Novel heterozygous<i>OTX2</i>mutations and whole gene deletions in anophthalmia, microphthalmia and coloboma

Alexander W. Wyatt; Preeti Bakrania; David J. Bunyan; Robert J. Osborne; John A. Crolla; Alison Salt; Carmen Ayuso; Ruth Newbury‐Ecob; Yassir Abou-Rayyah; J. R. O. Collin; David Robinson; Nicola Ragge

doi:10.1002/humu.20869

Novel heterozygous<i>OTX2</i>mutations and whole gene deletions in anophthalmia, microphthalmia and coloboma

Alexander W. Wyatt(University of Oxford), Preeti Bakrania(University of Oxford), David J. Bunyan(Salisbury University), Robert J. Osborne(University of Oxford), John A. Crolla(Salisbury University), Alison Salt(Moorfields Eye Hospital), Carmen Ayuso(Instituto de Salud Carlos III), Ruth Newbury‐Ecob(Royal United Hospital), Yassir Abou-Rayyah(Moorfields Eye Hospital), J. R. O. Collin(University College London), David Robinson(Salisbury University), Nicola Ragge(Moorfields Eye Hospital)

Human Mutation

September 9, 2008

10.1002/humu.20869

Cited by 97Open Access

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Abstract

Severe ocular malformations, including anophthalmia-microphthalmia (AM), are responsible for around 25% of severe visual impairment in childhood. Recurrent interstitial deletions of 14q22-23 are associated with AM and a wide range of extra-ocular phenotypes including brain anomalies. The homeobox gene OTX2 is located at 14q22.3 and has recently been identified as mutated in AM patients. Eight human OTX2 mutations have been reported in subjects with severe eye malformations, including AM, and variable developmental delay. We screened a novel AM cohort for mutations and deletions in OTX2, and identified four new mutations in six individuals and two cases of whole gene deletions. Our data suggest that OTX2 mutations and deletions account for 2-3% of AM cases.

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