AI Article Synopsis
- A case study reports an infant with Opitz trigonocephaly C syndrome (OTCS) showing symptoms of ciliopathy, including short ribs and renal dysplasia.
- Exome sequencing revealed two rare mutations in the IFT140 gene linked to the ciliopathy symptoms, inherited from both parents.
- This study is the first to connect IFT140 mutations with OTCS, supporting prior findings of skeletal and nonskeletal ciliopathy traits in OTCS.
Article Abstract
〈 We report on an infant with Opitz trigonocephaly C syndrome (OTCS), who also had manifestations of ciliopathy, including short ribs (non-asphyxiating), trident acetabular roofs, postaxial polydactyly cone-shaped epiphyses, and dysplasia of the renal, hepatic and pancreatic tissues. To investigate the molecular cause, we used an exome sequencing strategy followed by Sanger sequencing. Two rare variants, both predicted to result in loss of functional protein, were identified in the IFT140 gene; a substitution at the splice donor site of exon 24 (c.723 + 1 G > T) and a 17 bp deletion, impacting the first coding exon (c.-11_6del). The variants were confirmed as being biallelic using Sanger sequencing, showing that the splice variant was inherited from the propositus mother and the deletion from the father. To date, Mainzer-Saldino syndrome, Jeune syndrome, and a form of nonsyndromic retinal dystrophy, have been identified as ciliopathies caused by IFT140 mutations. We provide the first description of an OTCS phenotype that appears to result from IFT140 mutations. The presentation of this patient is consistent with previous reports showing that OTCS already exhibited skeleletal and nonskeletal features of a ciliopathy.
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| http://dx.doi.org/10.1111/cge.12924 | DOI Listing |
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