Absence of NR2E1 mutations in patients with aniridia.

[aniridia]

Nuclear receptor 2 E 1 (NR 2 E 1 ) is a transcription factor with many roles during eye development and thus may be responsible for the occurrence of certain congenital eye disorders in humans . To test this hypothesis , we screened NR 2 E 1 for candidate mutations in patients with aniridia and other congenital ocular malformations (anterior segment dysgenesis , congenital optic nerve malformation , and microphthalmia ).The NR 2 E 1 coding region , 5 ' and 3 ' untranslated regions (UTRs ), exon flanking regions including consensus splice sites , and six evolutionarily conserved non-coding candidate regulatory regions were analyzed by sequencing 58 probands with aniridia of whom 42 were negative for PAX 6 mutations . Nineteen probands with anterior segment dysgenesis , one proband with optic nerve malformation , and two probands with microphthalmia were also sequenced . The control population comprised 376 healthy individuals . All sequences were analyzed against the GenBank sequence AL 078596 .8 for NR 2 E 1 . In addition , the coding region and flanking intronic sequences of FOXE 3 , FOXC 1 , PITX 2 , CYP 1 B 1 , PAX 6 , and B 3 GALTL were sequenced in one patient and his relatives .Sequencing analysis showed 17 NR 2 E 1 variants including two novel rare non-coding variants (g .-1507 G >A , g .14258 C >T ), and one novel rare coding variant (p .Arg 274 Gly ). The latter was present in a male diagnosed with Peters ' anomaly who subsequently was found to have a known causative mutation for Peters ' plus syndrome in B 3 GALTL (c .660 +1 G >A ). In addition , the NR 2 E 1 novel rare variant Arg 274 G ly was present in the unaffected mother of the patient but absent in 746 control chromosomes .We eliminated a major role for NR 2 E 1 regulatory and coding mutations in aniridia and found a novel rare coding variant in NR 2 E 1 . In addition , we found no coding region variation in the control population for NR 2 E 1 , which further supports its previously reported high level of conservation and low genetic diversity . Future NR 2 E 1 studies in ocular disease groups such as those involving retinal and optic nerve abnormalities should be undertaken to determine whether NR 2 E 1 plays a role in these conditions .

Diseases
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Diseases presenting "previously reported high level" symptom

aniridia

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