| Literature DB >> 21664999 |
Emma M M Burkitt Wright1, Helen L Spencer1, Sarah B Daly1, Forbes D C Manson1, Leo A H Zeef2, Jill Urquhart1, Nicoletta Zoppi3, Richard Bonshek4, Ioannis Tosounidis5, Meyyammai Mohan6, Colm Madden7, Annabel Dodds8, Kate E Chandler1, Siddharth Banka1, Leon Au9, Jill Clayton-Smith1, Naz Khan1, Leslie G Biesecker10, Meredith Wilson11, Marianne Rohrbach12, Marina Colombi3, Cecilia Giunta12, Graeme C M Black13.
Abstract
Extreme corneal fragility and thinning, which have a high risk of catastrophic spontaneous rupture, are the cardinal features of brittle cornea syndrome (BCS), an autosomal-recessive generalized connective tissue disorder. Enucleation is frequently the only management option for this condition, resulting in blindness and psychosocial distress. Even when the cornea remains grossly intact, visual function could also be impaired by a high degree of myopia and keratoconus. Deafness is another common feature and results in combined sensory deprivation. Using autozygosity mapping, we identified mutations in PRDM5 in families with BCS. We demonstrate that regulation of expression of extracellular matrix components, particularly fibrillar collagens, by PRDM5 is a key molecular mechanism that underlies corneal fragility in BCS and controls normal corneal development and maintenance. ZNF469, encoding a zinc finger protein of hitherto undefined function, has been identified as a quantitative trait locus for central corneal thickness, and mutations in this gene have been demonstrated in Tunisian Jewish and Palestinian kindreds with BCS. We show that ZNF469 and PRDM5, two genes that when mutated cause BCS, participate in the same regulatory pathway.Entities:
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Year: 2011 PMID: 21664999 PMCID: PMC3113239 DOI: 10.1016/j.ajhg.2011.05.007
Source DB: PubMed Journal: Am J Hum Genet ISSN: 0002-9297 Impact factor: 11.025