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Laing early onset distal myopathy: slow mysosin defect with variable abnormalities on muscle biopsy

Laing early onset distal myopathy: slow mysosin defect with variable abnormalities on muscle biopsy
Laing early onset distal myopathy: slow mysosin defect with variable abnormalities on muscle biopsy
Background: Laing early onset distal myopathy (MPD1) is an autosomal dominant myopathy caused by mutations within the slow skeletal muscle fibre myosin heavy chain gene, MYH7. It is allelic with myosin storage myopathy, with the commonest form of familial hypertrophic cardiomyopathy, and with one form of dilated cardiomyopathy. However, the clinical picture of MPD1 is distinct from these three conditions.
Objective: To collate and discuss the histological features reported in the muscle biopsies of MPD1 patients and to outline the clinical features.
Results: The phenotype of MPD1 was consistent, with initial weakness of great toe/ankle dorsiflexion, and later development of weakness of finger extension and neck flexion. Age of onset was the only variable, being from birth up to the 20s, but progression was always very slow. The pathological features were variable. In this retrospective series, there were no pathognomonic diagnostic features, although atrophic type I fibres were found in half the families. Rimmed vacuoles are consistently seen in all other distal myopathies with the exception of Myoshi distal myopathy. However, they were found in a minority of patients with MPD1, and were not prominent when present. Immunohistochemical staining for slow and fast myosin showed co-expression of slow and fast myosin in some type I fibres, possibly indicating a switch to type II status. This may be a useful aid to diagnosis.
Conclusions: The pathological findings in MPD1 are variable and appear to be affected by factors such as the specific muscle biopsied, the age of the patient at biopsy, and the duration of disease manifestations.
Abbreviations: IHC, immunohistochemical; MPD1, Laing early onset distal myopathy
slow myosin, distal myopathy, MPD1, MYH7, Laing
0022-3050
208-215
Lamont, P.J.
244b562c-72db-479c-9711-ebd508cf30a7
Udd, B.
cf9d754b-c926-4fe2-b83a-07340323c40d
Mastaglia, F.L.
9c9ae8da-90d0-4a87-8c83-21cb24d80659
DeVisser, M.
380c80da-4f07-494f-b533-d0d386beaeaa
Hedera, P.
0e5bca7c-0897-400e-b5ba-c3526bb772b6
Voit, T.
715f7d26-6d3e-4ed6-a78e-680fd220ab10
Bridges, L.R.
4858d61d-57ff-4265-9164-745dc342ca4c
Fabian, V.
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Rozemuller, A.
6b3d6eac-6a97-4c77-bb0d-1f3ebf420a5f
Laing, N.G.
d77081eb-41f3-4a76-8f5c-ac409dda92ff
Lamont, P.J.
244b562c-72db-479c-9711-ebd508cf30a7
Udd, B.
cf9d754b-c926-4fe2-b83a-07340323c40d
Mastaglia, F.L.
9c9ae8da-90d0-4a87-8c83-21cb24d80659
DeVisser, M.
380c80da-4f07-494f-b533-d0d386beaeaa
Hedera, P.
0e5bca7c-0897-400e-b5ba-c3526bb772b6
Voit, T.
715f7d26-6d3e-4ed6-a78e-680fd220ab10
Bridges, L.R.
4858d61d-57ff-4265-9164-745dc342ca4c
Fabian, V.
284b8d21-9a52-493f-96f2-9eeaf0a61058
Rozemuller, A.
6b3d6eac-6a97-4c77-bb0d-1f3ebf420a5f
Laing, N.G.
d77081eb-41f3-4a76-8f5c-ac409dda92ff

Lamont, P.J., Udd, B., Mastaglia, F.L., DeVisser, M., Hedera, P., Voit, T., Bridges, L.R., Fabian, V., Rozemuller, A. and Laing, N.G. (2006) Laing early onset distal myopathy: slow mysosin defect with variable abnormalities on muscle biopsy. Journal of Neurology Neurosurgery and Psychiatry, 77 (2), 208-215. (doi:10.1136/jnnp.2005.073825).

Record type: Article

Abstract

Background: Laing early onset distal myopathy (MPD1) is an autosomal dominant myopathy caused by mutations within the slow skeletal muscle fibre myosin heavy chain gene, MYH7. It is allelic with myosin storage myopathy, with the commonest form of familial hypertrophic cardiomyopathy, and with one form of dilated cardiomyopathy. However, the clinical picture of MPD1 is distinct from these three conditions.
Objective: To collate and discuss the histological features reported in the muscle biopsies of MPD1 patients and to outline the clinical features.
Results: The phenotype of MPD1 was consistent, with initial weakness of great toe/ankle dorsiflexion, and later development of weakness of finger extension and neck flexion. Age of onset was the only variable, being from birth up to the 20s, but progression was always very slow. The pathological features were variable. In this retrospective series, there were no pathognomonic diagnostic features, although atrophic type I fibres were found in half the families. Rimmed vacuoles are consistently seen in all other distal myopathies with the exception of Myoshi distal myopathy. However, they were found in a minority of patients with MPD1, and were not prominent when present. Immunohistochemical staining for slow and fast myosin showed co-expression of slow and fast myosin in some type I fibres, possibly indicating a switch to type II status. This may be a useful aid to diagnosis.
Conclusions: The pathological findings in MPD1 are variable and appear to be affected by factors such as the specific muscle biopsied, the age of the patient at biopsy, and the duration of disease manifestations.
Abbreviations: IHC, immunohistochemical; MPD1, Laing early onset distal myopathy

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Published date: 2006
Keywords: slow myosin, distal myopathy, MPD1, MYH7, Laing

Identifiers

Local EPrints ID: 27631
URI: http://eprints.soton.ac.uk/id/eprint/27631
DOI: doi:10.1136/jnnp.2005.073825
ISSN: 0022-3050
PURE UUID: b00ab50d-4acb-47eb-a491-850655507294

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Date deposited: 25 Apr 2006
Last modified: 15 Mar 2024 07:20

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Contributors

Author: P.J. Lamont
Author: B. Udd
Author: F.L. Mastaglia
Author: M. DeVisser
Author: P. Hedera
Author: T. Voit
Author: L.R. Bridges
Author: V. Fabian
Author: A. Rozemuller
Author: N.G. Laing

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