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Mutations in the JARID1C Gene, Which Is Involved in Transcriptional Regulation and Chromatin Remodeling, Cause X-Linked Mental Retardation

Identifieur interne : 000036 ( Pmc/Corpus ); précédent : 000035; suivant : 000037

Mutations in the JARID1C Gene, Which Is Involved in Transcriptional Regulation and Chromatin Remodeling, Cause X-Linked Mental Retardation

Auteurs : Lars Riff Jensen ; Marion Amende ; Ulf Gurok ; Bettina Moser ; Verena Gimmel ; Andreas Tzschach ; Andreas R. Janecke ; Gholamali Tariverdian ; Jamel Chelly ; Jean-Pierre Fryns ; Hilde Van Esch ; Tjitske Kleefstra ; Ben Hamel ; Claude Moraine ; Jozef Gécz ; Gillian Turner ; Richard Reinhardt ; Vera M. Kalscheuer ; Hans-Hilger Ropers ; Steffen Lenzner

Source :

RBID : PMC:1196368

Abstract

In families with nonsyndromic X-linked mental retardation (NS-XLMR), >30% of mutations seem to cluster on proximal Xp and in the pericentric region. In a systematic screen of brain-expressed genes from this region in 210 families with XLMR, we identified seven different mutations in JARID1C, including one frameshift mutation and two nonsense mutations that introduce premature stop codons, as well as four missense mutations that alter evolutionarily conserved amino acids. In two of these families, expression studies revealed the almost complete absence of the mutated JARID1C transcript, suggesting that the phenotype in these families results from functional loss of the JARID1C protein. JARID1C (Jumonji AT-rich interactive domain 1C), formerly known as “SMCX,” is highly similar to the Y-chromosomal gene JARID1D/SMCY, which encodes the H-Y antigen. The JARID1C protein belongs to the highly conserved ARID protein family. It contains several DNA-binding motifs that link it to transcriptional regulation and chromatin remodeling, processes that are defective in various other forms of mental retardation. Our results suggest that JARID1C mutations are a relatively common cause of XLMR and that this gene might play an important role in human brain function.


Url:
PubMed: 15586325
PubMed Central: 1196368

Links to Exploration step

PMC:1196368

Le document en format XML

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<p>In families with nonsyndromic X-linked mental retardation (NS-XLMR), >30% of mutations seem to cluster on proximal Xp and in the pericentric region. In a systematic screen of brain-expressed genes from this region in 210 families with XLMR, we identified seven different mutations in
<italic>JARID1C,</italic>
including one frameshift mutation and two nonsense mutations that introduce premature stop codons, as well as four missense mutations that alter evolutionarily conserved amino acids. In two of these families, expression studies revealed the almost complete absence of the mutated
<italic>JARID1C</italic>
transcript, suggesting that the phenotype in these families results from functional loss of the JARID1C protein.
<italic>JARID1C</italic>
(Jumonji AT-rich interactive domain 1C), formerly known as “
<italic>SMCX,</italic>
” is highly similar to the Y-chromosomal gene
<italic>JARID1D/SMCY,</italic>
which encodes the H-Y antigen. The JARID1C protein belongs to the highly conserved ARID protein family. It contains several DNA-binding motifs that link it to transcriptional regulation and chromatin remodeling, processes that are defective in various other forms of mental retardation. Our results suggest that
<italic>JARID1C</italic>
mutations are a relatively common cause of XLMR and that this gene might play an important role in human brain function.</p>
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<italic>JARID1C</italic>
Gene, Which Is Involved in Transcriptional Regulation and Chromatin Remodeling, Cause X-Linked Mental Retardation</article-title>
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<italic>JARID1C</italic>
: A New XLMR Gene</alt-title>
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<surname>Jensen</surname>
<given-names>Lars Riff</given-names>
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<name>
<surname>Amende</surname>
<given-names>Marion</given-names>
</name>
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<name>
<surname>Gurok</surname>
<given-names>Ulf</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Moser</surname>
<given-names>Bettina</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Gimmel</surname>
<given-names>Verena</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
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<contrib contrib-type="author">
<name>
<surname>Tzschach</surname>
<given-names>Andreas</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Janecke</surname>
<given-names>Andreas R.</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">2</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Tariverdian</surname>
<given-names>Gholamali</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">3</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Chelly</surname>
<given-names>Jamel</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">4</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Fryns</surname>
<given-names>Jean-Pierre</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">5</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Van Esch</surname>
<given-names>Hilde</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">5</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Kleefstra</surname>
<given-names>Tjitske</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">6</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Hamel</surname>
<given-names>Ben</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">6</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Moraine</surname>
<given-names>Claude</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">7</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Gécz</surname>
<given-names>Jozef</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">8</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Turner</surname>
<given-names>Gillian</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">9</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Reinhardt</surname>
<given-names>Richard</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Kalscheuer</surname>
<given-names>Vera M.</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Ropers</surname>
<given-names>Hans-Hilger</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
</contrib>
<contrib contrib-type="author">
<name>
<surname>Lenzner</surname>
<given-names>Steffen</given-names>
</name>
<xref ref-type="aff" rid="N0x91eb288.0x95de778">1</xref>
</contrib>
</contrib-group>
<aff id="N0x91eb288.0x95de778">
<sup>1</sup>
Max Planck Institute for Molecular Genetics, Berlin;
<sup>2</sup>
Department of Medical Biology and Human Genetics, Innsbruck Medical University, Innsbruck;
<sup>3</sup>
Institute for Human Genetics, University Heidelberg, Heidelberg;
<sup>4</sup>
Institut Cochin de Génétique Moleculaire, CNRS/INSERM, CHU Cochin, Paris;
<sup>5</sup>
Center for Human Genetics, Clinical Genetics Unit, Leuven, Belgium;
<sup>6</sup>
Department of Human Genetics, University Medical Centre, Nijmegen, The Netherlands;
<sup>7</sup>
Services de Génétique-INSERM U316, CHU Bretonneau, Tours, France;
<sup>8</sup>
Women’s and Children’s Hospital and the University of Adelaide, Adelaide; and
<sup>9</sup>
Genetics of Learning Disability (GOLD) Service, Hunter Genetics, University of Newcastle, New South Wales, Australia</aff>
<author-notes>
<corresp>Address for correspondence and reprints: Dr. Steffen Lenzner, Max Planck Institute for Molecular Genetics, Ihnestrasse 73, D-14195 Berlin, Germany. E-mail:
<email>Lenzner@molgen.mpg.de</email>
</corresp>
</author-notes>
<pub-date pub-type="ppub">
<month>2</month>
<year>2005</year>
</pub-date>
<pub-date pub-type="epub">
<day>7</day>
<month>12</month>
<year>2004</year>
</pub-date>
<volume>76</volume>
<issue>2</issue>
<fpage>227</fpage>
<lpage>236</lpage>
<history>
<date date-type="received">
<day>7</day>
<month>9</month>
<year>2004</year>
</date>
<date date-type="accepted">
<day>17</day>
<month>11</month>
<year>2004</year>
</date>
</history>
<copyright-statement>© 2004 by The American Society of Human Genetics. All rights reserved.</copyright-statement>
<copyright-year>2004</copyright-year>
<self-uri>15586325</self-uri>
<abstract>
<p>In families with nonsyndromic X-linked mental retardation (NS-XLMR), >30% of mutations seem to cluster on proximal Xp and in the pericentric region. In a systematic screen of brain-expressed genes from this region in 210 families with XLMR, we identified seven different mutations in
<italic>JARID1C,</italic>
including one frameshift mutation and two nonsense mutations that introduce premature stop codons, as well as four missense mutations that alter evolutionarily conserved amino acids. In two of these families, expression studies revealed the almost complete absence of the mutated
<italic>JARID1C</italic>
transcript, suggesting that the phenotype in these families results from functional loss of the JARID1C protein.
<italic>JARID1C</italic>
(Jumonji AT-rich interactive domain 1C), formerly known as “
<italic>SMCX,</italic>
” is highly similar to the Y-chromosomal gene
<italic>JARID1D/SMCY,</italic>
which encodes the H-Y antigen. The JARID1C protein belongs to the highly conserved ARID protein family. It contains several DNA-binding motifs that link it to transcriptional regulation and chromatin remodeling, processes that are defective in various other forms of mental retardation. Our results suggest that
<italic>JARID1C</italic>
mutations are a relatively common cause of XLMR and that this gene might play an important role in human brain function.</p>
</abstract>
</article-meta>
</front>
</pmc>
</record>

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