x02191; cholestanol assoc w/neurologic issues &#x00026; osteoporosis</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tar_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"><ul><li class="half_rhythm"><div>Long-term treatment w/CDCA&#x000a0;<sup>1</sup>: 750 mg/day in adults; 10-20 mg/kg/day in children</div></li><li class="half_rhythm"><div>Should be started early as effect of therapy depends largely on extent of irreversible structural damage to axons</div></li></ul>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tar_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"><ul><li class="half_rhythm"><div>Normalizes plasma &#x00026; CSF concentration of cholestanol by suppressing cholestanol biosynthesis</div></li><li class="half_rhythm"><div>Improves neurophysiologic findings (normalization of NCVs &#x00026; stabilization; slow &#x00026; continuous improvement of MEPs &#x00026; SEPs)</div></li><li class="half_rhythm"><div>Also improves osteoporosis</div></li><li class="half_rhythm"><div>See <a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_tre/?report=objectonly" target="object" rid-ob="figobctxTcerebrotendinousxanthomatosistre">Table 7</a> for alternative/combination treatments.</div></li></ul>
</td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt></dt><dd><div><p class="no_margin">CDCA = chenodeoxycholic acid; CSF = cerebrospinal fluid; MEP = motor evoked potential; NCV = nerve conduction velocity, SEP = sensory evoked potential</p></div></dd><dt>1. </dt><dd><div id="ctx.TF.6.1"><p class="no_margin"><a class="bk_pop" href="#ctx.REF.verrips.2020.943">Verrips et al [2020]</a> highlighted the efficacy and safety of therapeutic treatment with CDCA through two retrospective studies.</p></div></dd></dl></div></div></div></div><div id="ctx.Supportive_Care"><h4>Supportive Care</h4><div id="ctx.T.cerebrotendinous_xanthomatosis_tre" class="table"><h3><span class="label">Table 7. </span></h3><div class="caption"><p>Cerebrotendinous Xanthomatosis: Treatment of Manifestations</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_tre/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.cerebrotendinous_xanthomatosis_tre_lrgtbl__"><table class="no_bottom_margin"><thead><tr><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Manifestation/Concern</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Treatment</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Considerations/Other</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_1" rowspan="3" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">
<b>&#x02191; cholestanol assoc w/neurologic issues &#x00026; osteoporosis</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Long-term treatment w/CDCA (See <a href="#ctx.Targeted_Therapy">Targeted Therapy</a>.)</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">See <a href="#ctx.Targeted_Therapy">Targeted Therapy</a>.</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">Inhibitors of HMG-CoA reductase (statins such as simvastatin &#x00026; pravastatin) can be used as alternative treatment alone or in combination w/CDCA.</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Caution required when using these drugs: may induce muscle damage or even rhabdomyolysis</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_2" colspan="1" scope="col" rowspan="1" style="text-align:left;vertical-align:middle;"><ul><li class="half_rhythm"><div>Cholic acid treatment has been used in a few persons&#x000a0;<sup>1</sup> &#x00026; is assoc w/&#x02193; of cholestanol level &#x00026; improvement of neurologic symptoms.</div></li><li class="half_rhythm"><div>Such therapy may be useful in those who experience side effects w/CDCA treatments.</div></li></ul>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Cataracts</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Surgical cataract extraction</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Typically required in at least 1 eye by age 50 yrs</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Epilepsy</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_2" rowspan="3" colspan="1" style="text-align:left;vertical-align:middle;">Symptomatic treatments</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Spasticity</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" colspan="1" rowspan="1" style="text-align:left;vertical-align:middle;"></td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Parkinsonism</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_tre_1_1_1_3" colspan="1" rowspan="1" style="text-align:left;vertical-align:middle;">Persons w/CTX &#x00026; parkinsonism are poorly responsive to levodopa.</td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt></dt><dd><div><p class="no_margin">CDCA = chenodeoxycholic acid; HMG-CoA = 3-hydroxy-3-methylglutaryl coenzyme A</p></div></dd><dt>1. </dt><dd><div id="ctx.TF.7.1"><p class="no_margin"><a class="bk_pop" href="#ctx.REF.pierre.2008.s241">Pierre et al [2008]</a>, <a class="bk_pop" href="#ctx.REF.mandia.2019.2043">Mandia et al [2019]</a></p></div></dd></dl></div></div></div></div></div><div id="ctx.Surveillance"><h3>Surveillance</h3><div id="ctx.T.cerebrotendinous_xanthomatosis_rec_1" class="table"><h3><span class="label">Table 8. </span></h3><div class="caption"><p>Cerebrotendinous Xanthomatosis: Recommended Surveillance</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_rec_1/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.cerebrotendinous_xanthomatosis_rec_1_lrgtbl__"><table><thead><tr><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">System/Concern</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Evaluation</th><th id="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_3" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Frequency</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>&#x02191; cholestanol levels</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Cholestanol plasma concentration</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_3" rowspan="5" colspan="1" style="text-align:left;vertical-align:middle;">Annually</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_1" rowspan="2" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Neurologic &#x00026;</b>
<br />
<b>neuropsychologic issues</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Neurologic &#x00026; neuropsychologic eval</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_2" colspan="1" scope="col" rowspan="1" style="text-align:left;vertical-align:middle;">Brain MRI</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Cardiac concerns</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Echocardiogram</td></tr><tr><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_1" scope="row" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">
<b>Osteoporosis</b>
</td><td headers="hd_h_ctx.T.cerebrotendinous_xanthomatosis_rec_1_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Bone density eval</td></tr></tbody></table></div></div></div><div id="ctx.AgentsCircumstances_to_Avoid"><h3>Agents/Circumstances to Avoid</h3><p>Caution in the use of statins has been suggested [<a class="bk_pop" href="#ctx.REF.federico.2001.1743">Federico &#x00026; Dotti 2001</a>]. See <a href="/books/NBK1409/table/ctx.T.cerebrotendinous_xanthomatosis_tre/?report=objectonly" target="object" rid-ob="figobctxTcerebrotendinousxanthomatosistre">Table 7</a>.</p></div><div id="ctx.Evaluation_of_Relatives_at_Risk"><h3>Evaluation of Relatives at Risk</h3><p>It is appropriate to clarify the genetic status of apparently asymptomatic older and younger at-risk relatives of an affected individual in order to identify as early as possible those who would benefit from prompt initiation of CDCA treatment and surveillance. Early treatment with CDCA in presymptomatic individuals appears to prevent clinical manifestations (see <a href="#ctx.Treatment_of_Manifestations">Treatment of Manifestations</a>). Evaluations can include:</p><ul><li class="half_rhythm"><div>Molecular genetic testing if the <i>CYP27A1</i> pathogenic variants in the family are known;</div></li><li class="half_rhythm"><div>Biochemical testing including cholestanol plasma concentration if the pathogenic variants in the family are not known.</div></li></ul><p>See <a href="#ctx.Related_Genetic_Counseling_Issues">Genetic Counseling</a> for issues related to testing of at-risk relatives for <a class="def" href="/books/n/gene/glossary/def-item/genetic-counseling/">genetic counseling</a> purposes.</p></div><div id="ctx.Pregnancy_Management"><h3>Pregnancy Management</h3><p>Treatment with CDCA should not be interrupted during pregnancy.</p></div><div id="ctx.Therapies_Under_Investigation"><h3>Therapies Under Investigation</h3><p>Gene therapies are under investigation in a mouse model of CTX [<a class="bk_pop" href="#ctx.REF.lumbreras.2021.210">Lumbreras et al 2021</a>].</p><p>Search <a href="https://clinicaltrials.gov/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">ClinicalTrials.gov</a> in the US and <a href="https://www.clinicaltrialsregister.eu/ctr-search/search" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">EU Clinical Trials Register</a> in Europe for access to information on clinical studies for a wide range of diseases and conditions.</p></div></div><div id="ctx.Genetic_Counseling"><h2 id="_ctx_Genetic_Counseling_">Genetic Counseling</h2><p>
<i>Genetic counseling is the process of providing individuals and families with
information on the nature, mode(s) of inheritance, and implications of genetic disorders to help them
make informed medical and personal decisions. The following section deals with genetic
risk assessment and the use of family history and genetic testing to clarify genetic
status for family members; it is not meant to address all personal, cultural, or
ethical issues that may arise or to substitute for consultation with a genetics
professional</i>. &#x02014;ED.</p><div id="ctx.Mode_of_Inheritance"><h3>Mode of Inheritance</h3><p>Cerebrotendinous xanthomatosis (CTX) is inherited in an <a class="def" href="/books/n/gene/glossary/def-item/autosomal-recessive/">autosomal recessive</a> manner.</p></div><div id="ctx.Risk_to_Family_Members"><h3>Risk to Family Members</h3><p>
<b>Parents of a <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a></b>
</p><ul><li class="half_rhythm"><div>The parents of an affected child are presumed to be <a class="def" href="/books/n/gene/glossary/def-item/heterozygous/">heterozygous</a> for a <i>CYP27A1</i> <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a>.</div></li><li class="half_rhythm"><div>If a molecular diagnosis has been established in the <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a>, <a class="def" href="/books/n/gene/glossary/def-item/molecular-genetic-testing/">molecular genetic testing</a> is recommended for the parents of the proband to confirm that both parents are <a class="def" href="/books/n/gene/glossary/def-item/heterozygous/">heterozygous</a> for a <i>CYP27A1</i> <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a> and to allow reliable <a class="def" href="/books/n/gene/glossary/def-item/recurrence-risk/">recurrence risk</a> assessment.</div></li><li class="half_rhythm"><div>If a <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a> is detected in only one parent and parental identity testing has confirmed biological maternity and paternity, it is possible that one of the pathogenic variants identified in the <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a> occurred as a <a class="def" href="/books/n/gene/glossary/def-item/de-novo/"><i>de novo</i></a> event in the proband or as a <a class="def" href="/books/n/gene/glossary/def-item/postzygotic/">postzygotic</a> <i>de novo</i> event in a mosaic parent [<a class="bk_pop" href="#ctx.REF.j_nsson.2017.519">J&#x000f3;nsson et al 2017</a>]. If the proband appears to have <a class="def" href="/books/n/gene/glossary/def-item/homozygous/">homozygous</a> pathogenic variants (i.e., the same two pathogenic variants), additional possibilities to consider include:</div><ul><li class="half_rhythm"><div>A single- or multiexon <a class="def" href="/books/n/gene/glossary/def-item/deletion/">deletion</a> in the <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a> that was not detected by <a class="def" href="/books/n/gene/glossary/def-item/sequence-analysis/">sequence analysis</a> and that resulted in the artifactual appearance of homozygosity;</div></li><li class="half_rhythm"><div>Uniparental isodisomy for the parental <a class="def" href="/books/n/gene/glossary/def-item/chromosome/">chromosome</a> with the <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a> that resulted in homozygosity for the pathogenic variant in the <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a>.</div></li></ul></li><li class="half_rhythm"><div>Heterozygotes (carriers) are generally asymptomatic; however, clinical findings have been reported in heterozygotes ranging from an increased incidence of cardiovascular disorders to gallstones [Author, personal observation].</div></li></ul><p>
<b>Sibs of a <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a></b>
</p><ul><li class="half_rhythm"><div>If both parents are known to be <a class="def" href="/books/n/gene/glossary/def-item/heterozygous/">heterozygous</a> for a <i>CYP27A1</i> <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a>, each sib of an affected individual has at conception a 25% chance of being affected, a 50% chance of being a <a class="def" href="/books/n/gene/glossary/def-item/carrier/">carrier</a>, and a 25% chance of inheriting neither of the <a class="def" href="/books/n/gene/glossary/def-item/familial/">familial</a> pathogenic variants.</div></li><li class="half_rhythm"><div>Significant clinical variability may be observed between affected family members: a sib with <a class="def" href="/books/n/gene/glossary/def-item/biallelic/">biallelic</a> pathogenic variants may experience less severe manifestations with later onset of neurologic signs than the <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a> [<a class="bk_pop" href="#ctx.REF.guenzel.2021.3">Guenzel et al 2021</a>, <a class="bk_pop" href="#ctx.REF.stelten.2021b.1039">Stelten et al 2021b</a>] and may not develop xanthomas [<a class="bk_pop" href="#ctx.REF.verrips.2000b.520">Verrips et al 2000b</a>, <a class="bk_pop" href="#ctx.REF.gelzo.2021.561">Gelzo et al 2021</a>].</div></li><li class="half_rhythm"><div>Heterozygotes (carriers) are generally asymptomatic; however, clinical findings have been reported in heterozygotes ranging from an increased incidence of cardiovascular disorders to gallstones [Author, personal observation].</div></li></ul><p>
<b>Offspring of a <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a></b>
</p><ul><li class="half_rhythm"><div>The offspring of an individual with CTX are obligate heterozygotes for a <i>CYP27A1</i> <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a>.</div></li><li class="half_rhythm"><div>If the reproductive partner of a <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a> is <a class="def" href="/books/n/gene/glossary/def-item/heterozygous/">heterozygous</a> for a <i>CYP27A1</i> <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a> &#x02013; a situation more likely to be seen in Israel or Morocco and/or in reproductive partners of Druze ancestry, due to a <a class="def" href="/books/n/gene/glossary/def-item/founder-effect/">founder effect</a> &#x02013; offspring are at risk of inheriting <a class="def" href="/books/n/gene/glossary/def-item/biallelic/">biallelic</a> <i>CYP27A1</i> pathogenic variants and being affected with CTX.</div></li></ul><p><b>Other family members.</b> Each sib of the <a class="def" href="/books/n/gene/glossary/def-item/proband/">proband</a>'s parents is at a 50% risk of being a <a class="def" href="/books/n/gene/glossary/def-item/carrier/">carrier</a> of a <i>CYP27A1</i> <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a>.</p></div><div id="ctx.Carrier_Heterozygote_Detection"><h3>Carrier (Heterozygote) Detection</h3><p>Carrier testing for at-risk relatives requires prior identification of the <i>CYP27A1</i> pathogenic variants in the family.</p></div><div id="ctx.Related_Genetic_Counseling_Issues"><h3>Related Genetic Counseling Issues</h3><p>See Management, <a href="#ctx.Evaluation_of_Relatives_at_Risk">Evaluation of Relatives at Risk</a> for information on evaluating at-risk relatives for the purpose of early diagnosis and treatment.</p><p>
<b>Family planning</b>
</p><ul><li class="half_rhythm"><div>The optimal time for determination of genetic risk and discussion of the availability of prenatal/<a class="def" href="/books/n/gene/glossary/def-item/preimplantation-genetic-testing/">preimplantation genetic testing</a> is before pregnancy.</div></li><li class="half_rhythm"><div>It is appropriate to offer <a class="def" href="/books/n/gene/glossary/def-item/genetic-counseling/">genetic counseling</a> (including discussion of potential risks to offspring and reproductive options) to young adults who are affected, are carriers, or are at risk of being carriers.</div></li></ul><p><b>DNA banking.</b> Because it is likely that testing methodology and our understanding of genes, pathogenic mechanisms, and diseases will improve in the future, consideration should be given to banking DNA from probands in whom a molecular diagnosis has not been confirmed (i.e., the causative pathogenic mechanism is unknown). For more information, see <a class="bk_pop" href="#ctx.REF.huang.2022.389">Huang et al [2022]</a>.</p></div><div id="ctx.Prenatal_Testing_and_Preimplantation"><h3>Prenatal Testing and Preimplantation Genetic Testing</h3><p>Once the <i>CYP27A1</i> pathogenic variants have been identified in an affected family member, prenatal and <a class="def" href="/books/n/gene/glossary/def-item/preimplantation-genetic-testing/">preimplantation genetic testing</a> are possible.</p><p>Differences in perspective may exist among medical professionals and within families regarding the use of prenatal and <a class="def" href="/books/n/gene/glossary/def-item/preimplantation-genetic-testing/">preimplantation genetic testing</a>. While most health care professionals would consider use of prenatal and preimplantation genetic testing to be a personal decision, discussion of these issues may be helpful.</p></div></div><div id="ctx.Resources"><h2 id="_ctx_Resources_">Resources</h2><p>
<i>GeneReviews staff has selected the following disease-specific and/or umbrella
support organizations and/or registries for the benefit of individuals with this disorder
and their families. GeneReviews is not responsible for the information provided by other
organizations. For information on selection criteria, click <a href="/books/n/gene/app4/">here</a>.</i></p>
<ul><li class="half_rhythm"><div>
<b>United Leukodystrophy Foundation</b>
</div><div><b>Phone:</b> 815-748-0844</div><div><b>Email:</b> office@ulf.org</div><div>
<a href="https://ulf.org/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">ulf.org</a>
</div></li><li class="half_rhythm"><div>
<b>Metabolic Support UK</b>
</div><div>United Kingdom</div><div><b>Phone:</b> 0845 241 2173</div><div>
<a href="https://metabolicsupportuk.org/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">metabolicsupportuk.org</a>
</div></li><li class="half_rhythm"><div>
<b>National Organization for Rare Disorders (NORD)</b>
</div><div><b>Phone:</b> 800-999-6673</div><div>
<a href="https://rarediseases.org/for-patients-and-families/help-access-medications/patient-assistance-programs-2/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">RareCare&#x000ae; Patient Assistance Programs</a>
</div></li><li class="half_rhythm"><div>
<b>Myelin Disorders Bioregistry Project</b>
</div><div><b>Phone:</b> 215-590-1719</div><div><b>Email:</b> sherbinio@chop.edu</div><div>
<a href="https://www.chop.edu/research/myelin-disorders-biorepository-project" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">Myelin Disorders Bioregistry Project</a>
</div></li><li class="half_rhythm"><div>
<b>RDCRN Contact Registry for Sterol and Isoprenoid Research (STAIR) Consortium</b>
</div><div>
<a href="https://www.rarediseasesnetwork.org/cms/stair/Get-Involved/Studies" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">RDCRN Patient Contact Registry</a>
</div></li></ul>
</div><div id="ctx.Molecular_Genetics"><h2 id="_ctx_Molecular_Genetics_">Molecular Genetics</h2><p><i>Information in the Molecular Genetics and OMIM tables may differ from that elsewhere in the GeneReview: tables may contain more recent information. &#x02014;</i>ED.</p><div id="ctx.molgen.TA" class="table"><h3><span class="label">Table A.</span></h3><div class="caption"><p>Cerebrotendinous Xanthomatosis: Genes and Databases</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.molgen.TA/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.molgen.TA_lrgtbl__"><table class="no_bottom_margin"><tbody><tr><th id="hd_b_ctx.molgen.TA_1_1_1_1" rowspan="1" colspan="1" style="vertical-align:top;">Gene</th><th id="hd_b_ctx.molgen.TA_1_1_1_2" rowspan="1" colspan="1" style="vertical-align:top;">Chromosome Locus</th><th id="hd_b_ctx.molgen.TA_1_1_1_3" rowspan="1" colspan="1" style="vertical-align:top;">Protein</th><th id="hd_b_ctx.molgen.TA_1_1_1_4" rowspan="1" colspan="1" style="vertical-align:top;">Locus-Specific Databases</th><th id="hd_b_ctx.molgen.TA_1_1_1_5" rowspan="1" colspan="1" style="vertical-align:top;">HGMD</th><th id="hd_b_ctx.molgen.TA_1_1_1_6" rowspan="1" colspan="1" style="vertical-align:top;">ClinVar</th></tr><tr><td headers="hd_b_ctx.molgen.TA_1_1_1_1" rowspan="1" colspan="1" style="vertical-align:top;">
<a href="/gene/1593" ref="pagearea=body&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=gene">
<i>CYP27A1</i>
</a>
</td><td headers="hd_b_ctx.molgen.TA_1_1_1_2" rowspan="1" colspan="1" style="vertical-align:top;">
<a href="https://www.ncbi.nlm.nih.gov/genome/gdv/?context=gene&#x00026;acc=1593" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">2q35</a>
</td><td headers="hd_b_ctx.molgen.TA_1_1_1_3" rowspan="1" colspan="1" style="vertical-align:top;">
<a href="http://www.uniprot.org/uniprot/Q02318" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">Sterol 26-hydroxylase, mitochondrial</a>
</td><td headers="hd_b_ctx.molgen.TA_1_1_1_4" rowspan="1" colspan="1" style="vertical-align:top;">
<a href="http://www.LOVD.nl/CYP27A1" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">CYP27A1 @ LOVD</a>
</td><td headers="hd_b_ctx.molgen.TA_1_1_1_5" rowspan="1" colspan="1" style="vertical-align:top;">
<a href="http://www.hgmd.cf.ac.uk/ac/gene.php?gene=CYP27A1" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">CYP27A1</a>
</td><td headers="hd_b_ctx.molgen.TA_1_1_1_6" rowspan="1" colspan="1" style="vertical-align:top;">
<a href="https://www.ncbi.nlm.nih.gov/clinvar/?term=CYP27A1[gene]" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">CYP27A1</a>
</td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt></dt><dd><div id="ctx.TFA.1"><p class="no_margin">Data are compiled from the following standard references: <a class="def" href="/books/n/gene/glossary/def-item/gene/">gene</a> from
<a href="http://www.genenames.org/index.html" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">HGNC</a>;
<a class="def" href="/books/n/gene/glossary/def-item/chromosome/">chromosome</a> <a class="def" href="/books/n/gene/glossary/def-item/locus/">locus</a> from
<a href="http://www.omim.org/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">OMIM</a>;
protein from <a href="http://www.uniprot.org/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">UniProt</a>.
For a description of databases (Locus Specific, HGMD, ClinVar) to which links are provided, click
<a href="/books/n/gene/app1/">here</a>.</p></div></dd></dl></div></div></div><div id="ctx.molgen.TB" class="table"><h3><span class="label">Table B.</span></h3><div class="caption"><p>OMIM Entries for Cerebrotendinous Xanthomatosis (<a href="/omim/213700,606530" ref="pagearea=body&amp;targetsite=entrez&amp;targetcat=term&amp;targettype=omim">View All in OMIM</a>) </p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.molgen.TB/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.molgen.TB_lrgtbl__"><table><tbody><tr><td rowspan="1" colspan="1" style="text-align:left;vertical-align:top;">
<a href="/omim/213700" ref="pagearea=body&amp;targetsite=entrez&amp;targetcat=term&amp;targettype=omim">213700</a></td><td rowspan="1" colspan="1" style="text-align:left;vertical-align:top;">CEREBROTENDINOUS XANTHOMATOSIS; CTX</td></tr><tr><td rowspan="1" colspan="1" style="text-align:left;vertical-align:top;">
<a href="/omim/606530" ref="pagearea=body&amp;targetsite=entrez&amp;targetcat=term&amp;targettype=omim">606530</a></td><td rowspan="1" colspan="1" style="text-align:left;vertical-align:top;">CYTOCHROME P450, SUBFAMILY XXVIIA, POLYPEPTIDE 1; CYP27A1</td></tr></tbody></table></div></div><div id="ctx.Molecular_Pathogenesis"><h3>Molecular Pathogenesis</h3><p>Cerebrotendinous xanthomatosis (CTX) is caused by <a class="def" href="/books/n/gene/glossary/def-item/biallelic/">biallelic</a> pathogenic variants in <i>CYP27A1</i>. Many of the reported pathogenic variants involve splice sites and are predicted to affect <a class="def" href="/books/n/gene/glossary/def-item/mrna/">mRNA</a> stability or lead to the formation of abnormal mRNA with translation products that are devoid of an adrenodoxin-binding region and/or the heme-binding site, important for enzyme activity. Other pathogenic variants are predicted to result in truncated peptides devoid of function. The associated deficiency of a functional mitochondrial enzyme sterol 27-hydroxylase causes cholestanol and cholesterol accumulation in virtually every tissue.</p><p><b>Mechanism of disease causation.</b> CTX occurs via a <a class="def" href="/books/n/gene/glossary/def-item/loss-of-function/">loss-of-function</a> mechanism.</p><div id="ctx.T.notable_cyp27a1_pathogenic_variant" class="table"><h3><span class="label">Table 9. </span></h3><div class="caption"><p>Notable <i>CYP27A1</i> Pathogenic Variants</p></div><p class="large-table-link" style="display:none"><span class="right"><a href="/books/NBK1409/table/ctx.T.notable_cyp27a1_pathogenic_variant/?report=objectonly" target="object">View in own window</a></span></p><div class="large_tbl" id="__ctx.T.notable_cyp27a1_pathogenic_variant_lrgtbl__"><table class="no_bottom_margin"><thead><tr><th id="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_1" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Reference Sequences</th><th id="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_2" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">DNA Nucleotide<br />Change</th><th id="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_3" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Predicted<br />Protein Change</th><th id="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_4" scope="col" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Comment [Reference]</th></tr></thead><tbody><tr><td headers="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_1" rowspan="2" scope="row" colspan="1" style="text-align:left;vertical-align:middle;">
<a href="https://www.ncbi.nlm.nih.gov/nuccore/NM_000784.4" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">NM_000784<wbr style="display:inline-block"></wbr>.4</a>
<br />
<p>
<a href="https://www.ncbi.nlm.nih.gov/protein/NP_000775.1" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">NP_000775<wbr style="display:inline-block"></wbr>.1</a>
</p>
</td><td headers="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_2" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">c.355delC</td><td headers="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">p.(Arg119GlyfsTer24)</td><td headers="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Founder variant in Israeli Druze [<a class="bk_pop" href="#ctx.REF.falikzaccai.2008.903">Falik-Zaccai et al 2008</a>]</td></tr><tr><td headers="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_2" colspan="1" scope="row" rowspan="1" style="text-align:left;vertical-align:middle;">c.1183C&#x0003e;T</td><td headers="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_3" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">p.Arg395Cys</td><td headers="hd_h_ctx.T.notable_cyp27a1_pathogenic_variant_1_1_1_4" rowspan="1" colspan="1" style="text-align:left;vertical-align:middle;">Common <a class="def" href="/books/n/gene/glossary/def-item/pathogenic-variant/">pathogenic variant</a> [<a class="bk_pop" href="#ctx.REF.cali.1991.7779">Cali et al 1991</a>; Authors, personal observation]</td></tr></tbody></table></div><div><div><dl class="temp-labeled-list small"><dt></dt><dd><div><p class="no_margin">Variants listed in the table have been provided by the authors. <i>GeneReviews</i> staff have not independently verified the classification of variants.</p></div></dd><dt></dt><dd><div><p class="no_margin"><i>GeneReviews</i> follows the standard naming conventions of the Human Genome Variation Society (<a href="https://varnomen.hgvs.org/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">varnomen<wbr style="display:inline-block"></wbr>.hgvs.org</a>). See <a href="/books/n/gene/app3/">Quick Reference</a> for an explanation of nomenclature.</p></div></dd></dl></div></div></div></div></div><div id="ctx.Chapter_Notes"><h2 id="_ctx_Chapter_Notes_">Chapter Notes</h2><div id="ctx.Author_Notes"><h3>Author Notes</h3><p>Antonio Federico is Emeritus professor of Clinical Neurology, Department of Medicine, Surgery and Neurosciences, Medical School, University of Siena, Siena Italy.</p><p>Gian Nicola Gallus is a postdoctoral fellow in Molecular Biology, Department of Medicine, Surgery and Neurosciences, Medical School, University of Siena, Siena, Italy.</p></div><div id="ctx.Acknowledgments"><h3>Acknowledgments</h3><p>We acknowledge all our colleagues who in the last 40 years have collaborated with us in the investigation of this condition: Prof GC Guazzi, Prof N De Stefano, Prof A Malandrini, Dr C Battisti, Dr E Cardaioli, Dr P Formichi, Dr S Bianchi, Dr A Rufa, Dr F Sicurelli; particular thanks to Prof MT Dotti and Dr A Mignarri, and all the physicians who referred patients from Italy and abroad. We also acknowledge all our patients.</p></div><div id="ctx.Author_History"><h3>Author History</h3><p>Maria Teresa Dotti, MD; University of Siena (2003-2022)<br />Antonio Federico, MD (2003-present)<br />Gian Nicola Gallus, DSci (2003-present)</p></div><div id="ctx.Revision_History"><h3>Revision History</h3><ul><li class="half_rhythm"><div>14 November 2024 (ma) Revision: <a href="#ctx.Targeted_Therapy">Targeted Therapy</a> Key Section added</div></li><li class="half_rhythm"><div>17 March 2022 (ha) Comprehensive update posted live</div></li><li class="half_rhythm"><div>14 April 2016 (ma) Comprehensive update posted live</div></li><li class="half_rhythm"><div>1 August 2013 (me) Comprehensive update posted live</div></li><li class="half_rhythm"><div>16 November 2010 (me) Comprehensive update posted live</div></li><li class="half_rhythm"><div>7 February 2006 (me) Comprehensive update posted live</div></li><li class="half_rhythm"><div>16 July 2003 (me) Review posted live</div></li><li class="half_rhythm"><div>18 December 2002 (af) Original submission</div></li></ul></div></div><div id="ctx.References"><h2 id="_ctx_References_">References</h2><div id="ctx.Published_Guidelines__Consensus_Stat"><h3>Published Guidelines / Consensus Statements</h3><ul class="simple-list"><li class="half_rhythm"><div>Stelten BML, Dotti MT, Verrips A, Elibol B, Falik-Zaccai TC, Hanman K, Mignarri A, Sithole B, Steiner RD, Verma S, Yahalom G, Zubarioglu T, Mochel F, Federico A. Expert opinion on diagnosing, treating and managing patients with cerebrotendinous xanthomatosis (CTX): a modified Delphi study. Available <a href="https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8349076/" ref="pagearea=body&amp;targetsite=external&amp;targetcat=link&amp;targettype=uri">online</a>. 2021. Accessed 3-9-22.</div></li></ul></div><div id="ctx.Literature_Cited"><h3>Literature Cited</h3><ul class="simple-list"><li class="half_rhythm"><div class="bk_ref" id="ctx.REF.androdias.2012.364">Androdias
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H, Coskun
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S, et al.
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M. Enlarging brain xanthomas in a patient with cerebrotendinous xanthomatosis.
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JJ, Hsieh
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U, Russell
DW. Mutations in the bile acid biosynthetic enzyme sterol 27-hydroxylase underlie cerebrotendinous xanthomatosis.
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[<a href="/pmc/articles/PMC4449724/" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pmc">PMC free article<span class="bk_prnt">: PMC4449724</span></a>] [<a href="https://pubmed.ncbi.nlm.nih.gov/2019602" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pubmed">PubMed<span class="bk_prnt">: 2019602</span></a>]</div></li><li class="half_rhythm"><div class="bk_ref" id="ctx.REF.catarino.2018.388">Catarino
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G, Del Puppo
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G. Case report: early treatment with chenodeoxycholic acid in cerebrotendinous xanthomatosis presenting as neonatal cholestasis.
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TC, Kfir
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[<a href="https://pubmed.ncbi.nlm.nih.gov/11706139" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pubmed">PubMed<span class="bk_prnt">: 11706139</span></a>]</div></li><li class="half_rhythm"><div class="bk_ref" id="ctx.REF.fraidakis.2013.e302">Fraidakis
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[<a href="/pmc/articles/PMC3784765/" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pmc">PMC free article<span class="bk_prnt">: PMC3784765</span></a>] [<a href="https://pubmed.ncbi.nlm.nih.gov/24002088" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pubmed">PubMed<span class="bk_prnt">: 24002088</span></a>]</div></li><li class="half_rhythm"><div class="bk_ref" id="ctx.REF.freedman.2019.1312">Freedman
SF, Brennand
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MA, Duell
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R. Prevalence of cerebrotendinous xanthomatosis among patients diagnosed with acquired juvenile-onset idiopathic bilateral cataracts.
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[<a href="https://pubmed.ncbi.nlm.nih.gov/15795599" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pubmed">PubMed<span class="bk_prnt">: 15795599</span></a>]</div></li><li class="half_rhythm"><div class="bk_ref" id="ctx.REF.zhang.2021.116">Zhang
P, Zhao
J, Peng
XM, Qian
YY, Zhao
XM, Zhou
WH, Wang
JS, Wu
BB, Wang
HJ. Cholestasis as a dominating symptom of patients with CYP27A1 mutations: an analysis of 17 Chinese infants.
J Clin Lipidol.
2021;15:116&#x02013;23.
[<a href="https://pubmed.ncbi.nlm.nih.gov/33414089" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pubmed">PubMed<span class="bk_prnt">: 33414089</span></a>]</div></li><li class="half_rhythm"><div class="bk_ref" id="ctx.REF.zhang.2020.1372">Zhang
S, Li
W, Zheng
R, Zhao
B, Zhang
Y, Zhao
D, Zhao
C, Yan
C, Zhao
Y. Cerebrotendinous xanthomatosis with peripheral neuropathy: a clinical and neurophysiological study in Chinese population.
Ann Transl Med.
2020;8:1372.
[<a href="/pmc/articles/PMC7723652/" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pmc">PMC free article<span class="bk_prnt">: PMC7723652</span></a>] [<a href="https://pubmed.ncbi.nlm.nih.gov/33313117" ref="pagearea=cite-ref&amp;targetsite=entrez&amp;targetcat=link&amp;targettype=pubmed">PubMed<span class="bk_prnt">: 33313117</span></a>]</div></li></ul></div></div><div id="bk_toc_contnr"></div></div></div>
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