Inclusion body myositis
| Inclusion body myositis | |
|---|---|
| Synonyms | IBM |
| Pronounce | N/A |
| Specialty | N/A |
| Symptoms | Progressive muscle weakness, difficulty swallowing |
| Complications | N/A |
| Onset | Typically after age 50 |
| Duration | Chronic |
| Types | N/A |
| Causes | Unknown, possibly autoimmune |
| Risks | Age, male gender, genetic factors |
| Diagnosis | Muscle biopsy, Electromyography, Blood test |
| Differential diagnosis | Polymyositis, Dermatomyositis, Amyotrophic lateral sclerosis |
| Prevention | N/A |
| Treatment | Physical therapy, Occupational therapy, supportive care |
| Medication | N/A |
| Prognosis | Progressive, no cure |
| Frequency | Rare |
| Deaths | N/A |
A progressive muscle disorder
| Inclusion body myositis | |
|---|---|
| [[File:|250px|alt=|]] | |
| Synonyms | sIBM |
| Pronounce | |
| Field | Rheumatology, Neurology, Neuromuscular medicine |
| Symptoms | Progressive muscle weakness, muscle wasting |
| Complications | Mobility issues, difficulty swallowing (dysphagia) |
| Onset | Typically after age 45 |
| Duration | Chronic, lifelong |
| Types | Sporadic inclusion body myositis (sIBM), Hereditary IBM |
| Causes | Unknown, possibly autoimmune and degenerative |
| Risks | Advanced age, genetic predisposition |
| Diagnosis | Muscle biopsy, clinical assessment, electromyography (EMG) |
| Differential diagnosis | Deconditioning, hereditary muscle diseases, polymyositis, dermatomyositis |
| Prevention | None known |
| Treatment | Supportive therapies (physical therapy, occupational therapy), symptomatic management |
| Medication | Immunotherapy generally ineffective; symptomatic medications as needed |
| Prognosis | Slowly progressive disability, typically non-fatal |
| Frequency | 5-71 per 1,000,000 |
| Deaths | Rarely directly fatal; associated complications can increase risk |
Inclusion body myositis (IBM), specifically sporadic inclusion body myositis (sIBM), is a chronic, slowly progressive inflammatory muscle disease characterized primarily by progressive muscle weakness and wasting. It predominantly affects older adults, typically beginning after the age of 45.
Signs and Symptoms[edit]
Symptoms generally develop slowly and include:
- Progressive weakness in the forearms, wrists, thighs, and muscles controlling finger flexion
- Difficulty swallowing (dysphagia)
- Gradual muscle atrophy, especially in the quadriceps and forearm muscles
Causes[edit]
The exact cause of IBM remains unknown. The condition is thought to involve both autoimmune and degenerative processes, possibly influenced by genetic factors.
Risk Factors[edit]
Factors increasing the likelihood of developing IBM include:
- Advanced age, typically over 45
- Genetic susceptibility
Diagnosis[edit]
Diagnosis typically involves:
- Clinical evaluation and detailed patient history
- Electromyography (EMG) to assess muscle activity
- Muscle biopsy revealing characteristic inclusions and inflammation
Differential diagnosis should consider:
Treatment[edit]
There is currently no curative treatment for IBM. Management primarily includes:
- Physical therapy and occupational therapy to maintain mobility and functionality
- Supportive interventions such as speech therapy for dysphagia
Immunotherapy typically has limited or no benefit in IBM patients.
Prognosis[edit]
IBM progresses slowly, causing increasing disability but rarely affecting life expectancy directly. However, complications such as severe swallowing difficulties can contribute to health risks.
Epidemiology[edit]
IBM is a relatively rare condition, with prevalence estimates ranging from 5 to 71 cases per million people worldwide, making it one of the most common inflammatory muscle diseases in adults over 50.
Prevention[edit]
No known preventive measures exist for inclusion body myositis.
Related pages[edit]
| Systemic connective tissue disorders | ||||||
|---|---|---|---|---|---|---|
|
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