Exome sequencing identifies WDR35 variants involved in Sensenbrenner syndrome.

Authors :: Gilissen, C.F.H.A.
Arts, H.H.
Hoischen, A.
Spruijt, L.
Mans, D.A.
Arts, P.J.W.
Lier, B. van
Steehouwer, M.
Reeuwijk, J. van
Kant, S.G.
Roepman, R.
Knoers, N.V.A.M.
Veltman, J.A.
Brunner, H.G.
Gilissen, C.F.H.A.
Arts, H.H.
Hoischen, A.
Spruijt, L.
Mans, D.A.
Arts, P.J.W.
Lier, B. van
Steehouwer, M.
Reeuwijk, J. van
Kant, S.G.
Roepman, R.
Knoers, N.V.A.M.
Veltman, J.A.
Brunner, H.G.
Source :: American Journal of Human Genetics; 418; 23; 0002-9297; 3; vol. 87; ~American Journal of Human Genetics~418~23~~~0002-9297~3~87~~
Publication Year :: 2010
Abstract: Contains fulltext : 88664.pdf (publisher's version ) (Closed access)<br />Sensenbrenner syndrome/cranioectodermal dysplasia (CED) is an autosomal-recessive disease that is characterized by craniosynostosis and ectodermal and skeletal abnormalities. We sequenced the exomes of two unrelated CED patients and identified compound heterozygous mutations in WDR35 as the cause of the disease in each of the two patients independently, showing that it is possible to find the causative gene by sequencing the exome of a single sporadic patient. With RT-PCR, we demonstrate that a splice-site mutation in exon 2 of WDR35 alters splicing of RNA on the affected allele, introducing a premature stop codon. WDR35 is homologous to TULP4 (from the Tubby superfamily) and has previously been characterized as an intraflagellar transport component, confirming that Sensenbrenner syndrome is a ciliary disorder.

Database :: OAIster
Journal :: American Journal of Human Genetics; 418; 23; 0002-9297; 3; vol. 87; ~American Journal of Human Genetics~418~23~~~0002-9297~3~87~~
Publication Type :: Electronic Resource
Accession number :: edsoai.on1284157330
Document Type :: Electronic Resource