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Stevens-Johnson syndrome

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Synonyms and keywords: SJS

Overview

Overview

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

Stevens-Johnson syndrome is a life-threatening condition affecting the skin, in which due to cell death the epidermis separates from the dermis. The syndrome is thought to be a hypersensitivity complex affecting the skin and the mucous membranes. Although the majority of cases are idiopathic, the main class of known causes is medications, followed by infections and (rarely) cancers.

Historical Perspective

It is named for Dr. Albert Mason Stevens and Dr. Frank Chambliss Johnson, American pediatricians who jointly published a description of the disorder in 1922.[1][2]

Classification

There is agreement in the medical literature that Stevens-Johnson syndrome can be considered a milder form of toxic epidermal necrolysis (TEN). Stevens-Johnson Syndrome involves less than 10 percent of body surface area while TEN involve more than 30 percent body surface area. However, there is debate whether it falls on a spectrum of disease that includes erythema multiforme and erythema multiforme major (also known as erythema multiforme majus).[3][4][5][6][7]

Pathophysiology

SJS, like toxic epidermal necrolysis and erythema multiforme, are characterized by confluent epidermal necrosis with minimal associated inflammation. The acuity is apparent from the (normal) basket weave-like pattern of the stratum corneum. The exact pathogenesis of SJS/TEN is not completely understood. However, It is believed that SJS/TEN is immune mediated and the result of a MHC Class-I restricted T-cell mediated cytotoxic reaction to drug antigens in keratinocytes leading to apoptosis[8]. Drug antigens bind to MHC-I and T cell Receptors (TCR) leading to the clonal proliferation of the drug specific cytotoxic T cells. On the activation of these T cells, various cytotoxic signals, including Fas/Fas ligand , Perforin/Granzyme B , and Granulysin, are known to be responsible for mediating the damages in skin lesions and the subsequent worsening of the disease.

Causes

Stevens-Johnson Syndrome is caused by drug reactions in the majority of the cases although it is also seen in certain viral and bacterial infections, and certain malignancies. Most commonly implicated drugs include sulfa drugs, Allopurinol, anti-epileptics (phenobarbital, carbamazepine, lamotrigine), antibiotics (for example Penicillin), and NSAIDs. Infections that are associated with SJS may include HIV, HSV, Mumps, Mycoplasma, Mycobacteria, Hepatitis and Streptococcal Infection.

Risk Factors

Common risk factors in the development of SJS include Immunodeficiency, HIV infection, active malignancy (particularly Hematological cancers), genetic Predisposition ( HLA-B 1502 and HLA-B 5801 variants in particular) on exposure to anti-epileptic medications or Allopurinol. Other risk factors may include past or family history of SJS/TEN, radiation therapy and rapid use of medications.

Epidemiology and Demographics

SJS is a rare condition, with a reported incidence of around 2-7 per 1000,000 people per year and a mean mortality rate of 4.8 percent. It is seen in patients of all age groups but particularly in children and young adults. Females are more commonly affected than males

Natural History, Complications and Prognosis

SJS proper (with less than 10% of body surface area involved) has the mortality rate of around 5%. The risk of death can be estimated using the SCORTEN scale, which takes a number of prognostic indicators into account. Other outcomes include organ damage and blindness.

Diagnosis

History and Symptoms

Stevens-Johnson syndrome (SJS) usually begins with a fever, sore throat, and fatigue, which is misdiagnosed and usually treated with antibiotics. Ulcers and other lesions begin to appear in the mucous membranes, almost always in the mouth and lips but also in the genital and anal regions. Those in the mouth are usually extremely painful and reduce the patient’s ability to eat or drink. Conjunctivitis of the eyes occurs in about 30% of children who develop SJS. A rash of round lesions about an inch across arises on the face, trunk, arms and legs, and soles of the feet, but usually not the scalp.[9]

Physical Examination

Common physical examination findings of SJS include rash or redness that is seen as red or reddish purple macules that enlarge to form bullae, vesicles and may rupture later to leave denuded skin underneath. Nikolsky sign may be positive which shows sloughing of the skin by gentle lateral pressure on the erythematous skin. In addition to skin, mucosal involvement is found mostly in oral mucosa in addition to the nasopharynx and ocular involvement-can be seen as edema, erythema, blistering, sloughing, necrosis and ulceration. In addition to these changes: fever, hypotension, and tachycardia can be seen in patients with SJS

Laboratory Findings

SJS is mainly diagnosed through the clinical skin findings. However, a skin biopsy is helpful in making the definitive diagnosis. Other tests are done to either rule out the superimposed bacterial infection, measure disease severity or detect the causative agent or organism. Tests include CBC, BMP, Blood cultures, ESR, CRP, IL-6, ELISA for virus detection among others[10].

Chest X-Ray

There are no x-ray findings associated with SJS. However, an x-ray may be helpful in the diagnosis of pulmonary complications of Stevens-Johnson Syndrome, in which CXR may show interstitial lung infiltrates[11]

Treatment

Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis should be managed in a burn unit, Specialized dermatology or Intensive Care unit. Patient’s fluid status, hemodynamic stability, wound surface area and pain should be assessed and managed immediately upon admission. Treatment is initially similar to that of patients with thermal burns, and continued care can only be supportive (e.g. IV fluids) and symptomatic (e.g. analgesic mouth rinse for mouth ulcer); there is no specific drug treatment. Treatment with corticosteroids is controversial since it might aggravate the condition or increase risk of secondary infections. Other agents have been used, including cyclophosphamide and cyclosporine, among with cyclosporin has exhibited some therapeutic success. Intravenous immunoglobulin (IVIG) treatment has shown some promise in reducing the length of the reaction and improving symptoms. Other common supportive measures include the use of topical pain anesthetics and antiseptics, maintaining a warm environment, and intravenous analgesics. An ophthalmologist should be consulted immediately, as SJS frequently causes the formation of scar tissue inside the eyelids leading to corneal vascularization and impaired vision, as well as a host of other ocular problems. Also, an extensive physical therapy program ensues after the patient is discharged from the hospital.

References

  1. Template:WhoNamedIt
  2. [http://dictionary.reference.com/browse/Stevens-Johnson%20syndrome Stevens-Johnson syndrome – Definitions from Dictionary.com
  3. Carrozzo M, Togliatto M, Gandolfo S (1999). “[Erythema multiforme. A heterogeneous pathologic phenotype]”. Minerva Stomatol. 48 (5): 217–26. PMID 10434539.
  4. Farthing P, Bagan J, Scully C (2005). “Mucosal disease series. Number IV. Erythema multiforme”. Oral Dis. 11 (5): 261–7. PMID 16120111.
  5. Bastuji-Garin S, Rzany B, Stern RS, Shear NH, Naldi L, Roujeau JC (1993). “Clinical classification of cases of toxic epidermal necrolysis, Stevens-Johnson syndrome, and erythema multiforme”. Archives of dermatology. 129 (1): 92–6. doi:10.1001/archderm.129.1.92. PMID 8420497.
  6. Ogundele O, Silverberg MA. Erythema Multiforme. eMedicine.com. URL: http://www.emedicine.com/emerg/topic173.htm. Accessed on: May 6, 2007.
  7. Auquier-Dunant A, Mockenhaupt M, Naldi L, Correia O, Schröder W, Roujeau JC (2002). “Correlations between clinical patterns and causes of erythema multiforme majus, Stevens-Johnson syndrome, and toxic epidermal necrolysis: results of an international prospective study”. Arch Dermatol. 138 (8): 1019–24. PMID 12164739. Unknown parameter |month= ignored (help)
  8. Correia O, Delgado L, Ramos JP, Resende C, Torrinha JA (1993). “Cutaneous T-cell recruitment in toxic epidermal necrolysis. Further evidence of CD8+ lymphocyte involvement”. Arch Dermatol. 129 (4): 466–8. PMID 8466217.
  9. Tigchelaar H (2008). “Stevens–Johnson Syndrome: An Intriguing Diagnosis”. Consultant for Pediatricians. Unknown parameter |coauthors= ignored (help); Unknown parameter |month= ignored (help)
  10. Çekiç Ş, Canıtez Y, Sapan N (2016). “Evaluation of the patients diagnosed with Stevens-Johnson syndrome and toxic epidermal necrolysis: a single center experience”. Turk Pediatric Ars. 51 (3): 152–158. doi:10.5152/TurkPediatriArs.2016.3836. PMC 5047364. PMID 27738400.
  11. Amanda M.. Oakley & Karthik Krishnamurthy (2018). “Stevens Johnson Syndrome (Toxic Epidermal Necrolysis)”. PMID 29083827. Unknown parameter |month= ignored (help)


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Historical Perspective

Historical Perspective

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

It is named for Dr. Albert Mason Stevens and Dr. Frank Chambliss Johnson, American pediatricians who jointly published a description of the disorder in 1922.[1][2]

Historical Perspective

Discovery

  • SJS was first discovered by Dr. Albert Mason Stevens and Dr. Frank Chambliss Johnson, American pediatricians who jointly published a description of the disorder in 1922 in two patients, boys aged 7 and 8 years

Famous Cases

The following are a few famous cases of disease name:

  • Manute Bol (Oct. 16, 1962 – June 19, 2010) was a Sudanese-born basketball player and political activist
  • Padma Lakshmi – Actress, Model, cookbook author
  • Gene Sauers – American professional golfer [3]
  • Karen Elaine Morton (Oct. 3,1958 – Feb.11, 2014) – Playboy Playmate of the Month July 1978, died from organ failure due to complications from Stevens-Johnson Syndrome[4].
  • Samantha Reckis -The child was given the popular pain reliever after showing signs of fever around thanksgiving in 2003 and later developed TEN which is more severe form of SJS – Family was awarded $63 million in Motrin case in their lawsuit against Johnson & Johnson[5]

References

  1. Template:WhoNamedIt
  2. [http://dictionary.reference.com/browse/Stevens-Johnson%20syndrome Stevens-Johnson syndrome – Definitions from Dictionary.com
  3. Graff, Chad (31 July 2013). “3M golf: Gene Sauers thriving after torturous battle with skin disease”. St. Paul Pioneer Press. Archived from the original on 3 October 2014
  4. Morton, Karen. “Karen Morton Biography”. imdb.com. Archived from the original on 2 October 2016.
  5. $63 million verdict in Children’s Motrin case upheld”. Boston Globe. 17 April 2015. Archived from the original on 31 October 2016.

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Classification

Classification

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

There is agreement in the medical literature that Stevens-Johnson syndrome can be considered a milder form of toxic epidermal necrolysis (TEN). Stevens-Johnson Syndrome involves less than 10 percent of body surface area while TEN involve more than 30 percent body surface area. However, there is debate whether it falls on a spectrum of disease that includes erythema multiforme and erythema multiforme major (also known as erythema multiforme majus).[1][2][3][4][5]

Classification

Skin lesions can be classified into 5 Different Categories as defined below[6]:

  • Bullous Eythema Multiforme: Detachment below 10% of the body surface area (BSA) plus localized typical targets or raised atypical targets
  • Stevens-Johnson Syndrome: Detachment below 10% of the body surface area plus widespread erythematous or purpuric macules or flat atypical targets
  • Stevens-Johnson and Toxic Epidermal Necrolysis Overlap: Detachment between 10% and 30% of the body surface area plus widespread purpuric macules or flat atypical targets
  • Toxic Epidermal Necrolysis with Spots: Detachment above 30% of the body surface area plus widespread purpuric macules or flat atypical targets
  • Toxic Epidermal Necrolysis without Spots: Detachment above 10% of the body surface area with large epidermal sheets and without any purpuric macule or target

References

  1. Carrozzo M, Togliatto M, Gandolfo S (1999). “[Erythema multiforme. A heterogeneous pathologic phenotype]”. Minerva Stomatol. 48 (5): 217–26. PMID 10434539.
  2. Farthing P, Bagan J, Scully C (2005). “Mucosal disease series. Number IV. Erythema multiforme”. Oral Dis. 11 (5): 261–7. PMID 16120111.
  3. Bastuji-Garin S, Rzany B, Stern RS, Shear NH, Naldi L, Roujeau JC (1993). “Clinical classification of cases of toxic epidermal necrolysis, Stevens-Johnson syndrome, and erythema multiforme”. Archives of dermatology. 129 (1): 92–6. doi:10.1001/archderm.129.1.92. PMID 8420497.
  4. Ogundele O, Silverberg MA. Erythema Multiforme. eMedicine.com. URL: http://www.emedicine.com/emerg/topic173.htm. Accessed on: May 6, 2007.
  5. Auquier-Dunant A, Mockenhaupt M, Naldi L, Correia O, Schröder W, Roujeau JC (2002). “Correlations between clinical patterns and causes of erythema multiforme majus, Stevens-Johnson syndrome, and toxic epidermal necrolysis: results of an international prospective study”. Arch Dermatol. 138 (8): 1019–24. PMID 12164739. Unknown parameter |month= ignored (help)
  6. Bastuji-Garin S, Rzany B, Stern RS, Shear NH, Naldi L, Roujeau JC (1993). “Clinical classification of cases of toxic epidermal necrolysis, Stevens-Johnson syndrome, and erythema multiforme”. Arch Dermatol. 129 (1): 92–6. PMID 8420497.

Template:WH Template:WS

Pathophysiology

Pathophysiology

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

SJS, like toxic epidermal necrolysis and erythema multiforme, are characterized by confluent epidermal necrosis with minimal associated inflammation. The acuity is apparent from the (normal) basket weave-like pattern of the stratum corneum. The exact pathogenesis of SJS/TEN is not completely understood. However, It is believed that SJS/TEN is immune-mediated and the result of an MHC Class-I restricted T-cell mediated cytotoxic reaction to drug antigens in keratinocytes leading to apoptosis[1]. Drug antigens bind to MHC-I and T cell Receptors (TCR) leading to the clonal proliferation of the drug-specific cytotoxic T cells. On the activation of these T cells, various cytotoxic signals, including Fas/Fas ligand, perforin/granzyme B, and granulysin, are known to be responsible for mediating the damages in skin lesions and the subsequent worsening of the disease.

Pathophysiology

Pathogenesis

  • The exact pathogenesis of SJS/TEN is not completely understood
  • However, It is believed that SJS/TEN is immune mediated and the result of a MHC Class-I restricted T-cell mediated cytotoxic reaction to drug antigens in keratinocytes leading to apoptosis[1]
  • Drug antigens bind to MHC-I and T cell Receptors (TCR) leading to the clonal proliferation of the drug specific cytotoxic T cells
  • On the activation of these T cells, various cytotoxic signals, including Fas/Fas ligand , perforin/granzyme B , and granulysin, are known to be responsible for mediating the damages in skin lesions and the subsequent worsening of the disease as explained below.
    • T lymphocytes found in bisters were CD8+, HLA-DR+, CLA+ (cutaneous lymphocyte antigen), CD56+ and were shown to be strongly immunoreactive for granzyme B suggesting perforin/granzyme mediated cytotoxicity[2]
    • There is also beleived to be some involvement of the soluble FasL (sFasL) in keratinocyte apoptosis in SJS and TEN. sFasL is secreted by peripheral bood mononuclear cells (PBMC’s) and interacts with the Fas that is expressed on keratinocyte leading to apoptosis. Higher serum levels of sFasL may be seen in patients with suspicion of SJS/TEN[3]
    • Recent studies suggest that the Granulysin, which is a cytotoxic protein released from cytotoxic T cells or natural killer (NK) cells, is a key mediator for disseminated keratinocyte apoptosis in SJS/TEN[4] and is identified by gene expression profiling as the highly cytotoxic molecule and confirmed by PCR and immunohistochemistry. Granulysin concentrations in blister fluid were found to be 2x to 4x more than the Perforin/Granzyme B/sFasL thus making it the most important cytotoxic molecule in SJS/TEN pathogenesis[5]
    • Other cytokines that may be associated with trafficking, activation and proliferation of cytotoxic T cells and other immune cells include IFN-Y(gamma), TNF-aplha, IL-2, IL-5, IL-6, IL-10, IL-13. IL-15 was one of the cytokines that was seen in the highest amount and also correlated with disease severity and mortality. Studies also suggest that IL-15 is important in mentaining long-lasting cytotoxic T lymphocyte responses as well as generating and mentaining Nk cells. It is also responsible for enhancing MHC-I antigen presentation thus has an important contribution in SJS/TEN pathogenesis[6]

Genetics

  • Some people have genetic predisposition which increases their risk of developing SJS in response to certain trigger medications. The most common genetic variation contributing to the predisposition is seen in the HLA-B gene. Examples include
    • People with HLA-B 1502 gene have 10 percent risk of developing SJS on exposure to anti-epileptic drugs like Phenytoin, Carbamazepine, Phenobarbital, Lamotrigine[7]
    • People with HLA-B 5801 have high risk of developing SJS on exposure to Allupurinol[8]
    • Certain studies have identified HLA-B 3101 as a genetic risk factor for carbamazepine induced skin reactions including SJS[9]
    • HLA-B 1511, HLA-B 2402 are also considered to increase SJS risk in certain populations
  • Genetic Polymorphism in CYP2C gene variants may lead to an increased risk of SJS/TEN on exposure to certain anti-seizure medications in some populations[10]

Associated Conditions

Some conditions that are associated with an increased risk of SJS/TEN include HIV, immunodeficiency, active cancers (mostly hematological) and some genetic factors.

Gross Pathology

  • On gross examination in SJS/TEN, blisters/erosions/bullae and vesicles are seen along with Confluent redness and skin sloughing. Nikolsky Sign may be positive which is the detachment of superficial epidermis on gentle pressure or rubbing of skin

Microscopic Pathology

On microscopic histopathological analysis,full-thickness extensive keratinocyte necrosis that develop into subepidermal bullae is seen in established SJS/TEN[11]. Satellite cell necrosis may also be seen[12]

References

  1. 1.0 1.1 Correia O, Delgado L, Ramos JP, Resende C, Torrinha JA (1993). “Cutaneous T-cell recruitment in toxic epidermal necrolysis. Further evidence of CD8+ lymphocyte involvement”. Arch Dermatol. 129 (4): 466–8. PMID 8466217.
  2. Nassif A, Bensussan A, Boumsell L, Deniaud A, Moslehi H, Wolkenstein P; et al. (2004). “Toxic epidermal necrolysis: effector cells are drug-specific cytotoxic T cells”. J Allergy Clin Immunol. 114 (5): 1209–15. doi:10.1016/j.jaci.2004.07.047. PMID 15536433.
  3. Abe R, Shimizu T, Shibaki A, Nakamura H, Watanabe H, Shimizu H (2003). “Toxic epidermal necrolysis and Stevens-Johnson syndrome are induced by soluble Fas ligand”. Am J Pathol. 162 (5): 1515–20. doi:10.1016/S0002-9440(10)64284-8. PMC 1851208. PMID 12707034.
  4. Chung WH, Hung SI (2012). “Recent advances in the genetics and immunology of Stevens-Johnson syndrome and toxic epidermal necrosis”. J Dermatol Sci. 66 (3): 190–6. doi:10.1016/j.jdermsci.2012.04.002. PMID 22541332.
  5. Chung WH, Hung SI, Yang JY, Su SC, Huang SP, Wei CY; et al. (2008). “Granulysin is a key mediator for disseminated keratinocyte death in Stevens-Johnson syndrome and toxic epidermal necrolysis”. Nat Med. 14 (12): 1343–50. doi:10.1038/nm.1884. PMID 19029983.
  6. Su SC, Mockenhaupt M, Wolkenstein P, Dunant A, Le Gouvello S, Chen CB; et al. (2017). “Interleukin-15 Is Associated with Severity and Mortality in Stevens-Johnson Syndrome/Toxic Epidermal Necrolysis”. J Invest Dermatol. 137 (5): 1065–1073. doi:10.1016/j.jid.2016.11.034. PMID 28011147.
  7. Li X, Yu K, Mei S, Huo J, Wang J, Zhu Y; et al. (2015). “HLA-B*1502 increases the risk of phenytoin or lamotrigine induced Stevens-Johnson Syndrome/toxic epidermal necrolysis: evidence from a meta-analysis of nine case-control studies”. Drug Res (Stuttg). 65 (2): 107–11. doi:10.1055/s-0034-1375684. PMID 24871931.
  8. Somkrua R, Eickman EE, Saokaew S, Lohitnavy M, Chaiyakunapruk N (2011). “Association of HLA-B*5801 allele and allopurinol-induced Stevens Johnson syndrome and toxic epidermal necrolysis: a systematic review and meta-analysis”. BMC Med Genet. 12: 118. doi:10.1186/1471-2350-12-118. PMC 3189112. PMID 21906289.
  9. McCormack M, Alfirevic A, Bourgeois S, Farrell JJ, Kasperavičiūtė D, Carrington M; et al. (2011). “HLA-A*3101 and carbamazepine-induced hypersensitivity reactions in Europeans”. N Engl J Med. 364 (12): 1134–43. doi:10.1056/NEJMoa1013297. PMC 3113609. PMID 21428769.
  10. Manuyakorn W, Siripool K, Kamchaisatian W, Pakakasama S, Visudtibhan A, Vilaiyuk S; et al. (2013). “Phenobarbital-induced severe cutaneous adverse drug reactions are associated with CYP2C19*2 in Thai children”. Pediatr Allergy Immunol. 24 (3): 299–303. doi:10.1111/pai.12058. PMID 23551241.
  11. Orime M (2017). “Immunohistopathological Findings of Severe Cutaneous Adverse Drug Reactions”. J Immunol Res. 2017: 6928363. doi:10.1155/2017/6928363. PMC 5684554. PMID 29226159.
  12. Hosaka H, Ohtoshi S, Nakada T, Iijima M (2010). “Erythema multiforme, Stevens-Johnson syndrome and toxic epidermal necrolysis: frozen-section diagnosis”. J Dermatol. 37 (5): 407–12. doi:10.1111/j.1346-8138.2009.00746.x. PMID 20536645.

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Causes

Causes

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

Stevens-Johnson Syndrome is caused by drug reactions in the majority of the cases although it is also seen in certain viral and bacterial infections, and certain malignancies. Most commonly implicated drugs include sulfa drugs, Allopurinol, Anti-epileptics (phenobarbital, carbamazepine, lamotrigine), antibiotics (for example Penicillin), and NSAIDs. Infections that are associated with SJS may include HIV, HSV, Mumps, Mycoplasma, Mycobacteria, Hepatitis and streptococcal Infection.

Causes

There are different triggers for Stevens-Johnson Syndrome Include drug-induced, infections, some systemic and Autoimmune disease among others.

Drug Induced SJS:

One of the main triggers to cause SJS is the drug induced reaction

Infection Induced SJS

SJS can be caused by infections, usually following viral infections:

Some bacterial infections may be associated with SJS, including following[8]:

Other Causes

References

  1. Levi N, Bastuji-Garin S, Mockenhaupt M, Roujeau JC, Flahault A, Kelly JP; et al. (2009). “Medications as risk factors of Stevens-Johnson syndrome and toxic epidermal necrolysis in children: a pooled analysis”. Pediatrics. 123 (2): e297–304. doi:10.1542/peds.2008-1923. PMID 19153164.
  2. Halevy S, Ghislain PD, Mockenhaupt M, Fagot JP, Bouwes Bavinck JN, Sidoroff A; et al. (2008). “Allopurinol is the most common cause of Stevens-Johnson syndrome and toxic epidermal necrolysis in Europe and Israel”. J Am Acad Dermatol. 58 (1): 25–32. doi:10.1016/j.jaad.2007.08.036. PMID 17919772.
  3. Hällgren J, Tengvall-Linder M, Persson M, Wahlgren CF (2003). “Stevens-Johnson syndrome associated with ciprofloxacin: a review of adverse cutaneous events reported in Sweden as associated with this drug”. J Am Acad Dermatol. 49 (5 Suppl): S267–9. doi:10.1016/S0190. PMID 14576649.
  4. Medsafe Data Sheet March 8, 2005. Accessed April 26, 2007.
  5. Raksha MP, Marfatia YS (2008). “Clinical study of cutaneous drug eruptions in 200 patients”. Indian J Dermatol Venereol Leprol. 74 (1): 80. PMID 18193504.
  6. Fagot J, Mockenhaupt M, Bouwes-Bavinck J, Naldi L, Viboud C, Roujeau J (2001). “Nevirapine and the risk of Stevens-Johnson syndrome or toxic epidermal necrolysis”. AIDS. 15 (14): 1843–8. doi:10.1097/00002030-200109280-00014. PMID 11579247.
  7. Devi K, George S, Criton S, Suja V, Sridevi P (2005). “Carbamazepine–the commonest cause of toxic epidermal necrolysis and Stevens-Johnson syndrome: a study of 7 years”. Indian J Dermatol Venereol Leprol. 71 (5): 325–8. PMID 16394456.
  8. “Stevens-Johnson syndrome and toxic epidermal necrolysis: a review”.
  9. Wetter DA, Camilleri MJ (2010). “Clinical, etiologic, and histopathologic features of Stevens-Johnson syndrome during an 8-year period at Mayo Clinic”. Mayo Clin Proc. 85 (2): 131–8. doi:10.4065/mcp.2009.0379. PMC 2813820. PMID 20118388.
  10. Stevens-Johnson Syndrome-emerg/555 at eMedicine


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Differentiating Stevens-Johnson Syndrome from other Diseases

Differentiating Stevens-Johnson Syndrome from other Diseases

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: João André Alves Silva, M.D. [2]

Overview

Stevens-Johnson syndrome must be differentiated from other diseases that cause fever, ulcers in the mucous membranes and skin, sore throat, and fatigue, including chickenpox, herpes zoster, erythema multiforme, among others.

Differential Diagnosis

Different rash-like conditions can be confused with Stevens-Johnson syndrome and are thus included in its differential diagnosis. The various conditions that should be differentiated from Stevens-Johnson syndrome include:[1][2][3][4][5][6][7]

Disease Features
Impetigo 
  • It commonly presents with pimple-like lesions surrounded by erythematous skin. Lesions are pustules, filled with pus, which then break down over 4-6 days and form a thick crust. It’s often associated with insect bites, cuts, and other forms of trauma to the skin.
Insect bites
  • The insect injects formic acid, which can cause an immediate skin reaction often resulting in a rash and swelling in the injured area, often with formation of vesicles.
Kawasaki disease
Measles
Monkeypox
  • The presentation is similar to smallpox, although it is often a milder form, with fever, headache, myalgia, back pain, swollen lymph nodes, a general feeling of discomfort, and exhaustion. Within 1 to 3 days (sometimes longer) after the appearance of fever, the patient develops a papular rash, often first on the face. The lesions usually develop through several stages before crusting and falling off.
Rubella
Atypical measles
Coxsackievirus
  • The most commonly caused disease is the Coxsackie A disease, presenting as hand, foot and mouth disease. It may be asymptomatic or cause mild symptoms, or it may produce fever and painful blisters in the mouth (herpangina), on the palms and fingers of the hand, or on the soles of the feet. There can also be blisters in the throat or above the tonsils. Adults can also be affected. The rash, which can appear several days after high temperature and painful sore throat, can be itchy and painful, especially on the hands/fingers and bottom of feet.
Acne
Syphilis It commonly presents with gneralized systemic symptoms such as malaise, fatigue, headache and fever. Skin eruptions may be subtle and asymptomatic It is classically described as:
Molluscum contagiosum
  • The lesions are commonly flesh-colored, dome-shaped, and pearly in appearance. They are often 1-5 millimeters in diameter, with a dimpled center. Generally not painful, but they may itch or become irritated. Picking or scratching the lesions may lead to further infection or scarring. In about 10% of the cases, eczema develops around the lesions. They may occasionally be complicated by secondary bacterial infections.
Mononucleosis
Toxic erythema
  • It is a common rash in infants, with clustered and vesicular appearance.
Rat-bite fever
  • It commonly presents with fever, chills, open sore at the site of the bite and rash, which may show red or purple plaques.
Parvovirus B19
  • The rash of fifth disease is typically described as “slapped cheeks,” with erythema across the cheeks and sparing the nasolabial folds, forehead, and mouth.
Cytomegalovirus
Scarlet fever
Rocky Mountain spotted fever
Stevens-Johnson syndrome
  • The symptoms may include fever, sore throat and fatigue. Commonly presents ulcers and other lesions in the mucous membranes, almost always in the mouth and lips but also in the genital and anal regions. Those in the mouth are usually extremely painful and reduce the patient’s ability to eat or drink. Conjunctivitis of the eyes occurs in about 30% of children. A rash of round lesions about an inch across, may arise on the face, trunk, arms and legs, and soles of the feet, but usually not on the scalp.
Varicella-zoster virus
  • It commonly starts as a painful rash on one side of the face or body. The rash forms blisters that typically scab over in 7-10 days and clears up within 2-4 weeks.
Chickenpox
  • It commonly starts with conjunctival and catarrhal symptoms and then characteristic spots appearing in two or three waves, mainly on the body and head, rather than the hands, becoming itchy raw pox (small open sores which heal mostly without scarring). Touching the fluid from a chickenpox blister can also spread the disease.
Meningococcemia
Rickettsial pox
Meningitis

References

  1. Hartman-Adams H, Banvard C, Juckett G (2014). “Impetigo: diagnosis and treatment”. Am Fam Physician. 90 (4): 229–35. PMID 25250996.
  2. Mehta N, Chen KK, Kroumpouzos G (2016). “Skin disease in pregnancy: The approach of the obstetric medicine physician”. Clin Dermatol. 34 (3): 320–6. doi:10.1016/j.clindermatol.2016.02.003. PMID 27265069.
  3. Moore, Zack S; Seward, Jane F; Lane, J Michael (2006). “Smallpox”. The Lancet. 367 (9508): 425–435. doi:10.1016/S0140-6736(06)68143-9. ISSN 0140-6736.
  4. Ibrahim F, Khan T, Pujalte GG (2015). “Bacterial Skin Infections”. Prim Care. 42 (4): 485–99. doi:10.1016/j.pop.2015.08.001. PMID 26612370.
  5. Ramoni S, Boneschi V, Cusini M (2016). “Syphilis as “the great imitator”: a case of impetiginoid syphiloderm”. Int J Dermatol. 55 (3): e162–3. doi:10.1111/ijd.13072. PMID 26566601.
  6. Kimura U, Yokoyama K, Hiruma M, Kano R, Takamori K, Suga Y (2015). “Tinea faciei caused by Trichophyton mentagrophytes (molecular type Arthroderma benhamiae ) mimics impetigo : a case report and literature review of cases in Japan”. Med Mycol J. 56 (1): E1–5. doi:10.3314/mmj.56.E1. PMID 25855021.
  7. CEDEF (2012). “[Item 87–Mucocutaneous bacterial infections]”. Ann Dermatol Venereol. 139 (11 Suppl): A32–9. doi:10.1016/j.annder.2012.01.002. PMID 23176858.


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Epidemiology and Demographics

Epidemiology and Demographics

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

SJS is a rare condition, with a reported incidence of around 2-7 per 1000,000 people per year and a mean mortality rate of 4.8 percent. It is seen in patients of all age groups but particularly in children and young adults. Females are more commonly affected than males

Epidemiology and Demographics

Incidence

  • The incidence of SJS is approximately 2-7 per 1000,000 individuals per year.[1]
  • The incidences of SJS, SJS-TEN, and TEN were found to be a mean 5.3, 0.8, and 0.4 cases per million children per year in the US[2]
  • The mean estimated incidences of SJS, SJS/TEN, and TEN were found to be 9.2, 1.6, and 1.9 per million adults per year in the US[3]

Case-fatality rate/Mortality rate

  • Between years 2009-2012, the Mean adjusted mortality was 4.8% for SJS, 19.4% for SJS/TEN, and 14.8% for TEN[4]

Age

  • Patients of all age groups may develop SJS.

Race

  • The incidence of SJS might be higher in Non White/Multiracial people as compared to White“Redirecting”.

Gender

References

  1. Strom BL, Carson JL, Halpern AC, Schinnar R, Snyder ES, Shaw M; et al. (1991). “A population-based study of Stevens-Johnson syndrome. Incidence and antecedent drug exposures”. Arch Dermatol. 127 (6): 831–8. PMID 2036028.
  2. Hsu DY, Brieva J, Silverberg NB, Paller AS, Silverberg JI (2017). “Pediatric Stevens-Johnson syndrome and toxic epidermal necrolysis in the United States”. J Am Acad Dermatol. 76 (5): 811–817.e4. doi:10.1016/j.jaad.2016.12.024. PMC 5502094. PMID 28285784.
  3. Hsu DY, Brieva J, Silverberg NB, Silverberg JI (2016). “Morbidity and Mortality of Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis in United States Adults”. J Invest Dermatol. 136 (7): 1387–1397. doi:10.1016/j.jid.2016.03.023. PMID 27039263.
  4. Hsu DY, Brieva J, Silverberg NB, Silverberg JI (2016). “Morbidity and Mortality of Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis in United States Adults”. J Invest Dermatol. 136 (7): 1387–1397. doi:10.1016/j.jid.2016.03.023. PMID 27039263.

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Risk Factors

Risk Factors

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

Common risk factors in the development of SJS include immunodeficiency, HIV infection, active malignancy (particularly Hematological cancers), genetic Predisposition ( HLA-B 1502 and HLA-B 5801 variants in particular) on exposure to antiepileptic medications or Allopurinol. Other risk factors may include past or family history of SJS/TEN, radiation therapy and rapid use of medications.

Risk Factors

Common risk factors in the development of Stevens-Johnson Syndrome include the following:

HIV Infection

  • Risk of Developing SJS is 100 times greater in HIV Infected people as compared to the general population[1]

Immunodeffeciency

Malignancy

Genetic Factors

  • Some people have genetic predisposition which increases their risk of developing SJS in response to certain trigger medications. The most common genetic variation contributing to the predisposition is seen in the HLA-B gene. Examples include
    • People with HLA-B 1502 gene have 10 percent risk of developing SJS on exposure to anti-epileptic drugs like Phenytoin, Carbamazepine, Phenobarbital, Lamotrigine[4]
    • People with HLA-B 5801 have high risk of developing SJS on exposure to Allupurinol[5]
    • Certain studies have identified HLA-B 3101 as a genetic risk factor for Carbamazepine induced skin reactions including SJS[6]
    • HLA-B 1511, HLA-B 2402 are also considered to increase SJS risk in certain populations
  • Genetic polymorphism in CYP2C gene variants may lead to an increased risk of SJS/TEN on exposure to certain anti-seizure medications in some populations[7]

Others

Other factors that may increase the risk of SJS inclde;

  • Past history of SJS
  • Family history of SJS
  • High dose of medications
  • Rapid Intake of medications
  • Physical stimuli like radiation therapy[8]

References

  1. Mittmann N, Knowles SR, Koo M, Shear NH, Rachlis A, Rourke SB (2012). “Incidence of toxic epidermal necrolysis and Stevens-Johnson Syndrome in an HIV cohort: an observational, retrospective case series study”. Am J Clin Dermatol. 13 (1): 49–54. doi:10.2165/11593240-000000000-00000. PMID 22145749.
  2. Horne NS, Narayan AR, Young RM, Frieri M (2006). “Toxic epidermal necrolysis in systemic lupus erythematosus”. Autoimmun Rev. 5 (2): 160–4. doi:10.1016/j.autrev.2005.10.003. PMID 16431352.
  3. Hsu DY, Brieva J, Silverberg NB, Silverberg JI (2016). “Morbidity and Mortality of Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis in United States Adults”. J Invest Dermatol. 136 (7): 1387–1397. doi:10.1016/j.jid.2016.03.023. PMID 27039263.
  4. Li X, Yu K, Mei S, Huo J, Wang J, Zhu Y; et al. (2015). “HLA-B*1502 increases the risk of phenytoin or lamotrigine induced Stevens-Johnson Syndrome/toxic epidermal necrolysis: evidence from a meta-analysis of nine case-control studies”. Drug Res (Stuttg). 65 (2): 107–11. doi:10.1055/s-0034-1375684. PMID 24871931.
  5. Somkrua R, Eickman EE, Saokaew S, Lohitnavy M, Chaiyakunapruk N (2011). “Association of HLA-B*5801 allele and allopurinol-induced Stevens Johnson syndrome and toxic epidermal necrolysis: a systematic review and meta-analysis”. BMC Med Genet. 12: 118. doi:10.1186/1471-2350-12-118. PMC 3189112. PMID 21906289.
  6. McCormack M, Alfirevic A, Bourgeois S, Farrell JJ, Kasperavičiūtė D, Carrington M; et al. (2011). “HLA-A*3101 and carbamazepine-induced hypersensitivity reactions in Europeans”. N Engl J Med. 364 (12): 1134–43. doi:10.1056/NEJMoa1013297. PMC 3113609. PMID 21428769.
  7. Manuyakorn W, Siripool K, Kamchaisatian W, Pakakasama S, Visudtibhan A, Vilaiyuk S; et al. (2013). “Phenobarbital-induced severe cutaneous adverse drug reactions are associated with CYP2C19*2 in Thai children”. Pediatr Allergy Immunol. 24 (3): 299–303. doi:10.1111/pai.12058. PMID 23551241.
  8. Duncan KO, Tigelaar RE, Bolognia JL (1999). “Stevens-Johnson syndrome limited to multiple sites of radiation therapy in a patient receiving phenobarbital”. J Am Acad Dermatol. 40 (3): 493–6. PMID 10071329.

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Screening

Screening

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief:

Overview

There is insufficient evidence to recommend routine screening for SJS

Screening

There is insufficient evidence to recommend routine screening for SJS

References

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Natural History, Complications and Prognosis

Natural History, Complications and Prognosis

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Anila Hussain, MD [2]

Overview

  • The symptoms of SJS usually start within 2 months of starting a drug or other inciting trigger with symptoms such as red or reddish blue macules/papules on trunk and extremities and later increase in size and coalesce. Blisters/erosions/bullae and vesicles are seen later with confluent redness with skin sloughing. Most lesions heal rapidly within 1-3 weeks unless secondary bacterial infection of lesions occurs. Recovery can take longer, although it usually depends on the severity of symptoms and body surface area involved. Mortality rate is 1-5 percent in SJS and in TEN is 25-35 percent[1]

Natural History, Complications, and Prognosis

Natural History

  • The symptoms of SJS usually start within 2 months of starting a drug or other inciting trigger with symptoms such as red or reddish blue macules/papules on trunk and extremities and later increase in size and coalesce.Blisters/erosions/bullae and vesicles are seen later with confluent redness with skin sloughing.
  • Most lesions heal rapidly within 1-3 weeks unless secondary bacterial infection of lesions occurs.
  • Recovery can take longer, although it usually depends on the severity of symptoms and body surface area involved

Complications

  • Common complications of SJS/TEN include:
    • Bacterial Infections leading to sepsis – more common in age>40, WBC>10,00, BSA more than or equal to 30 percent[2]
    • Opthalmologic – Ranging from pain, photophobia, conjuctivitis to keratitis and endopthalmitis. Appropriate treatment of acute ocular complications can prevent long term complications[3]
    • Pulmonary – Pnemonia, Interstitial pneumonitis, ARDS (25 percent of patients have been reported to require mechanical ventilation)[4]
    • Skin – Scarring or hypertrophic changes

Prognosis[5]

  • Prognosis and severity of SJS/TEN should be determined immediately after diagnosis to decide upon the appropriate medical management and setting.
  • SCORTEN Severity of illness score may be used to determine the severity and prognosis
SCORTEN SEVERITY OF ILLNESS SCORE[6]
SCORTEN Parameter Individual score SCORTEN (sum of individual scores) Predicted mortality (%)
Age > 40 years Yes = 1, No = 0 0-1 3.2
Malignancy Yes = 1, No = 0 2 12.1
Tachycardia (> 120/min) Yes = 1, No = 0 3 35.8
Initial surface of epidermal detachment >10% Yes = 1, No = 0 4 58.3
Serum urea >10 mmol/l Yes = 1, No = 0 >5 90
Serum glucose >14 mmol/l Yes = 1, No = 0
Bicarbonate >20 mmol/l Yes = 1, No = 0
  • Patients with SCORTEN score of 0-1 with limited skin involvement can be manged in non-specialized wards[7]
  • Patients with the SCORTEN score of 3 or more should be treated in an ICU.
  • Depending on the extent of the skin sloughing/ Body surface are involved at the time of diagnosis, the prognosis may vary. However, the prognosis is generally regarded as good
  • Mortality rate is 1-5 percent in SJS and in TEN is 25-35 percent[1]
  • Mortality rate can be higher in elderly and those with extensive skin involvement

Negative Prognostic Factors:

May include[8][9][10]:

References

  1. 1.0 1.1 Harr T, French LE (2010). “Toxic epidermal necrolysis and Stevens-Johnson syndrome”. Orphanet J Rare Dis. 5: 39. doi:10.1186/1750-1172-5-39. PMC 3018455. PMID 21162721.
  2. de Prost N, Ingen-Housz-Oro S, Duong Ta, Valeyrie-Allanore L, Legrand P, Wolkenstein P; et al. (2010). “Bacteremia in Stevens-Johnson syndrome and toxic epidermal necrolysis: epidemiology, risk factors, and predictive value of skin cultures”. Medicine (Baltimore). 89 (1): 28–36. doi:10.1097/MD.0b013e3181ca4290. PMID 20075702.
  3. Catt CJ, Hamilton GM, Fish J, Mireskandari K, Ali A (2016). “Ocular Manifestations of Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis in Children”. Am J Ophthalmol. 166: 68–75. doi:10.1016/j.ajo.2016.03.020. PMID 27018234.
  4. de Prost N, Mekontso-Dessap A, Valeyrie-Allanore L, Van Nhieu JT, Duong TA, Chosidow O; et al. (2014). “Acute respiratory failure in patients with toxic epidermal necrolysis: clinical features and factors associated with mechanical ventilation”. Crit Care Med. 42 (1): 118–28. doi:10.1097/CCM.0b013e31829eb94f. PMID 23989174.
  5. Harr T, French LE (2010). “Toxic epidermal necrolysis and Stevens-Johnson syndrome”. Orphanet J Rare Dis. 5: 39. doi:10.1186/1750-1172-5-39. PMC 3018455. PMID 21162721.
  6. Bastuji-Garin S, Fouchard N, Bertocchi M, Roujeau JC, Revuz J, Wolkenstein P (2000). “SCORTEN: a severity-of-illness score for toxic epidermal necrolysis”. J Invest Dermatol. 115 (2): 149–53. doi:10.1046/j.1523-1747.2000.00061.x. PMID 10951229.
  7. Valeyrie-Allanore L, Roujeau J-C. Epidermal necrolysis (Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis). In: Fitzpatrick’s Dermatology in General Medicine, 8th Edition, Goldsmith LA, Katz SI, Gilchrest BA, Paller AS. (Eds), Mcgraw-Hill, 2012.
  8. Schulz J, Sheridan RL, Ryan CM, et al. A 10-year experience with toxic epidermal necrolysis. J Burn Care Rehabil 2000. 21: 199-204
  9. Namdar T, von Wild T, Siemers F, et al. Does hypernatremia impact mortality in toxic epidermal necrolysis? Ger Med Sci 2010; 8:doc30
  10. Westly ED, Wechsler HL. Toxic epidermal necrolysis: granulocytic leucopenia as a prognostic indicator. Arch Dermatol 1984; 120:721-726

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Diagnosis

Diagnosis

Diagnostic Study of Choice | History and Symptoms | Physical Examination | Laboratory Findings | Electrocardiogram | X Ray | CT | MRI | Other Imaging Findings | Other Diagnostic Studies

Treatment

Treatment

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Case Studies

Case Studies

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