BMP4 loss-of-function mutations in developmental eye disorders including SHORT syndrome

被引:0
|
作者
Linda M. Reis
Rebecca C. Tyler
Kala F. Schilter
Omar Abdul-Rahman
Jeffrey W. Innis
Beth A. Kozel
Adele S. Schneider
Tanya M. Bardakjian
Edward J. Lose
Donna M. Martin
Ulrich Broeckel
Elena V. Semina
机构
[1] Medical College of Wisconsin,Department of Pediatrics
[2] Children’s Hospital of Wisconsin,Children’s Research Institute
[3] Medical College of Wisconsin,Department of Cell Biology, Neurobiology and Anatomy
[4] The University of Michigan Medical Center,Department of Pediatrics and Human Genetics
[5] University of Mississippi Medical Center,Department of Pediatrics
[6] Washington University School of Medicine,Division of Genetics and Genomic Medicine, Department of Pediatrics
[7] Albert Einstein Medical Center,Division of Genetics, Department of Pediatrics
[8] University of Alabama,Department of Clinical Genetics
[9] C3520,undefined
[10] Translational and Biomedical Research Center,undefined
[11] Medical College of Wisconsin,undefined
来源
Human Genetics | 2011年 / 130卷
关键词
High Myopia; Microphthalmia; Brain Anomaly; Postaxial Polydactyly; Craniofacial Dysmorphism;
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中图分类号
学科分类号
摘要
BMP4 loss-of-function mutations and deletions have been shown to be associated with ocular, digital, and brain anomalies, but due to the paucity of these reports, the full phenotypic spectrum of human BMP4 mutations is not clear. We screened 133 patients with a variety of ocular disorders for BMP4 coding region mutations or genomic deletions. BMP4 deletions were detected in two patients: a patient affected with SHORT syndrome and a patient with anterior segment anomalies along with craniofacial dysmorphism and cognitive impairment. In addition to this, three intragenic BMP4 mutations were identified. A patient with anophthalmia, microphthalmia with sclerocornea, right-sided diaphragmatic hernia, and hydrocephalus was found to have a c.592C>T (p.R198X) nonsense mutation in BMP4. A frameshift mutation, c.171dupC (p.E58RfsX17), was identified in two half-siblings with anophthalmia/microphthalmia, discordant developmental delay/postaxial polydactyly, and poor growth as well as their unaffected mother; one affected sibling carried an additional BMP4 mutation in the second allele, c.362A>G (p.H121R). This is the first report indicating a role for BMP4 in SHORT syndrome, Axenfeld–Rieger malformation, growth delay, macrocephaly, and diaphragmatic hernia. These results significantly expand the number of reported loss-of-function mutations, further support the critical role of BMP4 in ocular development, and provide additional evidence of variable expression/non-penetrance of BMP4 mutations.
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页码:495 / 504
页数:9
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