Mutations of CEP83 Cause Infantile Nephronophthisis and Intellectual Disability
Tarih
2014Yazar
Braun, Daniela A.
Kayserili, Hulya
Failler, Marion
Gee, Heon Yung
Krug, Pauline
Joo, Kwangsic
Halbritter, Jan
Belkacem, Lilya
Filhol, Emilie
Porath, Jonathan D.
Schueler, Markus
Frigo, Amandine
Alibeu, Olivier
Masson, Cecile
Brochard, Karine
de Ligny, Bruno Hurault
Novo, Robert
Pietrement, Christine
Salomon, Remi
Gubler, Marie-Claire
Otto, Edgar A.
Antignac, Corinne
Kim, Joon
Benmerah, Alexandre
Hildebrandt, Friedhelm
Saunier, Sophie
Üst veri
Tüm öğe kaydını gösterÖzet
Ciliopathies are a group of hereditary disorders associated with defects in cilia structure and function. The distal appendages (DAPs) of centrioles are involved in the docking and anchoring of the mother centriole to the cellular membrane during ciliogenesis. The molecular composition of DAPs was recently elucidated and mutations in two genes encoding DAPs components (CEP164/NPHP15, SCLT1) have been associated with human ciliopathies, namely nephronophthisis and orofaciodigital syndrome. To identify additional DAP components defective in ciliopathies, we independently performed targeted exon sequencing of 1,221 genes associated with cilia and 5 known DAP protein-encoding genes in 1,255 individuals with a nephronophthisis-related ciliopathy. We thereby detected biallelic mutations in a key component of DAP-encoding gene, CEP83, in seven families. All affected individuals had early-onset nephronophthisis and four out of eight displayed learning disability and/or hydrocephalus. Fibroblasts and tubular renal cells from affected individuals showed an altered DAP composition and ciliary defects. In summary, we have identified mutations in CEP83, another DAP-component-encoding gene, as a cause of infantile nephronophthisis associated with central nervous system abnormalities in half of the individuals.
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