Neurology JC032: Generalised Muscle Weakness: Myasthenia Gravis, Myopathy And Myositis, Neuropathy, Neurophysiology 2 Flashcards
Definition of terms in Positive sensory symptoms
- Allodynia (無痛覺得痛)
- pain due to a stimulus that does not normally provoke pain - Hyperalgesia
- ↑ response to stimulus that is normally painful - Hypoalgesia
- ↓ pain in response to a normally painful stimulus - Analgesia
- absence of pain in response to stimulation that would normally be painful - Hyperaesthesia
- ↑ sensitivity to stimulation, excluding the special senses - Hypoaesthesia
- ↓ sensitivity to stimulation, excluding the special senses - Hyperpathia (越黎越痛)
- a painful syndrome characterised by an abnormally painful reaction to a stimulus, especially a repetitive stimulus, as well as an ↑ threshold
Generalised weakness
Weakness: Dysfunction of anywhere along motor system
Causes:
1. Nerves —> Polyneuropathies, Motor neuron disease
2. Muscles —> Myopathies
3. NMJ —> Neuromuscular junction disorders
- Polyneuropathies / Generalised peripheral neuropathies
Clinical features:
1. Motor problems
- Weakness
- Wasting (if chronic)
- Fasciculations
- Hyporeflexia
—> S/S of LMN lesions
- Severe: **Bulbar, **Respiratory weakness
- Sensory problems
- Negative (cannot perceive what they should be perceiving)
- Positive (perceive something that they should not be perceiving)
- **Length-dependent process: Longest nerve will be symptomatic first —> Stocking —> **Glove pattern of sensory disturbance - Autonomic problems
- CVS: **tachycardia, exercise intolerance, cardiac denervation, painless MI, **postural hypotension, heat intolerance, alterations in skin blood flow
- GI: **esophageal dysfunction, gastroparesis diabeticorum, diarrhoea / constipation, **faecal incontinence
- Genitourinary: **erectile dysfunction, retrograde ejaculation, cystopathy, **neurogenic bladder
DDx (SpC Medicine):
- Cervical myelopathy (e.g. cervical spondylosis)
- Different etiologies of Polyneuropathies (DM, Vit deficiency, Drug-induced, Inflammatory)
Classification of Polyneuropathies / Generalised peripheral neuropathies
- Time course
- acute / subacute / chronic / relapsing - Distribution + Pattern of deficits
- generalised / focal - Types of functional fibres involved
- motor / sensory / autonomic / mixed
- some can affect one modality more, most are mixed - **Axonal (↓ amplitude) / **Demyelinating (↓ conduction velocity) / Mixed
Etiologies of Polyneuropathies / Generalised peripheral neuropathies
Very diverse (>100)
1. Systemic disease
- **DM (commonest in developed countries)
- **CTD (self notes)
- Infectious and Granulomatous neuropathy
- ***Leprosy (commonest) - Inflammatory demyelinating neuropathy
- **Guillain-Barré syndrome (medical emergency)
- **Chronic Inflammatory Demyelinating Polyneuropathy (CIDP) (self notes) - Ischaemic neuropathy
- Metabolic neuropathy
- ***Vit deficiency (commonest) - ***Hereditary neuropathy (appear in OSCE)
- Charcot-Marie-Tooth disease (HMSN, SMA) - ***Toxins (chemotherapy, environmental toxins)
Investigations of Polyneuropathies / Generalised peripheral neuropathies
- Look for systemic disease
- ***Electrophysiological studies
-
**CSF
- CSF protein: good for suspected **inflammatory causes - ***Nerve biopsy (seldom indicated)
- Genetic tests
Inflammatory demyelinating neuropathy: Guillain-Barré syndrome
- ***Acute / Subcute
- ***Generalised
- Mixed (some pure motor / sensory)
- Demyelinating / Axonal forms
- **Rapidly progressive Flaccid paralysis, Areflexia, **Raised CSF protein ***without ↑ in cells
- Not uncommon: 10-20 cases per year, incidence 1-2 per 100,000 per year
Dysimmune disorder
- **Immune-mediated, Inflammatory PN
- Preceded by mild **viral / bacterial infection (URTI, GE) (2/3 of cases)
—> trigger immune response **misdirected against **peripheral nervous system
—> Subacute / Acute neuritis onset over a few **days
—> peaks / plateau about 2-*4 weeks
- Inflammatory demyelination
—> impaired nerve function - Aka: AIDP (Acute Inflammatory Demyelinating Polyneuropathy)
- Other variants:
—> AMAN (Acute motor axonal neuropathy), AMSAN (Acute motor and sensory axonal neuropathy) (axonal forms affecting motor fibres + sensory fibres)
—> Ataxic form (affect mainly sensory fibres)
—> MFS (Miller Fisher syndrome), Polyneuritis cranialis (affect mainly cranial nerves)
Clinical features:
1. Ascending weakness with facial involvement (CN neuropathy (SpC Medicine))
- respiratory failure 30%
2. **Sensory symptoms
3. Hypo / Areflexia
4. **Muscle ache
5. ***Autonomic dysfunction (>2/3 patients) (e.g. BP variations, cardiac arrhythmias) (worse prognosis if present (SpC Medicine))
(6. Usually affect lower limb first before upper limb (SpC Medicine))
Investigations:
1. **↑ CSF protein **without pleocytosis
2. **Electrophysiology
3. **Anti-gangliocyte Ab (some cases)
Treatment:
1. General supportive measures
- **Monitor FVC, ABG, BP, ECG, bulbar function
- **Mechanical ventilation for respiratory failure
- General care for immobility, **nutritional support
- Treat complications
—> prevention, monitoring, detection, treatment of complication e.g. **respiratory failure, ***aspiration pneumonia, sepsis, cardiac, haemodynamic events during acute course of illness
- Specific immunotherapy
- **Plasmapheresis (SpC Medicine: Gold standard)
- **High dose IVIG (SpC Medicine: Convenient, additional benefit of preventing infection since bedbound)
Prognosis:
- Mortality: 2 (with appropriate treatment) - 12%
- 20% permanent disability
- 10% severe
Hereditary neuropathies: Charcot-Marie-Tooth disease
- ***Chronic
- Mixed / Motor
- Demyelinating / Axonal forms
- Hereditary condition(s)
- **Early onset, **Slowly progressive neuropathy
- ***Distal wasting
- Deformities: **Foot drop, **Pes cavus (high foot arch) (indicate childhood disease / onset during development —> also seen in poliomyelitis, cerebral palsy etc. (vs late onset disease e.g. diabetic neuropathy))
Charcot-Marie-Tooth disease is NOT just one disease —> many hereditary neuropathies
1. ***Hereditary motor-sensory neuropathies (HMSN)
- Demyelinating / Hypomyelination form
- Axonal degenerative form
- Autosomal dominant / recessive, X-linked
- Different identifiable mutations: PMP22, MPZ, MFN2, GJB1 etc.
- HMSN-1 (demyelinating PN): AD, AR, X-linked
- HMSN-2 (axonal PN): AD, AR, X-linked
- HMSN-3 (DSD)
- HMSN-4 (Refsum disease)
- HMSN-5 (axonal PN with pyramidal signs)
- HMSN-6 (with optic atrophy, HMSN-2a)
- HMSN-7 (with retinitis pigmentosa)
-
**Hereditary motor neuropathies
- **Spinomuscular atrophies (SMA)
—> SMA type 1 (60%), type 2 (30%), type 3 (20%), type 4
- Different identifiable mutations: UBA1, DYNC1H1, VAPB etc.
Motor neuron disease / Amyotrophic lateral sclerosis (ALS)
- Chronic
- Generalised
- Motor
- Axonal
- ***Idiopathic motor neuropathy
-
**Progressive degeneration of **α motor neurons:
1. **Anterior horn cells (LMN deficits)
2. **Corticospinal tract (UMN deficits)
Types:
1. ***ALS
2. PLS (Primary lateral sclerosis)
3. PMA (Progressive muscular atrophy)
4. PBP (Progressive bulbar palsy)
5. Pseudobulbar palsy
- ***NO sensory involvement
- Onset: middle to old age (peak ***6th decade)
- Incidence: 1 per 100,000 per year
- M:F = 3:2
- ***~10% Familial (SOD1, C9orf72, TARDBP, FUS)
Treatment:
1. ***No specific treatment
- die within 3 years (aspiration, respiratory failure, death)
- General supportive care
- **nutritional support
- **Riluzole, Endaravone?
- euthanasia vs long-term ventilation
- Myopathies
Clinical features:
1. **Proximal weakness
2. **Waddling gait (unable to stabilise pelvis when walking —> pelvic tilting)
3. **Bulbar, Respiratory weakness
4. **Muscle tenderness (inflammatory myopathies)
5. Sensory disturbance, Sphincter dysfunction (Pure myopathies does not involve sensory disturbance)
DDx of Proximal muscle weakness:
1. **Metabolic (e.g. DM)
2. **Electrolyte imbalance (e.g. HypoK)
3. **Drug induced (e.g. Steroid —> Cushing, Statin)
4. **Paraneoplastic
5. ***Neuropathy
***Etiologies of Myopathies
Inherited
1. ***Muscular dystrophies
- Dystrophinopathies (Duchenne, Becker)
- Facioscapulohumeral dystrophy (FSHD)
- Limb-girdle dystrophies (LGMD)
- Metabolic
- Mitochondropathies
- Glycogenoses
- Lipid myopathies - Congenital myopathies
- Channelopathies
- Myotonic disorders
- Periodic paralysis
- Malignant hyperthermia
Acquired (mostly treatable)
1. ***Inflammatory
- Polymyositis
- Dermatomyositis
- Inclusion body myositis
- Infection-related
- Complicating systemic diseases
- **Connective tissue diseases
- **Endocrinopathies (e.g. Hypo/Hyperthyroidism)
- Sarcoidosis
- Critical illness myopathy - Toxic myopathies
- ***Rhabdomyolysis
- Drug-induced (e.g. Statin myopathy)
Investigations of Myopathies
To identify reversible causes
1. Look for systemic diseases
2. **Electrophysiological studies
3. **Muscle enzymes (e.g. creatine kinase)
4. ***Muscle biopsy (not cause irreversible loss of function vs nerve biopsy)
5. Genetic tests
***Muscular dystrophies
***Hereditary myopathies
Old definition:
- Inherited disease
- All symptoms due to **muscle weakness
- **Progressive
- No histopathological abnormalities other than degeneration and regeneration
***Clinical classification:
X-linked recessive:
1. Duchenne (DMD)
2. Becker (BMD)
AD / AR:
3. Facioscapulohumeral (FSHD)
4. Limb-girdle (LGMD)
5. Myotonic dystrophy (MyoD)
X-linked muscular dystrophies
ONLY in boys, girls are asymptomatic carrier
- ***Gowers’ sign: proximal weakness
- Duchenne
- Mild delay in motor milestones
- **Progressive weakness (from 3-5) —> wheelchair-bound (9-12) —> respiratory failure + death (by late teens)
- **Cardiomyopathy
- Mild mental impairment
- ***No / Few dystrophin-positive fibres - Becker
- Mild form of Duchenne, more prolonged survival
- **Partial dystrophin deficiency
- Continue to ambulate beyond 15 —> death between **40-60
Facioscapulohumeral muscular dystrophy (FSHD)
Dystrophy in Facial, Scapular, Humeral muscles:
1. Facial
- SCM
- ***facial weakness
- ptosis
- Scapular
- neck muscles
- ***scapula winging
- spinati, pectoralis, trapezii - Humeral
- brachio-radialis
- ***biceps
- deltoid (compensatory hypertrophy)
May be additional involvement of Femoral / Peroneal muscles
