Homozygous mutations in PXDN cause congenital cataract, corneal opacity, and developmental glaucoma
journal contribution
posted on 2023-05-17, 23:50authored byKhan, K, Rudkin, A, Parry, DA, Kathryn BurdonKathryn Burdon, McKibbin, M, Logan, CV, Abdelhamed, ZIA, Muecke, JS, Fernandez-Fuentes, N, Laurie, KJ, Shires, M, Fogarty, R, Carr, IM, Poulter, JA, Morgan, JE, Mohamed, MD, Jafri, H, Raashid, Y, Meng, N, Piseth, H, Toomes, C, Casson, RJ, Taylor, GR, Hammerton, M, Sheridan, E, Johnson, CA, Inglehearn, CF, Craig, JE, Ali, M
Anterior segment dysgenesis describes a group of heterogeneous developmental disorders that affect the anterior chamber of the eye and are associated with an increased risk of glaucoma. Here, we report homozygous mutations in peroxidasin (PXDN) in two consanguineous Pakistani families with congenital cataract-microcornea with mild to moderate corneal opacity and in a consanguineous Cambodian family with developmental glaucoma and severe corneal opacification. These results highlight the diverse ocular phenotypes caused by PXDN mutations, which are likely due to differences in genetic background and environmental factors. Peroxidasin is an extracellular matrix-associated protein with peroxidase catalytic activity, and we confirmed localization of the protein to the cornea and lens epithelial layers. Our findings imply that peroxidasin is essential for normal development of the anterior chamber of the eye, where it may have a structural role in supporting cornea and lens architecture as well as an enzymatic role as an antioxidant enzyme in protecting the lens, trabecular meshwork, and cornea against oxidative damage.
History
Publication title
American Journal of Human Genetics: A Record of Research, Review and Bibliographic Material Relating to Heredity in Man
Volume
89
Pagination
464-473
ISSN
0002-9297
Department/School
Menzies Institute for Medical Research
Publisher
Univ Chicago Press
Place of publication
1427 E 60Th St, Chicago, USA, Il, 60637-2954
Rights statement
Copyright 2011 The American Society of Human Genetics