| Literature DB >> 24804704 |
Junichi Suzuki1, Noriyuki Azuma2, Sumito Dateki3, Shun Soneda4, Koji Muroya5, Yukiyo Yamamoto6, Reiko Saito6, Shinichiro Sano4, Toshiro Nagai7, Hiroshi Wada8, Akira Endo9, Tatsuhiko Urakami10, Tsutomu Ogata11, Maki Fukami4.
Abstract
Multiple mutations in SOX2 have been identified in patients with ocular anomalies and/or pituitary dysfunction. Here, we identified SOX2 abnormalities in nine patients. The molecular defects included one missense, one nonsense and four frameshift mutations, and three submicroscopic deletions involving SOX2. Three of the six mutations and all deletions were hitherto unreported. The breakpoints determined in one deletion were located within Alu repeats and accompanied by an overlap of 11 bp. Three of the six mutations encoded SOX2 proteins that lacked in vitro transactivation activity for the HESX1 promoter, whereas the remaining three generated proteins with ∼15-∼20% of transactivation activity. All cases manifested ocular anomalies of various severities, together with several complications including arachnoid cyst and hamartoma. There was no apparent correlation between the residual activity and clinical severity. The results indicate that molecular defects in SOX2 are highly variable and include Alu repeat-mediated genomic rearrangements. Our data provide further evidence for wide phenotypic variation of SOX2 abnormalities and the lack of genotype-phenotype correlation in patients carrying SOX2 lesions.Entities:
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Year: 2014 PMID: 24804704 DOI: 10.1038/jhg.2014.34
Source DB: PubMed Journal: J Hum Genet ISSN: 1434-5161 Impact factor: 3.172