Guillain-Barré Syndrome (GBS)

GBS is an autoimmune disorder (a postinfectious polyneuropathy) Involving motor, sensory and autonomic nerves.
GBS is a heterogeneous condition With several variant forms that is the most common cause of Acute flaccid paralysis.
The peak incidences Occur at late adolescence.

More than 60% Of patients with GBS have been diagnosed with an infection in the 3 weeks prior to the onset of weakness.
The most common antecedent symptoms is: Fever, cough, sore throat, and nasal discharge.

Antecedent events in GBS:

Rabies and swine influenza vaccines.
Cytomegalovirus, Epstein-Barr, Varicella Zoster, Zika virus infection.
Hepatitis A, B, C, E and HIV.
Campylobacter Jejuni, Mycoplasma Pneumonia bacterial infections.
Chlamydia Pneumoniae, acute Toxoplasmosis protozoan infection.
Mandible surgery, operation of the spine, cardiac surgery.
Blood transfusion and transplantation.
Antibiotics, allopurinol, thiabendazole, danazol, corticosteroids, D-penicillamine, gold salt, vincristine, zimelidine, stavudine, organophosphate poisoning, arsenic poisoning.
Genetic predisposition: HLA, immunoglobulin KM genes.

Symptoms:

Initial symptoms include numbness and paresthesia, Followed by weakness.
The paresthesias spread proximally, But rarely pass the wrists and ankles.
Tenderness on palpation and pain in muscles (Neck, back, buttock, and leg pain) are common in the initial stages. Affected children are irritable.
Weakness usually begins in the lower extremities And progressively involves the trunk, the upper limbs, and, finally, the bulbar muscles.
Proximal and distal muscles Are involved relatively symmetrically, but asymmetry is found in 9% of patients.
Onset is gradual And progresses over days or weeks; the process plateaus in 1-28 days.
Weakness can progress To inability or refusal to walk and later to “Flaccid tetraplegia”. Maximal severity of weakness is usually reached by 4 wk after onset.
The weakness is more prominent in proximal muscles, With the lower limbs being more affected than the upper limbs.

Phases of GBS:

The progressive phase, Which lasts a few days to 4 weeks.
The plateau phase, Which consists of persistent symptoms and lasts for a few days or weeks.
The improvement phase, When recovery takesplace.

Complications:

Cranial nerve involvement: Facial droop (may mimic Bell palsy), diplopias, dysarthria, dysphagia, ophthalmoplegia, pupillary disturbances.
Respiratory complaints: Dyspnea on exertion, shortness of breath, difficulty swallowing, slurred speech.
Cardiovascular complications: Heart rhythm abnormalities, blood pressure variability (both hypo- and hypertension), myocardial involvement, acute coronary syndromes, and electrocardiographic changes.
Other complications: Bowel and bladder function problems, facial flushing, anhidrosis and/or diaphoresis, Deep venous thrombosis (DVT) And consequent pulmonary embolism, residual numbness or other sensations.
Relapse: 7%.
Congenital Guillain-Barré syndrome.

Characteristic features:

Reduced strength of muscles.
Lower extremity weakness, Symmetrically and progressively.
Upper extremity, trunk, facial, and oropharyngeal weakness.
Facial weakness (cranial nerve VII), cranial nerves VI, III, XII, V, IX, and X.
- (Involvement of facial, oropharyngeal, and ocular muscles results in facial droop, dysphagia, dysarthria).
Ophthalmoparesis, ptosis.
Reduced or absent tendon reflexes (Hypo- or areflexia, respectively).
Hypotonia.
Sensory changes.

Specific signs to look for:

Diagnosis:

The typical clinical features.
Progressive weakness In both arms and both legs. The progression of the typical symptoms over days to 4 weeks, the relative symmetry of the symptoms, the presence of mild sensory symptoms, and symptoms indicative of cranial nerve involvement and/or autonomic dysfunction.
Cerebrospinal fluid (CSF): Protein level (>400 mg/l), with normal CSF cell counts.
Electromyography (EMG) and nerve conduction studies (NCS).
Pulmonary function.
A basic peripheral neuropathy workup Is recommended if the diagnosis is uncertain.
Magnetic resonance imaging (MRI) and computed tomography (CT) Scanning of the spine.
Labs: Electrolyte levels, calcium and glucose, LFTS, kidney function tests, CPK level, CBC and ESR.

Differential diagnosis:

Spinal cord lesions: Acute transverse myelitis, epidural abscess, tumors/vascular malformations, poliomyelitis (natural or live virus)/enteroviruses, cord compression from vertebral subluxation related to congenital abnormalities or trauma.
Peripheral neuropathies:
- Toxic: Vincristine / glue sniffing / heavy metal: Gold, arsenic, lead / organophosphate pesticides.
- Infections: HIV / diphtheria / lyme disease.
- Inborn errors of metabolism: Porphyria.
- Critical illness: Polyneuropathy.
Neuromuscular junction disorders: Tick paralysis, myasthenia gravis, botulism.
Myopathies: Periodic paralyses, dermatomyositis, critical illness myopathy.
Other: Hypercalcemia.

Normal nerve vs. Nerve affected by guillain-barre (damaged myelin / exposed fiber).

Optimal care In a hospital setting with Intensive care Facilities.
Plasma exchange (Plasmapheresis).
Intravenous immunoglobulin g.
Mechanical ventilation.
Pain management (NSAIDS, Gabapentin, opioids).
Monitoring for infectious complications (Eg, Pneumonia, urinary tract infections, septicemia).
Physical, occupational, and speech therapy.

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