Oculopharyngeal muscular dystrophy. Phenotypic and genotypic studies in a UK population
Oculopharyngeal muscular dystrophy. Phenotypic and genotypic studies in a UK population
Oculopharyngeal muscular dystrophy (OPMD) is an autosomal dominant disorder of late onset that commonly presents with ptosis and dysphagia. The genetic basis of the condition has been identified recently as a stable trinucleotide repeat expansion in exon 1 of the poly(A) binding protein 2 gene (PABP2), in which (GCG)6 is the normal repeat length. The prevalence of OPMD is greatest in patients of French-Canadian origin. It is not clear if expansion repeat length is a reliable test in other populations. In this study, we analysed the phenotypic and genotypic characteristics of 31 patients with OPMD in the UK. Ptosis was the first reported symptom in two-thirds of the patients, and half of the subjects studied had evidence of ophthalmoplegia. All but one family had a pathological expansion in the PABP2 gene, ranging from (GCG)8 to (GCG)13. In contrast to the French-Canadian population, (GCG)10 was almost as common as (GCG)9, evidence against a strong founder effect in the UK population. There was a weak association between repeat length and age of disease onset. Patients with longer repeat lengths, such as (GCG)13, developed severe limb weakness early in the disease. We were unable to detect the (GCG)7 polymorphism in over 200 normal controls, suggesting that the frequency of this expansion is lower than that found in the French-Canadian population. One family was negative for the expansion. Affected members presented with the classical features of OPMD, namely ptosis, dysphagia and cytoplasmic inclusions on muscle biopsy, although with some atypical features, such as early age of onset, high serum levels of creatine kinase and a profound ophthalmoplegia. This family is an example of a GCG expansion-negative oculopharyngeal syndrome requiring further genetic investigation. We conclude that PABP2 analysis is a reliable non-invasive diagnostic test for OPMD in the UK population.
oculopharyngeal muscular dystrophy, trinucleotide repeat, uk population
522-526
Hill, M.E.
7821ba06-51cb-4960-a4ab-a6f5c0f61bd9
Creed, G.A.
6f33f60b-186e-46cf-9bae-7d1e9130f44e
McMullan, T.F.
d854e6a3-0cd9-46dd-aac0-be1da2c8662b
Tyers, A.G.
6cb4bd6f-853d-4d96-b53e-9025127729bc
Hilton-Jones, D.
a56bcdea-c3c8-482b-8a75-38872315f50b
Robinson, D.O.
6b7e8cdc-b9c4-4ecf-a344-1bf0ae990f8a
Hammans, S.R.
6553eac5-9322-4f2b-b677-d4ba698fc10b
March 2001
Hill, M.E.
7821ba06-51cb-4960-a4ab-a6f5c0f61bd9
Creed, G.A.
6f33f60b-186e-46cf-9bae-7d1e9130f44e
McMullan, T.F.
d854e6a3-0cd9-46dd-aac0-be1da2c8662b
Tyers, A.G.
6cb4bd6f-853d-4d96-b53e-9025127729bc
Hilton-Jones, D.
a56bcdea-c3c8-482b-8a75-38872315f50b
Robinson, D.O.
6b7e8cdc-b9c4-4ecf-a344-1bf0ae990f8a
Hammans, S.R.
6553eac5-9322-4f2b-b677-d4ba698fc10b
Hill, M.E., Creed, G.A., McMullan, T.F., Tyers, A.G., Hilton-Jones, D., Robinson, D.O. and Hammans, S.R.
(2001)
Oculopharyngeal muscular dystrophy. Phenotypic and genotypic studies in a UK population.
Brain, 124 (3), .
(doi:10.1093/brain/124.3.522).
Abstract
Oculopharyngeal muscular dystrophy (OPMD) is an autosomal dominant disorder of late onset that commonly presents with ptosis and dysphagia. The genetic basis of the condition has been identified recently as a stable trinucleotide repeat expansion in exon 1 of the poly(A) binding protein 2 gene (PABP2), in which (GCG)6 is the normal repeat length. The prevalence of OPMD is greatest in patients of French-Canadian origin. It is not clear if expansion repeat length is a reliable test in other populations. In this study, we analysed the phenotypic and genotypic characteristics of 31 patients with OPMD in the UK. Ptosis was the first reported symptom in two-thirds of the patients, and half of the subjects studied had evidence of ophthalmoplegia. All but one family had a pathological expansion in the PABP2 gene, ranging from (GCG)8 to (GCG)13. In contrast to the French-Canadian population, (GCG)10 was almost as common as (GCG)9, evidence against a strong founder effect in the UK population. There was a weak association between repeat length and age of disease onset. Patients with longer repeat lengths, such as (GCG)13, developed severe limb weakness early in the disease. We were unable to detect the (GCG)7 polymorphism in over 200 normal controls, suggesting that the frequency of this expansion is lower than that found in the French-Canadian population. One family was negative for the expansion. Affected members presented with the classical features of OPMD, namely ptosis, dysphagia and cytoplasmic inclusions on muscle biopsy, although with some atypical features, such as early age of onset, high serum levels of creatine kinase and a profound ophthalmoplegia. This family is an example of a GCG expansion-negative oculopharyngeal syndrome requiring further genetic investigation. We conclude that PABP2 analysis is a reliable non-invasive diagnostic test for OPMD in the UK population.
This record has no associated files available for download.
More information
Published date: March 2001
Keywords:
oculopharyngeal muscular dystrophy, trinucleotide repeat, uk population
Identifiers
Local EPrints ID: 24747
URI: http://eprints.soton.ac.uk/id/eprint/24747
ISSN: 0006-8950
PURE UUID: 03b6fad7-22d7-47f4-a4d5-c1807a3eb389
Catalogue record
Date deposited: 04 Apr 2006
Last modified: 15 Mar 2024 06:58
Export record
Altmetrics
Contributors
Author:
M.E. Hill
Author:
G.A. Creed
Author:
T.F. McMullan
Author:
A.G. Tyers
Author:
D. Hilton-Jones
Author:
D.O. Robinson
Author:
S.R. Hammans
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics