Multiple sclerosis: Difference between revisions
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==Background== | ==Background== | ||
*CNS myelin destruction causes variable motor, sensory, visual and cerebellar dysfunction<ref>Multiple sclerosis: a practical overview for clinicians. British Medical Bulletin, Volume 95, Issue 1, September 2010, Pages 79–104. https://doi.org/10.1093/bmb/ldq017</ref> | |||
*Peak onset age 20-40 years, F:M ratio ~3:1 | |||
*More common in populations of Northern European descent and at higher latitudes | |||
===Types=== | |||
*Clinically isolated syndrome (CIS) | |||
**Single first episode of neurologic symptoms lasting ≥24 hours, caused by CNS demyelination | |||
**May or may not progress to MS | |||
*Radiologically isolated syndrome (RIS) | |||
**Incidental MRI findings suggestive of MS in asymptomatic patients | |||
*Relapsing/remitting (most common) | |||
**Relapse (days-months) followed by remission | |||
*Secondary progressive | |||
**Relapses and partial recoveries occur, but disability does not fade away between cycles | |||
*Primary progressive | |||
**Symptoms progress slowly and steadily without remission | |||
*Progressive relapsing | |||
**Similar to primary progressive but with superimposed flares | |||
==Clinical Features== | |||
*Classic patient has multiple presentations for neuro symptoms of different areas of pathology | |||
**Patient often has resolution of the earlier symptoms | |||
*Symptoms worsen with increases in body temperature, classically after hot showers (Uhthoff's phenomenon<ref>Flensner G, et al. "Sensitivity to heat in MS patients: a factor strongly influencing symptomology-an explorative survey". BMC Neurol. 2011. 11:27.</ref>) | |||
*Muscle/sensory signs: | |||
**Lower extremity [[weakness]] usually worse than upper extremity | |||
**Upper motor neuron signs: | |||
***Hyperreflexia | |||
***Positive Babinski | |||
**[[numbness|Decrease]] in proprioception/pain/temperature sensation | |||
**Lhermitte sign | |||
***Electric shock sensation radiating down back into arms/legs from neck flexion | |||
***If the discomfort is severe, carbamazepine or gabapentin may be beneficial for some patients. | |||
**Partial [[transverse myelitis]] | |||
***Asymmetric motor/sensory deficits at a spinal cord level | |||
***One of the most common acute presenting syndromes | |||
**[[Trigeminal neuralgia]] | |||
***Bilateral trigeminal neuralgia in a young patient should raise suspicion for MS | |||
*[[Optic neuritis]] | |||
**Initial sign in 30% of patients | |||
**[[Vision loss]] (usually unilateral) often preceded by retrobulbar pain | |||
**[[Blurred vision]] | |||
**Afferent pupillary defect is suggestive of optic neuritis | |||
**[[Nystagmus]] | |||
**[[Diplopia]] | |||
*[[Internuclear ophthalmoplegia]] | |||
**Impaired adduction of the adducting eye with nystagmus of the abducting eye | |||
**Bilateral INO is classic for MS | |||
**Convergence (both eyes center medially) is preserved | |||
*Dysautonomia | |||
**[[Urinary retention]] (increased risk of [[UTI]]/[[pyelo]]) | |||
**[[Constipation]] or incontinence | |||
**Sexual dysfunction (males) | |||
*Other common symptoms | |||
**Fatigue — most common symptom overall; frequent reason for ED presentation | |||
**Cognitive dysfunction (up to 50% of patients) | |||
==Differential Diagnosis== | |||
{{Weakness DDX}} | |||
==Evaluation== | |||
[[File:MS_MRI_1.jpg|thumb|MRI brain with contrast of a patient in her mid-20s with new onset MS. Large lesion in left parietal area.]] | |||
[[File:MS_MRI_2.jpg|thumb|MRI brain with contrast of same patient with new onset MS with another lesion in the left cerebellum.]] | |||
===Known MS Patient with Exacerbation=== | |||
*[[Urinalysis]] — rule out occult [[UTI]] as pseudorelapse trigger (very common in MS) | |||
*CBC, Chemistry | |||
*Consider [[chest X-ray|CXR]] or other infectious workup based on presentation | |||
*Temperature — fever suggests pseudorelapse or infection | |||
*[[brain MRI|MRI]] with GAD generally not needed emergently unless diagnostic uncertainty or concern for [[PML]] | |||
*LP is generally not needed for exacerbation of known MS — defer to neurology | |||
===Suspected New Diagnosis=== | |||
*[[brain MRI|MRI]] with GAD of brain (+/- spine) and orbits (if [[optic neuritis]] suspected) | |||
**Multiple lesions in supratentorial white matter, paraventricular area, spinal cord | |||
*[[LP|CSF]] | |||
**Elevated protein and gamma-globulin (increased oligoclonal bands) | |||
**Generally can be deferred to neurology | |||
*CBC, Chemistry | |||
*[[Urinalysis]] | |||
*TSH, B12, RPR/VDRL — rule out MS mimics | |||
*Consider NMO/aquaporin-4 antibody testing (especially if longitudinally extensive transverse myelitis or bilateral optic neuritis)<ref>Pelletier J, et al. "Multiple Sclerosis: An Emergency Medicine-Focused Narrative Review." J Emerg Med. 2024;66(4):e441-e456.</ref> | |||
==Management== | |||
===Pseudorelapse vs True Relapse=== | |||
{| class="wikitable" | |||
|- | |||
! !! '''True Relapse''' !! '''Pseudorelapse''' | |||
|- | |||
| '''Definition''' || New inflammatory demyelinating event || Temporary worsening of old symptoms from an external trigger | |||
|- | |||
| '''Duration''' || >24 hours, evolves over hours to days, persists days to weeks || Typically <24 hours; resolves when trigger is removed | |||
|- | |||
| '''Triggers''' || None (not explained by fever or infection) || Infection (especially UTI), fever, heat, stress, dehydration, medication changes | |||
|- | |||
| '''Symptoms''' || New neurologic symptoms OR worsening in a new distribution || Recurrence of prior/known deficits; symptoms may fluctuate | |||
|- | |||
| '''MRI''' || Often shows new gadolinium-enhancing lesion || No new lesion | |||
|- | |||
| '''Treatment''' || High-dose corticosteroids || Treat the underlying trigger; steroids are '''not''' indicated | |||
|} | |||
<ref>Mellen Center Approaches: Management of MS Relapses. Cleveland Clinic Mellen Center for Multiple Sclerosis Treatment and Research. https://my.clevelandclinic.org/departments/neurological/depts/multiple-sclerosis/ms-approaches/relapse-management-ms</ref><ref>Defined by Thompson AJ, et al. "Diagnosis of multiple sclerosis: 2017 revisions of the McDonald Criteria." Lancet Neurol. 2018;17(2):162-173.</ref> | |||
*Always check UA and infectious workup before initiating steroids — occult UTI is a very common pseudorelapse trigger in MS patients | |||
*If symptoms are identical to a prior relapse, pseudorelapse is more likely (MS rarely causes repeated inflammation in the same CNS location) | |||
*Symptoms that fluctuate or resolve completely and then return favor pseudorelapse<ref>Amin A, et al. "Triaging Patients with Multiple Sclerosis in the Emergency Department: Room for Improvement." Proc Bayl Univ Med Cent. 2022;36(2):186-189.</ref> | |||
== | ===Fever and Infection=== | ||
*Fever must be reduced to minimize weakness associated with elevated temperature | |||
*Antibiotics or surgical control of any infectious sources | |||
== | ===Steroids=== | ||
*High-dose [[Corticosteroids|steroid]] therapy for true relapses in the form of oral or intravenous methylprednisolone (1000 mg daily x 3-5 days)<ref>Le Page et al. Oral versus intravenous high-dose methylprednisolone for treatment of relapses in patients with multiple sclerosis (COPOUSEP): a randomised, controlled, double-blind, non-inferiority trial. Lancet. 2016 Jan 23;387(10016):340. https://core.ac.uk/download/pdf/52993687.pdf</ref> | |||
**Oral methylprednisolone at equivalent doses is non-inferior to IV and allows for outpatient treatment | |||
*Do not initiate steroids until infection has been ruled out as the cause of symptom worsening | |||
== | ===Plasma Exchange (PLEX)=== | ||
*Second-line treatment for severe relapses refractory to high-dose corticosteroids<ref>Ehler J, et al. "Therapeutic Plasma Exchange in Multiple Sclerosis and Autoimmune Encephalitis." J Clin Med. 2019;8(10):1793.</ref> | |||
*~20-35% of patients may not fully respond to steroids alone | |||
*Typically 5-7 sessions over 10-14 days | |||
*Consult neurology early if relapse is severe or not responding to steroids | |||
== | ===Disease-Modifying Therapies (DMTs)=== | ||
*Suppression therapies (IFN-β, Glatiramer, etc.) — initiation is generally not in ED | |||
*However, ED physicians should be aware of complications of DMTs in patients already on treatment: | |||
= | {| class="wikitable" | ||
|- | |||
! '''DMT''' !! '''ED-Relevant Complications''' | |||
|- | |||
| '''Natalizumab (Tysabri)''' || Risk of '''[[PML]]''' (progressive multifocal leukoencephalopathy) — any new neurologic worsening warrants urgent MRI and JC virus testing | |||
|- | |||
| '''Fingolimod / Siponimod''' || [[Bradycardia]], cardiac conduction abnormalities, macular edema | |||
|- | |||
| '''Ocrelizumab, Rituximab''' (anti-CD20) || Increased infection risk, infusion reactions, reactivation of hepatitis B | |||
|- | |||
| '''Interferons (Avonex, Rebif)''' || Flu-like symptoms (may mimic infection), hepatotoxicity, cytopenias | |||
|- | |||
| '''Dimethyl fumarate (Tecfidera)''' || Lymphopenia (increased infection risk); rare PML risk | |||
|} | |||
<ref>Pelletier J, et al. "Multiple Sclerosis: An Emergency Medicine-Focused Narrative Review." J Emerg Med. 2024;66(4):e441-e456.</ref> | |||
==Disposition== | ==Disposition== | ||
===Discharge=== | |||
*Mild relapse in a patient who can ambulate safely | |||
*Able to tolerate oral medications (oral methylprednisolone non-inferior to IV) | |||
*Has reliable follow-up with neurology (ideally within 1-3 days) | |||
*No untreated infection | |||
*Adequate social support | |||
== | ===Admission=== | ||
[[ | *Any disease exacerbation associated with significant morbidity or functional impairment | ||
*IV antibiotics or steroid therapy required | |||
*Inability to ambulate safely or care for self | |||
*[[Urinary retention]] requiring catheterization | |||
*Concern for [[PML]] or other serious DMT complication | |||
*Depression and significant risk of suicide | |||
*Need for plasma exchange | |||
== | ===Neurology Consultation=== | ||
*New suspected MS diagnosis | |||
*Severe relapse with significant functional impairment | |||
*Steroid-refractory symptoms (discuss PLEX) | |||
*Concern for PML or other DMT-related complication | |||
*Diagnostic uncertainty | |||
[[Category: | ===Return Precautions=== | ||
*Worsening weakness or new weakness | |||
*New or worsening visual symptoms | |||
*Inability to urinate or new incontinence | |||
*Difficulty breathing or swallowing | |||
*[[Fever]] | |||
==See Also== | |||
*[[Optic Neuritis]] | |||
*[[Transverse myelitis]] | |||
*[[Internuclear ophthalmoplegia]] | |||
==References== | |||
<references/> | |||
[[Category:Neurology]] | |||
Latest revision as of 09:26, 22 March 2026
Background
- CNS myelin destruction causes variable motor, sensory, visual and cerebellar dysfunction[1]
- Peak onset age 20-40 years, F:M ratio ~3:1
- More common in populations of Northern European descent and at higher latitudes
Types
- Clinically isolated syndrome (CIS)
- Single first episode of neurologic symptoms lasting ≥24 hours, caused by CNS demyelination
- May or may not progress to MS
- Radiologically isolated syndrome (RIS)
- Incidental MRI findings suggestive of MS in asymptomatic patients
- Relapsing/remitting (most common)
- Relapse (days-months) followed by remission
- Secondary progressive
- Relapses and partial recoveries occur, but disability does not fade away between cycles
- Primary progressive
- Symptoms progress slowly and steadily without remission
- Progressive relapsing
- Similar to primary progressive but with superimposed flares
Clinical Features
- Classic patient has multiple presentations for neuro symptoms of different areas of pathology
- Patient often has resolution of the earlier symptoms
- Symptoms worsen with increases in body temperature, classically after hot showers (Uhthoff's phenomenon[2])
- Muscle/sensory signs:
- Lower extremity weakness usually worse than upper extremity
- Upper motor neuron signs:
- Hyperreflexia
- Positive Babinski
- Decrease in proprioception/pain/temperature sensation
- Lhermitte sign
- Electric shock sensation radiating down back into arms/legs from neck flexion
- If the discomfort is severe, carbamazepine or gabapentin may be beneficial for some patients.
- Partial transverse myelitis
- Asymmetric motor/sensory deficits at a spinal cord level
- One of the most common acute presenting syndromes
- Trigeminal neuralgia
- Bilateral trigeminal neuralgia in a young patient should raise suspicion for MS
- Optic neuritis
- Initial sign in 30% of patients
- Vision loss (usually unilateral) often preceded by retrobulbar pain
- Blurred vision
- Afferent pupillary defect is suggestive of optic neuritis
- Nystagmus
- Diplopia
- Internuclear ophthalmoplegia
- Impaired adduction of the adducting eye with nystagmus of the abducting eye
- Bilateral INO is classic for MS
- Convergence (both eyes center medially) is preserved
- Dysautonomia
- Urinary retention (increased risk of UTI/pyelo)
- Constipation or incontinence
- Sexual dysfunction (males)
- Other common symptoms
- Fatigue — most common symptom overall; frequent reason for ED presentation
- Cognitive dysfunction (up to 50% of patients)
Differential Diagnosis
Weakness
- Neuromuscular weakness
- Upper motor neuron:
- CVA
- Hemorrhagic stroke
- Multiple sclerosis
- Amyotrophic Lateral Sclerosis (ALS) (upper and lower motor neuron)
- Lower motor neuron:
- Spinal and bulbar muscular atrophy (Kennedy's syndrome)
- Spinal cord disease:
- Infection (Epidural abscess)
- Infarction/ischemia
- Trauma (Spinal Cord Syndromes)
- Inflammation (Transverse Myelitis)
- Degenerative (Spinal muscular atrophy)
- Tumor
- Peripheral nerve disease:
- Neuromuscular junction disease:
- Muscle disease:
- Rhabdomyolysis
- Dermatomyositis
- Polymyositis
- Alcoholic myopathy
- Upper motor neuron:
- Non-neuromuscular weakness
- Can't miss diagnoses:
- ACS
- Arrhythmia/Syncope
- Severe infection/Sepsis
- Hypoglycemia
- Periodic paralysis (electrolyte disturbance, K, Mg, Ca)
- Respiratory failure
- Emergent Diagnoses:
- Symptomatic Anemia
- Severe dehydration
- Hypothyroidism
- Polypharmacy
- Malignancy
- Aortic disease - occlusion, stenosis, dissection
- Other causes of weakness and paralysis
- Acute intermittent porphyria (ascending weakness)
- Can't miss diagnoses:
Evaluation
Known MS Patient with Exacerbation
- Urinalysis — rule out occult UTI as pseudorelapse trigger (very common in MS)
- CBC, Chemistry
- Consider CXR or other infectious workup based on presentation
- Temperature — fever suggests pseudorelapse or infection
- MRI with GAD generally not needed emergently unless diagnostic uncertainty or concern for PML
- LP is generally not needed for exacerbation of known MS — defer to neurology
Suspected New Diagnosis
- MRI with GAD of brain (+/- spine) and orbits (if optic neuritis suspected)
- Multiple lesions in supratentorial white matter, paraventricular area, spinal cord
- CSF
- Elevated protein and gamma-globulin (increased oligoclonal bands)
- Generally can be deferred to neurology
- CBC, Chemistry
- Urinalysis
- TSH, B12, RPR/VDRL — rule out MS mimics
- Consider NMO/aquaporin-4 antibody testing (especially if longitudinally extensive transverse myelitis or bilateral optic neuritis)[3]
Management
Pseudorelapse vs True Relapse
| True Relapse | Pseudorelapse | |
|---|---|---|
| Definition | New inflammatory demyelinating event | Temporary worsening of old symptoms from an external trigger |
| Duration | >24 hours, evolves over hours to days, persists days to weeks | Typically <24 hours; resolves when trigger is removed |
| Triggers | None (not explained by fever or infection) | Infection (especially UTI), fever, heat, stress, dehydration, medication changes |
| Symptoms | New neurologic symptoms OR worsening in a new distribution | Recurrence of prior/known deficits; symptoms may fluctuate |
| MRI | Often shows new gadolinium-enhancing lesion | No new lesion |
| Treatment | High-dose corticosteroids | Treat the underlying trigger; steroids are not indicated |
- Always check UA and infectious workup before initiating steroids — occult UTI is a very common pseudorelapse trigger in MS patients
- If symptoms are identical to a prior relapse, pseudorelapse is more likely (MS rarely causes repeated inflammation in the same CNS location)
- Symptoms that fluctuate or resolve completely and then return favor pseudorelapse[6]
Fever and Infection
- Fever must be reduced to minimize weakness associated with elevated temperature
- Antibiotics or surgical control of any infectious sources
Steroids
- High-dose steroid therapy for true relapses in the form of oral or intravenous methylprednisolone (1000 mg daily x 3-5 days)[7]
- Oral methylprednisolone at equivalent doses is non-inferior to IV and allows for outpatient treatment
- Do not initiate steroids until infection has been ruled out as the cause of symptom worsening
Plasma Exchange (PLEX)
- Second-line treatment for severe relapses refractory to high-dose corticosteroids[8]
- ~20-35% of patients may not fully respond to steroids alone
- Typically 5-7 sessions over 10-14 days
- Consult neurology early if relapse is severe or not responding to steroids
Disease-Modifying Therapies (DMTs)
- Suppression therapies (IFN-β, Glatiramer, etc.) — initiation is generally not in ED
- However, ED physicians should be aware of complications of DMTs in patients already on treatment:
| DMT | ED-Relevant Complications |
|---|---|
| Natalizumab (Tysabri) | Risk of PML (progressive multifocal leukoencephalopathy) — any new neurologic worsening warrants urgent MRI and JC virus testing |
| Fingolimod / Siponimod | Bradycardia, cardiac conduction abnormalities, macular edema |
| Ocrelizumab, Rituximab (anti-CD20) | Increased infection risk, infusion reactions, reactivation of hepatitis B |
| Interferons (Avonex, Rebif) | Flu-like symptoms (may mimic infection), hepatotoxicity, cytopenias |
| Dimethyl fumarate (Tecfidera) | Lymphopenia (increased infection risk); rare PML risk |
Disposition
Discharge
- Mild relapse in a patient who can ambulate safely
- Able to tolerate oral medications (oral methylprednisolone non-inferior to IV)
- Has reliable follow-up with neurology (ideally within 1-3 days)
- No untreated infection
- Adequate social support
Admission
- Any disease exacerbation associated with significant morbidity or functional impairment
- IV antibiotics or steroid therapy required
- Inability to ambulate safely or care for self
- Urinary retention requiring catheterization
- Concern for PML or other serious DMT complication
- Depression and significant risk of suicide
- Need for plasma exchange
Neurology Consultation
- New suspected MS diagnosis
- Severe relapse with significant functional impairment
- Steroid-refractory symptoms (discuss PLEX)
- Concern for PML or other DMT-related complication
- Diagnostic uncertainty
Return Precautions
- Worsening weakness or new weakness
- New or worsening visual symptoms
- Inability to urinate or new incontinence
- Difficulty breathing or swallowing
- Fever
See Also
References
- ↑ Multiple sclerosis: a practical overview for clinicians. British Medical Bulletin, Volume 95, Issue 1, September 2010, Pages 79–104. https://doi.org/10.1093/bmb/ldq017
- ↑ Flensner G, et al. "Sensitivity to heat in MS patients: a factor strongly influencing symptomology-an explorative survey". BMC Neurol. 2011. 11:27.
- ↑ Pelletier J, et al. "Multiple Sclerosis: An Emergency Medicine-Focused Narrative Review." J Emerg Med. 2024;66(4):e441-e456.
- ↑ Mellen Center Approaches: Management of MS Relapses. Cleveland Clinic Mellen Center for Multiple Sclerosis Treatment and Research. https://my.clevelandclinic.org/departments/neurological/depts/multiple-sclerosis/ms-approaches/relapse-management-ms
- ↑ Defined by Thompson AJ, et al. "Diagnosis of multiple sclerosis: 2017 revisions of the McDonald Criteria." Lancet Neurol. 2018;17(2):162-173.
- ↑ Amin A, et al. "Triaging Patients with Multiple Sclerosis in the Emergency Department: Room for Improvement." Proc Bayl Univ Med Cent. 2022;36(2):186-189.
- ↑ Le Page et al. Oral versus intravenous high-dose methylprednisolone for treatment of relapses in patients with multiple sclerosis (COPOUSEP): a randomised, controlled, double-blind, non-inferiority trial. Lancet. 2016 Jan 23;387(10016):340. https://core.ac.uk/download/pdf/52993687.pdf
- ↑ Ehler J, et al. "Therapeutic Plasma Exchange in Multiple Sclerosis and Autoimmune Encephalitis." J Clin Med. 2019;8(10):1793.
- ↑ Pelletier J, et al. "Multiple Sclerosis: An Emergency Medicine-Focused Narrative Review." J Emerg Med. 2024;66(4):e441-e456.