High efficiency of mutation detection in type 1 stickler syndrome using a two-stage approach: vitreoretinal assessment coupled with exon sequencing for screening COL2A1

Stickler syndrome is a genetically heterogenous disorder that affects the ocular, skeletal, and auditory systems. To date three genes, COL2A1, COL11A1, and COL11A2, encoding the heterotypic type II/XI collagen fibrils present in vitreous and cartilage have been shown to have mutations that result in...

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Bibliographic Details
Published in:Human mutation 2006-07, Vol.27 (7), p.696-704
Main Authors: Richards, Allan J., Laidlaw, Maureen, Whittaker, Joanne, Treacy, Becky, Rai, Harjeet, Bearcroft, Philip, Baguley, David M., Poulson, Arabella, Ang, Alan, Scott, John D., Snead, Martin P.
Format: Article
Language:English
Subjects:
Adolescent
Adult
Base Sequence
Child
Child, Preschool
Cleft Palate - genetics
COL11A1
COL11A2
COL2A1
collagen
Collagen Type II - genetics
DNA Mutational Analysis - methods
Exons
Eye Diseases, Hereditary - diagnosis
Eye Diseases, Hereditary - genetics
Eye Diseases, Hereditary - pathology
Female
Genetic Testing
Hearing Loss - genetics
Humans
Male
Middle Aged
Molecular Sequence Data
Mutation
RNA Splice Sites
Stickler
Syndrome
Vitreous Body - abnormalities
Vitreous Body - pathology
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Summary:Stickler syndrome is a genetically heterogenous disorder that affects the ocular, skeletal, and auditory systems. To date three genes, COL2A1, COL11A1, and COL11A2, encoding the heterotypic type II/XI collagen fibrils present in vitreous and cartilage have been shown to have mutations that result in Stickler syndrome. As systemic features in this disorder are variable we have used an ophthalmic examination to differentiate those patients with a membranous vitreous phenotype associated with mutations in COL2A1, from other patients who may have mutations in other genes. Gene amplification and exon sequencing was used to screen 50 families or sporadic cases with this membranous phenotype, for mutations in COL2A1. Mutations were detected in 47 (94%) cases consisting of 166 affected and 78 unaffected individuals. We also demonstrate that the predominantly ocular form of type 1 Stickler syndrome is not confined to mutations in the alternatively spliced exon 2. Using splicing reporter constructs we demonstrate that a mutant GC donor splice site in intron 51 can be spliced normally; this contributed to the predominantly ocular phenotype in the family in which it occurred. Hum Mutat 27(7), 696–704, 2006. © 2006 Wiley‐Liss, Inc.
ISSN:1059-7794
1098-1004
DOI:10.1002/humu.20347