Human Molecular Genetics Advance Access first published online on September 19, 2006
This version published online on September 27, 2006
Human Molecular Genetics, doi:10.1093/hmg/ddl392
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1 Wellcome Trust Centre for Human Genetics, University of Oxford, Roosevelt Drive, Oxford, OX3 7BN, UK; Department of Physiology, Anatomy and Genetics, Le Gros Clark Building, South Parks Road, Oxford OX1 3QX, UK
* To whom correspondence should be addressed. Mutations in the FOXP2 gene cause a severe communication disorder involving speech deficits (developmental verbal dyspraxia), accompanied by wide-ranging impairments in expressive and receptive language. The protein encoded by FOXP2 belongs to a divergent subgroup of forkhead-box transcription factors, with a distinctive DNA-binding domain and motifs that mediate hetero- and homodimerisation. Here we report the first direct functional genetic investigation of missense and nonsense mutations in FOXP2 using human cell-lines, including a well established neuronal model system. We focused on three unusual FOXP2 coding variants, uniquely identified in cases of verbal dyspraxia, assessing expression, subcellular localisation, DNA-binding and transactivation properties. Analysis of the R553H forkhead-box substitution, found in all affected members of a large three-generation family, indicated that it severely affects FOXP2 function, chiefly by disrupting nuclear localisation and DNA-binding properties. The R328X truncation mutation, segregating with speech/language disorder in a second family, yields an unstable, predominantly cytoplasmic product that lacks transactivation capacity. A third coding variant (Q17L) observed in a single affected child did not have any detectable functional effect in the present study. In addition, we used the same systems to explore the properties of different isoforms of FOXP2, resulting from alternative splicing in human brain. Notably, one such isoform, FOXP2.10 + , contains dimerisation domains, but no DNA-binding domain, and displayed increased cytoplasmic localisation, coupled with aggresome formation. We hypothesize that expression of alternative isoforms of FOXP2 may provide mechanisms for post-translational regulation of transcription factor function.
Received July 13, 2006
Revised September 11, 2006
Accepted September 11, 2006
Article
Functional genetic analysis of mutations implicated in a human speech and language disorder
Sonja C. Vernes 1, Jérôme Nicod 2, Fanny M. Elahi 2, Julie A. Coventry 2, Niamh Kenny 2, Anne-Marie Coupe 2, Louise E. Bird 2, Kay E. Davies 3, and Simon E. Fisher 2 *
2 Wellcome Trust Centre for Human Genetics, University of Oxford, Roosevelt Drive, Oxford, OX3 7BN, UK
3 Department of Physiology, Anatomy and Genetics, Le Gros Clark Building, South Parks Road, Oxford OX1 3QX, UK
Simon E. Fisher, E-mail: simon.fisher{at};well.ox.ac.uk
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