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Biallelic variants in GTF3C3 result in an autosomal recessive disorder with intellectual disability.

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cris.virtualsource.author-orcid35c44611-045c-422d-8533-430abb08b3ae
cris.virtualsource.author-orcid02bd788b-c894-401f-8f3c-368cd59e6904
datacite.rightsopen.access
dc.contributor.authorDe Hayr, Lachlan
dc.contributor.authorBlok, Laura E R
dc.contributor.authorDias, Kerith-Rae
dc.contributor.authorLong, Jingyi
dc.contributor.authorBegemann, Anaïs
dc.contributor.authorMoir, Robyn D
dc.contributor.authorWillis, Ian M
dc.contributor.authorMocera, Martina
dc.contributor.authorSiegel, Gabriele
dc.contributor.authorSteindl, Katharina
dc.contributor.authorEvans, Carey-Anne
dc.contributor.authorZhu, Ying
dc.contributor.authorZhang, Futao
dc.contributor.authorField, Michael
dc.contributor.authorMa, Alan
dc.contributor.authorAdès, Lesley
dc.contributor.authorJosephi-Taylor, Sarah
dc.contributor.authorPfundt, Rolph
dc.contributor.authorZaki, Maha S
dc.contributor.authorTomoum, Hoda
dc.contributor.authorGregor, Anne
dc.contributor.authorLaube, Julia
dc.contributor.authorReis, André
dc.contributor.authorMaddirevula, Sateesh
dc.contributor.authorHashem, Mais O
dc.contributor.authorZweier, Markus
dc.contributor.authorAlkuraya, Fowzan S
dc.contributor.authorMaroofian, Reza
dc.contributor.authorBuckley, Michael F
dc.contributor.authorGleeson, Joseph G
dc.contributor.authorZweier, Christiane
dc.contributor.authorColl-Tané, Mireia
dc.contributor.authorKoolen, David A
dc.contributor.authorRauch, Anita
dc.contributor.authorRoscioli, Tony
dc.contributor.authorSchenck, Annette
dc.contributor.authorHarvey, Robert J
dc.date.accessioned2025-01-07T14:42:20Z
dc.date.available2025-01-07T14:42:20Z
dc.date.issued2025-01
dc.description.abstractPurpose This study details a novel syndromic form of autosomal recessive intellectual disability resulting from recessive variants in GTF3C3, encoding a key component of the DNA-binding transcription factor IIIC, which has a conserved role in RNA polymerase III-mediated transcription. Methods Exome sequencing, minigene analysis, molecular modeling, RNA polymerase III reporter gene assays, and Drosophila knockdown models were utilized to characterize GTF3C3 variants. Results Twelve affected individuals from 7 unrelated families were identified with homozygous or compound heterozygous missense variants in GTF3C3 including c.503C>T p.(Ala168Val), c.1268T>C p.(Leu423Pro), c.1436A>G p.(Tyr479Cys), c.2419C>T p.(Arg807Cys), and c.2420G>A p.(Arg807His). The cohort presented with intellectual disability, variable nonfamilial facial features, motor impairments, seizures, and cerebellar/corpus callosum malformations. Consistent with disruptions in intra- and intermolecular interactions observed in molecular modeling, RNA polymerase III reporter assays confirmed that the majority of missense variants resulted in a loss of function. Minigene analysis of the recurrent c.503C>T p.(Ala168Val) variant confirmed the introduction of a cryptic donor site into exon 4, resulting in mRNA missplicing. Consistent with the clinical features of this cohort, neuronal loss of Gtf3c3 in Drosophila induced seizure-like behavior, motor impairment, and learning deficits. Conclusion These findings confirm that GTF3C3 variants result in an autosomal recessive form of syndromic intellectual disability.
dc.description.numberOfPages1
dc.description.sponsorshipClinic of Human Genetics
dc.identifier.doi10.48620/78888
dc.identifier.pmid39636576
dc.identifier.publisherDOI10.1016/j.gim.2024.101253
dc.identifier.urihttps://boris-portal.unibe.ch/handle/20.500.12422/194314
dc.language.isoen
dc.publisherElsevier
dc.relation.ispartofGenetics in Medicine
dc.relation.issn1530-0366
dc.relation.issn1098-3600
dc.subjectGTF3C3
dc.subjectIntellectual disability
dc.subjectMinigene analysis
dc.subjectRNA polymerase III
dc.subjectTfc4
dc.subject.ddc600 - Technology::610 - Medicine & health
dc.titleBiallelic variants in GTF3C3 result in an autosomal recessive disorder with intellectual disability.
dc.typearticle
dspace.entity.typePublication
dspace.file.typetext
oaire.citation.issue1
oaire.citation.startPage101253
oaire.citation.volume27
oairecerif.author.affiliationClinic of Human Genetics
oairecerif.author.affiliationClinic of Human Genetics
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unibe.description.ispublishedpub
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unibe.subtype.articlejournal

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