Centronuclear myopathy: Difference between revisions
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{{Infobox medical condition (new) | |||
| name = Centronuclear myopathy | |||
| image = Centronuclear myotubular myopathy.JPEG | |||
| caption = Muscle biopsy from the quadriceps taken at 3 months of age from a girl with X-linked centronuclear ("myotubular") myopathy due to a mutation in the myotubularin (MTM1) gene and extremely skewed X-inactivation ([[H&E stain]], transverse section). Note marked variability in fibre size, moderate increase in connective tissue, and numerous central nuclei. | |||
| pronounce = | |||
| field = [[Neurology]], [[Genetics]], [[Musculoskeletal]] | |||
| synonyms = CNM | |||
| symptoms = Muscle weakness, hypotonia, delayed motor milestones, respiratory difficulties, and in severe cases, cardiac complications | |||
| complications = Respiratory failure, scoliosis, joint contractures, cardiac arrhythmias, and difficulty with swallowing | |||
| onset = Typically presents in infancy or early childhood, though some forms can appear later | |||
| duration = Lifelong, with severity varying greatly depending on the subtype | |||
| types = X-linked (most common), autosomal dominant, autosomal recessive | |||
| causes = Genetic mutations, most commonly in the [[MTM1]] gene (X-linked form) or in genes such as [[DNM2]], [[AMP1]], [[RYR1]] for autosomal forms | |||
| risks = Family history of centronuclear myopathy, genetic predisposition, male sex (in X-linked form) | |||
| diagnosis = Clinical presentation, genetic testing (for MTM1, DNM2, AMP1, RYR1 mutations), muscle biopsy showing central nuclei in muscle fibers | |||
| differential = [[Duchenne muscular dystrophy]], [[Myotonic dystrophy]], [[Becker muscular dystrophy]], [[Congenital muscular dystrophy]], other forms of [[muscular dystrophy]] | |||
| prevention = No primary prevention; genetic counseling may be beneficial for families with a history of the disease | |||
| treatment = Symptomatic management, physical therapy to maintain muscle strength and function, respiratory support, and orthopedic interventions for scoliosis or joint contractures | |||
| medication = No specific drug therapy; medications for managing symptoms such as respiratory support and anticonvulsants if needed for seizures | |||
| prognosis = Variable; in severe cases (particularly X-linked form), life expectancy may be reduced due to respiratory failure, while milder forms may allow for normal or near-normal life expectancy | |||
| frequency = Rare, with an estimated prevalence of 1 in 50,000 to 1 in 100,000 individuals | |||
| deaths = Higher mortality rate in severe cases due to respiratory failure or cardiac complications | |||
}} | |||
{{Short description|A group of rare congenital myopathies}} | {{Short description|A group of rare congenital myopathies}} | ||
'''Centronuclear myopathy''' (CNM) is a group of rare [[congenital myopathies]] characterized by muscle weakness and distinctive histological features, notably the presence of centrally located nuclei in muscle fibers. These myopathies are genetically heterogeneous and can be inherited in an [[autosomal dominant]], [[autosomal recessive]], or [[X-linked]] manner. | '''Centronuclear myopathy''' (CNM) is a group of rare [[congenital myopathies]] characterized by muscle weakness and distinctive histological features, notably the presence of centrally located nuclei in muscle fibers. These myopathies are genetically heterogeneous and can be inherited in an [[autosomal dominant]], [[autosomal recessive]], or [[X-linked]] manner. | ||
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* [[Genetic testing]] | * [[Genetic testing]] | ||
* [[Respiratory support]] | * [[Respiratory support]] | ||
{{stub}} | |||
[[Category:Congenital myopathies]] | [[Category:Congenital myopathies]] | ||
[[Category:Genetic disorders]] | [[Category:Genetic disorders]] | ||
[[Category:Neuromuscular disorders]] | [[Category:Neuromuscular disorders]] | ||
{{Diseases of myoneural junction and muscle}} | |||
{{X-linked disorders}} | |||
{{stub}} | |||
{{DEFAULTSORT:Centronuclear Myopathy}} | |||
[[Category:Myoneural junction and neuromuscular diseases]] | |||
Revision as of 21:15, 22 March 2025
| Centronuclear myopathy | |
|---|---|
| |
| Synonyms | CNM |
| Pronounce | |
| Field | Neurology, Genetics, Musculoskeletal |
| Symptoms | Muscle weakness, hypotonia, delayed motor milestones, respiratory difficulties, and in severe cases, cardiac complications |
| Complications | Respiratory failure, scoliosis, joint contractures, cardiac arrhythmias, and difficulty with swallowing |
| Onset | Typically presents in infancy or early childhood, though some forms can appear later |
| Duration | Lifelong, with severity varying greatly depending on the subtype |
| Types | X-linked (most common), autosomal dominant, autosomal recessive |
| Causes | Genetic mutations, most commonly in the MTM1 gene (X-linked form) or in genes such as DNM2, AMP1, RYR1 for autosomal forms |
| Risks | Family history of centronuclear myopathy, genetic predisposition, male sex (in X-linked form) |
| Diagnosis | Clinical presentation, genetic testing (for MTM1, DNM2, AMP1, RYR1 mutations), muscle biopsy showing central nuclei in muscle fibers |
| Differential diagnosis | Duchenne muscular dystrophy, Myotonic dystrophy, Becker muscular dystrophy, Congenital muscular dystrophy, other forms of muscular dystrophy |
| Prevention | No primary prevention; genetic counseling may be beneficial for families with a history of the disease |
| Treatment | Symptomatic management, physical therapy to maintain muscle strength and function, respiratory support, and orthopedic interventions for scoliosis or joint contractures |
| Medication | No specific drug therapy; medications for managing symptoms such as respiratory support and anticonvulsants if needed for seizures |
| Prognosis | Variable; in severe cases (particularly X-linked form), life expectancy may be reduced due to respiratory failure, while milder forms may allow for normal or near-normal life expectancy |
| Frequency | Rare, with an estimated prevalence of 1 in 50,000 to 1 in 100,000 individuals |
| Deaths | Higher mortality rate in severe cases due to respiratory failure or cardiac complications |
A group of rare congenital myopathies
Centronuclear myopathy (CNM) is a group of rare congenital myopathies characterized by muscle weakness and distinctive histological features, notably the presence of centrally located nuclei in muscle fibers. These myopathies are genetically heterogeneous and can be inherited in an autosomal dominant, autosomal recessive, or X-linked manner.
Classification
Centronuclear myopathy is classified based on the mode of inheritance and the specific genetic mutations involved. The main types include:
- X-linked centronuclear myopathy: Caused by mutations in the MTM1 gene, this form is also known as myotubular myopathy. It primarily affects males and is the most severe form, often presenting in infancy.
- Autosomal dominant centronuclear myopathy: Often associated with mutations in the DNM2 gene, this form can present at any age and varies in severity.
- Autosomal recessive centronuclear myopathy: This form can be caused by mutations in several genes, including BIN1, RYR1, and TTN. It typically presents in childhood or adolescence.
Pathophysiology
The hallmark of centronuclear myopathy is the abnormal positioning of nuclei in the center of muscle fibers, rather than at the periphery. This is thought to result from defects in muscle cell development and maintenance. The specific pathophysiological mechanisms vary depending on the genetic mutation involved. For example, mutations in the MTM1 gene affect the protein myotubularin, which is involved in phosphoinositide metabolism, while DNM2 mutations affect dynamin 2, a protein involved in endocytosis and membrane trafficking.
Clinical Features
The clinical presentation of centronuclear myopathy can vary widely depending on the type and severity of the condition. Common features include:
- Muscle weakness, particularly in the proximal muscles
- Hypotonia (reduced muscle tone)
- Delayed motor milestones
- Respiratory difficulties, especially in severe cases
- Facial muscle weakness, leading to a characteristic facial appearance
Diagnosis
Diagnosis of centronuclear myopathy typically involves a combination of clinical evaluation, muscle biopsy, and genetic testing. Muscle biopsy reveals the characteristic central nuclei in muscle fibers. Genetic testing can identify specific mutations responsible for the condition.
Management
There is currently no cure for centronuclear myopathy, and management focuses on supportive care to improve quality of life. This may include:
- Physical therapy to maintain muscle strength and flexibility
- Respiratory support, such as non-invasive ventilation
- Orthopedic interventions to address skeletal deformities
- Nutritional support to ensure adequate caloric intake
Prognosis
The prognosis for individuals with centronuclear myopathy varies widely depending on the type and severity of the condition. X-linked myotubular myopathy often has a poor prognosis due to severe respiratory involvement, while other forms may have a more favorable outcome with appropriate management.
Related pages
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| Diseases of muscle, neuromuscular junction, and neuromuscular disease | ||||||||||||||
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| X-linked disorders |
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