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Mutations in RIT1 cause Noonan syndrome – additional functional evidence and expanding the clinical phenotype

Identifieur interne : 003284 ( Pmc/Curation ); précédent : 003283; suivant : 003285

Mutations in RIT1 cause Noonan syndrome – additional functional evidence and expanding the clinical phenotype

Auteurs : Martin Koenighofer [Autriche] ; Christina Y. Hung [États-Unis] ; Jacob L. Mccauley [États-Unis] ; Julia Dallman [États-Unis] ; Emma J. Back [États-Unis] ; Ivana Mihalek [Singapour] ; Karen W. Gripp [États-Unis] ; Katia Sol-Church [États-Unis] ; Paolo Rusconi [États-Unis] ; Zhaiyi Zhang [États-Unis] ; Geng-Xian Shi [États-Unis] ; Douglas A. Andres [États-Unis] ; Olaf A. Bodamer [États-Unis]

Source :

RBID : PMC:4760689

Abstract

RASopathies are a clinically heterogeneous group of conditions caused by mutations in one of sixteen proteins in the RAS-MAPK pathway. Recently, mutations in RIT1 were identified as a novel cause for Noonan syndrome. Here we provide additional functional evidence for a causal role of RIT1 mutations and expand the associated phenotypic spectrum.

We identified two de novo missense variants p.Met90Ile and, p.Ala57Gly. Both variants resulted in increased MEK-ERK signaling compared to wild-type, underscoring gain-of-function as the primary functional mechanism. Introduction of p.Met90Ile and p.Ala57Gly into zebrafish embryos reproduced not only aspects of the human phenotype but also revealed abnormalities of eye development, emphasizing the importance of RIT1 for spatial and temporal organization of the growing organism. In addition, we observed severe lymphedema of the lower extremity and genitalia in one patient.

We provide additional evidence for a causal relationship between pathogenic mutations in RIT1, increased RAS-MAPK/MEK-ERK signaling and the clinical phenotype. The mutant RIT1 protein may possess reduced GTPase activity or a diminished ability to interact with cellular GTPase activating proteins, however the precise mechanism remains unknown. The phenotypic spectrum is likely to expand and includes lymphedema of the lower extremities in addition to nuchal hygroma.


Url:
DOI: 10.1111/cge.12608
PubMed: 25959749
PubMed Central: 4760689

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PMC:4760689

Le document en format XML

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<p id="P1">RASopathies are a clinically heterogeneous group of conditions caused by mutations in one of sixteen proteins in the RAS-MAPK pathway. Recently, mutations in
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<p id="P2">We identified two
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missense variants p.Met90Ile and, p.Ala57Gly. Both variants resulted in increased MEK-ERK signaling compared to wild-type, underscoring gain-of-function as the primary functional mechanism. Introduction of p.Met90Ile and p.Ala57Gly into zebrafish embryos reproduced not only aspects of the human phenotype but also revealed abnormalities of eye development, emphasizing the importance of
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<p id="P3">We provide additional evidence for a causal relationship between pathogenic mutations in
<italic>RIT1</italic>
, increased RAS-MAPK/MEK-ERK signaling and the clinical phenotype. The mutant RIT1 protein may possess reduced GTPase activity or a diminished ability to interact with cellular GTPase activating proteins, however the precise mechanism remains unknown. The phenotypic spectrum is likely to expand and includes lymphedema of the lower extremities in addition to nuchal hygroma.</p>
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<given-names>Douglas A.</given-names>
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Department of Otorhinolaryngology, Medical University of Vienna, Austria</aff>
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Division of Genetics and Genomics, Boston Children’s Hospital, Boston, MA, USA</aff>
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Dr. John T. Macdonald Foundation Department of Human Genetics and John P. Hussman Institute for Human Genomics, University of Miami, Miller School of Medicine, FL, USA</aff>
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Department of Biology, University of Miami, FL, USA</aff>
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Bioinformatics Institute A
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STAR Singapore, Singapore</aff>
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Division of Medical Genetics, Alfred I. duPont Hospital for Children, Wilmington, DE, USA</aff>
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Division of Pediatric Cardiology, Department of Pediatrics, University of Miami, Miller School of Medicine, FL, USA</aff>
<aff id="A8">
<label>8</label>
Department of Molecular and Cellular Biochemistry, University of Kentucky, College of Medicine, Lexington, KY, USA</aff>
<aff id="A9">
<label>9</label>
Harvard Medical School, Boston, MA, USA</aff>
<author-notes>
<corresp id="FN1">Correspondence to: Olaf A. Bodamer, MD, PhD, FACMG, FAAP; Division of Genetics and Genomics, Department of Medicine, Boston Children’s Hospital, 300 Longwood Avenue, Boston MA 02115. Tel: 8572185544 Fax: 6177300466;
<email>olaf.bodamer@childrens.harvard.edu</email>
</corresp>
<fn id="FN2" fn-type="equal">
<label>*</label>
<p>these authors contributed equally</p>
</fn>
</author-notes>
<pub-date pub-type="nihms-submitted">
<day>30</day>
<month>5</month>
<year>2015</year>
</pub-date>
<pub-date pub-type="epub">
<day>04</day>
<month>6</month>
<year>2015</year>
</pub-date>
<pub-date pub-type="ppub">
<month>3</month>
<year>2016</year>
</pub-date>
<pub-date pub-type="pmc-release">
<day>01</day>
<month>3</month>
<year>2017</year>
</pub-date>
<volume>89</volume>
<issue>3</issue>
<fpage>359</fpage>
<lpage>366</lpage>
<pmc-comment>elocation-id from pubmed: 10.1111/cge.12608</pmc-comment>
<abstract>
<p id="P1">RASopathies are a clinically heterogeneous group of conditions caused by mutations in one of sixteen proteins in the RAS-MAPK pathway. Recently, mutations in
<italic>RIT1</italic>
were identified as a novel cause for Noonan syndrome. Here we provide additional functional evidence for a causal role of
<italic>RIT1</italic>
mutations and expand the associated phenotypic spectrum.</p>
<p id="P2">We identified two
<italic>de novo</italic>
missense variants p.Met90Ile and, p.Ala57Gly. Both variants resulted in increased MEK-ERK signaling compared to wild-type, underscoring gain-of-function as the primary functional mechanism. Introduction of p.Met90Ile and p.Ala57Gly into zebrafish embryos reproduced not only aspects of the human phenotype but also revealed abnormalities of eye development, emphasizing the importance of
<italic>RIT1</italic>
for spatial and temporal organization of the growing organism. In addition, we observed severe lymphedema of the lower extremity and genitalia in one patient.</p>
<p id="P3">We provide additional evidence for a causal relationship between pathogenic mutations in
<italic>RIT1</italic>
, increased RAS-MAPK/MEK-ERK signaling and the clinical phenotype. The mutant RIT1 protein may possess reduced GTPase activity or a diminished ability to interact with cellular GTPase activating proteins, however the precise mechanism remains unknown. The phenotypic spectrum is likely to expand and includes lymphedema of the lower extremities in addition to nuchal hygroma.</p>
</abstract>
<kwd-group>
<kwd>Costello syndrome</kwd>
<kwd>Noonan syndrome</kwd>
<kwd>RASopathy</kwd>
<kwd>RIT1</kwd>
</kwd-group>
</article-meta>
</front>
</pmc>
</record>

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