Stevens-Johnson Syndrome

Stevens-Johnson Syndrome A Brief Summary

Source • Uptodate Articles

Introduction • Stevens-Johnson syndrome (SJS) and toxic epidermal necrolysis (TEN) are severe idiosyncratic reactions. • They are most commonly triggered by medications, which are characterized by fever and mucocutaneous lesions leading to necrosis and sloughing of the epidermis. • SJS and TEN are distinguished chiefly by severity and percentage of body surface involved.

Stevens-Johnson syndrome • SJS is the less severe condition, in which skin sloughing is limited to less than 10 percent of the body surface. • It is characterized by a prodrome of malaise and fever, followed by the rapid onset of erythematous or purpuric macules and plaque. • The skin lesions progress to epidermal necrosis and sloughing. • Mucosal membranes are affected in 92 to 100 percent of patients, usually at two or more distinct sites (ocular, oral, and genital)

Toxic epidermal necrolysis • Toxic epidermal necrolysis (TEN), or Lyell's syndrome, involves sloughing of greater than 30 percent of the body surface area. • TEN also begins with a prodrome of fever and malaise, although temperatures are typically higher than those seen with SJS, often exceeding 39 degrees Celsius. • Mucous membranes are involved in nearly all cases.

TEN (continued) • The skin lesions are widely distributed erythematous macules and patches, although about 50 percent of cases begin with diffuse erythema. • The skin lesions progress to full-thickness epidermal necrosis leads. • The ultimate appearance of the skin has been likened to that of extensive thermal injury.

SJS/TEN overlap syndrome • SJS/TEN overlap syndrome describes patients with involvement of greater than 10 percent, but less than 30 percent of body surface area.

Etiology • Medications are the leading trigger of SJS and TEN in both adults and children. • In adults, medications cause 30 to 50 percent of cases of SJS and up to 80 percent of cases of TEN. • Infections are the next most common trigger of adult SJS (up to 15 percent). • Rare causes of SJS and TEN include vaccinations, systemic diseases, chemical exposure, herbal medicines, and foods.

Medications • The following groups of agents are most commonly implicated : • Anti-gout agents (especially allopurinol) • Antibiotics (sulfonamides >> penicillins > cephalosporins) • Antipsychotics and anti-epileptics (including carbamazepine, dilantin,lamotrigine, and phenobarbital) • Analgesics and non-steroidal anti-inflammatory agents (especially piroxicam)

HISTORY AND CLINICAL PRESENTATION • Drug exposure commonly precedes the onset of symptoms by one to three weeks (average 14 days) in medication-related cases. • Reexposure may result in onset of symptoms in as little as 48 hours.

Prodrome • SJS and TEN typically have a prodrome of fever and influenza-like symptoms one to three days before the development of mucocutaneous lesions. • Fever is usually higher with TEN, and often exceeds 39 degrees Celsius. • Skin tenderness, photophobia, and conjunctival itching or burning may be early symptoms in both conditions.

Clinical presentation • The following signs and symptoms, when present early in the course of a drug reaction or illness, should alert clinicians to the possibility of SJS/TEN : • Confluent erythema (erythroderma) • Facial edema or central facial involvement • Skin pain • Palpable purpura • Skin necrosis • Blisters and/or epidermal detachment • Mucous membrane erosions and crusting • Swelling of tongue

Clinical presentation • There may be multiorgan involvement. • In the absence of complications, the disorder generally resolves sufficiently that the patient can be discharged from the hospital in two to four weeks.

diagnosis • the diagnosis of SJS or TEN would be appropriate in a patient with: • A suggestive history of antecedent drug exposure or illness • A prodrome of acute-onset febrile illness and malaise • Erythematous macules, targetoid lesions, or diffuse erythema progressing to vesicles and bullae • Necrosis and sloughing of the epidermis (of varying degrees)

diagnosis • The diagnosis of SJS or TEN is clinical. Histologic findings on skin biopsy are supportive, but not independently diagnostic. • The differential diagnosis includes: • erythema multiforme • other types of severe medication reactions • severe reactions to bacterial toxins (eg, toxic shock syndrome • staphylococcal scalded skin syndrome) • Kawasaki disease.

Management • Early recognition and immediate withdrawal of any potentially causative agents are critical first steps in the management of SJS/TEN. • Multiple specialists should be involved in the care of patients with SJS/TEN when possible, including experts in • critical care • plastic surgery • Dermatology • infectious disease • Ophthalmology • nutrition

To prevent possible sepsis • Sepsis is the major cause of death. Sterile handling, infection control measures, topical antibiotic agents, and surveillance cultures of possible sites of superinfection are important components of prevention.

Supportive care > adjunctive therapies • Supportive care should be the primary focus of management of SJS/TEN. • Beyond this, there is insufficient evidence to establish the benefit of any adjunctive therapies. • Systemic glucocorticoids and intravenous gammaglobulin (IVIG) are commonly used at many centers, although not all. • Other treatments: plasmapheresis, thalidomide.

Prognosis • The mortality of SJS is 1 to 3 percent, while the mortality of TEN ranges from 25 to 35 percent. • Predictors of mortality include older age at onset and greater extent of skin involvement. • Long-term sequelae of the skin and eyes are common among survivors.

End • Thank you.

Stevens-Johnson Syndrome