Start Over

Heterozygous missense mutations in SMARCA2 cause Nicolaides-Baraitser syndrome.

Authors :: Van Houdt JK
Nowakowska BA
Sousa SB
van Schaik BD
Seuntjens E
Avonce N
Sifrim A
Abdul-Rahman OA
van den Boogaard MJ
Bottani A
Castori M
Cormier-Daire V
Deardorff MA
Filges I
Fryer A
Fryns JP
Gana S
Garavelli L
Gillessen-Kaesbach G
Hall BD
Horn D
Huylebroeck D
Klapecki J
Krajewska-Walasek M
Kuechler A
Lines MA
Maas S
Macdermot KD
McKee S
Magee A
de Man SA
Moreau Y
Morice-Picard F
Obersztyn E
Pilch J
Rosser E
Shannon N
Stolte-Dijkstra I
Van Dijck P
Vilain C
Vogels A
Wakeling E
Wieczorek D
Wilson L
Zuffardi O
van Kampen AH
Devriendt K
Hennekam R
Vermeesch JR
Source :: Nature genetics [Nat Genet] 2012 Feb 26; Vol. 44 (4), pp. 445-9, S1. Date of Electronic Publication: 2012 Feb 26.
Publication Year :: 2012
Abstract: Nicolaides-Baraitser syndrome (NBS) is characterized by sparse hair, distinctive facial morphology, distal-limb anomalies and intellectual disability. We sequenced the exomes of ten individuals with NBS and identified heterozygous variants in SMARCA2 in eight of them. Extended molecular screening identified nonsynonymous SMARCA2 mutations in 36 of 44 individuals with NBS; these mutations were confirmed to be de novo when parental samples were available. SMARCA2 encodes the core catalytic unit of the SWI/SNF ATP-dependent chromatin remodeling complex that is involved in the regulation of gene transcription. The mutations cluster within sequences that encode ultra-conserved motifs in the catalytic ATPase region of the protein. These alterations likely do not impair SWI/SNF complex assembly but may be associated with disrupted ATPase activity. The identification of SMARCA2 mutations in humans provides insight into the function of the Snf2 helicase family.