Open AccessNR2F1 Mutations Cause Optic Atrophy with Intellectual Disability
Author(s) -
Daniëlle G.M. Bosch,
F. Nienke Boonstra,
Claudia GonzagaJauregui,
Mafei Xu,
Joep de Ligt,
Shalini N. Jhangiani,
Wojciech Wiszniewski,
Donna M. Muzny,
Helger G. Yntema,
Rolph Pfundt,
Lisenka E.L.M. Vissers,
Liesbeth Spruijt,
Ellen A.W. Blokland,
ChunAn Chen,
Richard A. Lewis,
Sophia Y. Tsai,
Richard A. Gibbs,
MingJer Tsai,
James R. Lupski,
Huda Y. Zoghbi,
Frans P.M. Cremers,
Bert B.A. de Vries,
Christian P. Schaaf
Publication year - 2014
Publication title -
the american journal of human genetics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 6.661
H-Index - 302
eISSN - 1537-6605
pISSN - 0002-9297
DOI - 10.1016/j.ajhg.2014.01.002
Subject(s) - atrophy , intellectual disability , medicine , psychiatry
Optic nerve atrophy and hypoplasia can be primary disorders or can result from trans-synaptic degeneration arising from cerebral visual impairment (CVI). Here we report six individuals with CVI and/or optic nerve abnormalities, born after an uneventful pregnancy and delivery, who have either de novo heterozygous missense mutations in NR2F1, also known as COUP-TFI, or deletions encompassing NR2F1. All affected individuals show mild to moderate intellectual impairment. NR2F1 encodes a nuclear receptor protein that regulates transcription. A reporter assay showed that missense mutations in the zinc-finger DNA-binding domain and the putative ligand-binding domain decrease NR2F1 transcriptional activity. These findings indicate that NR2F1 plays an important role in the neurodevelopment of the visual system and that its disruption can lead to optic atrophy with intellectual disability.
Accelerating Research
Robert Robinson Avenue,
Oxford Science Park, Oxford
OX4 4GP, United Kingdom
Address
John Eccles HouseRobert Robinson Avenue,
Oxford Science Park, Oxford
OX4 4GP, United Kingdom