In April 2016 Manchester eScholar was replaced by the University of Manchester’s new Research Information Management System, Pure. In the autumn the University’s research outputs will be available to search and browse via a new Research Portal. Until then the University’s full publication record can be accessed via a temporary portal and the old eScholar content is available to search and browse via this archive.

Related resources

Search for item elsewhere

University researcher(s)

Graeme Black's research staff profile

Academic department(s)

Missense and nonsense mutations in the alternatively-spliced exon 2 of COL2A1 cause the ocular variant of Stickler syndrome.

McAlinden A, Majava M, Bishop PN, Bishop PN, Perveen R, Black GCM, Pierpont ME, Ala-Kokko L, Männikkö M

Hum Mutat. 2007;.

Access to files

Full-text and supplementary files are not available from Manchester eScholar. Use our list of Related resources to find this item elsewhere. Alternatively, request a copy from the Library's Document supply service.

Abstract

Stickler syndrome type I (STL1) is a phenotypically heterogeneous disorder characterized by ocular and extraocular features. It is caused by null-allele mutations in the COL2A1 gene that codes for procollagen II. COL2A1 precursor mRNA undergoes alternative splicing, resulting in two isoforms, a long form including exon 2 (type IIA isoform) and a short form excluding exon 2 (type IIB isoform). The short form is predominantly expressed by differentiated chondrocytes in adult cartilage, and the long form in chondroprogenitor cells during early development and in the vitreous of the eye, which is the only adult tissue containing procollagen IIA. Recent evidence indicates that due to the tissue-specific expression of these two isoforms, premature termination codon mutations in exon 2 cause Stickler syndrome with minimal or no extraocular manifestations. We describe here two mutations in exon 2 of COL2A1 in three patients with predominantly ocular Stickler syndrome: Cys64Stop in two patients, and a novel structural mutation, Cys57Tyr, in one patient. RT-PCR of total lymphoblast RNA from one patient with the Cys64Stop mutation revealed that only the normal allele of the IIA form was present, indicating that the mutation resulted either in complete loss of the allele by nonsense-mediated mRNA decay or by skipping of exon 2 via nonsense-mediated altered splicing, resulting in production of the type IIB isoform. The results of COL2A1 minigene expression studies suggest that both Cys64Stop and Cys57Tyr alter positive cis regulatory elements for splicing, resulting in a lower IIA:IIB ratio. Hum Mutat 0, 1-8, 2007. Published 2007 Wiley-Liss, Inc.

Bibliographic metadata

Type of resource:

text

Content type:

Journal article

Publication type:

Original work

Publication form:

Academic journal article

Author list:

McAlinden A, Majava M, Bishop PN, Bishop PN, Perveen R, Black GCM, Pierpont ME, Ala-Kokko L, Männikkö M.

Published date:

2007-1

Article title:

Missense and nonsense mutations in the alternatively-spliced exon 2 of COL2A1 cause the ocular variant of Stickler syndrome.

Journal title:

Hum Mutat

ISSN:

1098-1004

Access state:

Active

Institutional metadata

University researcher(s):

Black, Graeme

Academic department(s):

Record metadata

Manchester eScholar ID:

uk-ac-man-scw:1d16483

Created:

30th August, 2009, 13:58:37

Last modified:

15th April, 2014, 12:58:09