Pemphigus foliaceus

Pemphigus foliaceus
Pemphigus foliaceus
Specialty	Dermatology
Treatment	Typically treated with topical corticosteroids in mild cases. In more severe treatment it is treated similarly to pemphigus vulgaris.

Last updated February 29, 2024

Pemphigus foliaceus is an autoimmune blistering disease of the skin.^[1]Pemphigus foliaceus causes a characteristic inflammatory attack at the subcorneal layer of epidermis, which results in skin lesions that are scaly or crusted erosions with an erythematous (red) base.^[2] Mucosal involvement is absent even with widespread disease.^[3]

Steric hindrance of the desmoglein 1: The antibody caps off the site for intracellular binding to another keratinocyte.
Activation of an endocytic pathway: The antibody activates a pathway which causes an internalization of desmogleïn 1, which in turn causes a loss of adhesion.
Disruption of function: In this case, the antibody blocks the desmoglein 1 from being formed into a desmosome. This in turn causes a loss of adhesion with acantholysis as a result.

Cause

The National Institute of Arthritis and Musculoskeletal and Skin Diseases describes the disease thus:

Normally, our immune system produces antibodies that attack viruses and harmful bacteria to keep us healthy. In people with pemphigus, however, the immune system mistakenly attacks the cells in the epidermis, or top layer of the skin, and the mucous membranes. The immune system produces antibodies against proteins in the skin known as desmogleins. These proteins form the glue that keeps skin cells attached and the skin intact. When desmogleins are attacked, skin cells separate from each other and fluid can collect between the layers of skin, forming blisters that do not heal. In some cases, these blisters can cover a large area of skin.^[4]

Signs and symptoms

The characteristic lesions are crusted, scaly erosions on an erythematous base. In more localized and early disease, lesions are well demarcated and have seborrheic distribution (face, upper trunk, scalp). Small flaccid vesicles, unlike pemphigus vulgaris, are not found. The disease may develop slowly or may rapidly progress, resulting in an exfoliative erythroderma. UV radiation exacerbates pemphigus foliaceus. Patients experience burning and pain. The colloquial term for Brazilian endemic pemphigus, fogo selvagem (Portuguese for “wild fire”), takes into account many of the clinical aspects of this disease: the burning feeling of the skin, the exacerbation of disease by the sun, and the crusted lesions that make the patients appear as if they had been burned.^[5]^[6]

Diagnosis

Pemphigus foliaceus is diagnosed base on history, biopsy of the affected skin, and testing either a blood sample or a skin sample for the antibodies that cause pemphigus.^{[ citation needed ]}

The differential diagnosis includes other forms of pemphigus, bullous impetigo, subcorneal pustular dermatosis, subacute cutaneous LE, and seborrheic dermatitis. As discussed earlier, the demonstration of IgG autoantibodies against epidermal cell surfaces is essential for separating these disorders from the pemphigus family. A complete review of medications should be done to exclude the possibility of drug-induced pemphigus foliaceus. Because the lesions of pemphigus foliaceus may become secondarily infected, the finding of bacteria does not confirm a diagnosis of bullous impetigo. Likewise, a clinical flare or recalcitrant disease may represent a superimposed disorder, e.g. tinea corporis, especially in patients on systemic corticosteroids.^[6]

Treatment

Patients with this type of pemphigus do not necessarily require treatment with systemic therapy; the use of topical corticosteroids may suffice.^[5] When the disease is active and widespread, however, the therapy for pemphigus foliaceus is, in general, similar to that for pemphigus vulgaris. In general, immunosuppressive agents, such as azathioprine , mycophenolate mofetil and cyclophosphamide , when combined with corticosteroids, may result in gaining early control of the disease and an increased percentage of clinical remissions.^[6]

Epidemiology

The prevalence of pemphigus vulgaris and pemphigus foliaceus in men and women is approximately equal. The mean age of onset of disease is 50 to 60 years, although the range is broad and disease arising in the elderly and in children has been described. In most countries, pemphigus vulgaris is more common than pemphigus foliaceus; exceptions include Finland, Tunisia and Brazil. Patients with fogo selvagem (Brazilian endemic pemphigus) are clinically, histologically and immuno-pathologically similar to patients with sporadic pemphigus foliaceus. However, fogo selvagem occurs in an endemic fashion in certain regions of Brazil (especially along inland riverbeds)^[2] and is thought to be caused by an environmental factor(s).^[6]

History

Pierre Louis Alphée Cazenave first described the disease in 1844.^[7]

Related Research Articles

Psoriasis is a long-lasting, noncontagious autoimmune disease characterized by patches of abnormal skin. These areas are red, pink, or purple, dry, itchy, and scaly. Psoriasis varies in severity from small localized patches to complete body coverage. Injury to the skin can trigger psoriatic skin changes at that spot, which is known as the Koebner phenomenon.

A desmosome, also known as a macula adherens, is a cell structure specialized for cell-to-cell adhesion. A type of junctional complex, they are localized spot-like adhesions randomly arranged on the lateral sides of plasma membranes. Desmosomes are one of the stronger cell-to-cell adhesion types and are found in tissue that experience intense mechanical stress, such as cardiac muscle tissue, bladder tissue, gastrointestinal mucosa, and epithelia.

Pemphigus is a rare group of blistering autoimmune diseases that affect the skin and mucous membranes. The name is derived from the Greek root pemphix, meaning "blister".

Erythroderma is an inflammatory skin disease with redness and scaling that affects nearly the entire cutaneous surface. This term applies when 90% or more of the skin is affected.

Bullous pemphigoid is an autoimmune pruritic skin disease that typically occurs in people aged over 60, that may involve the formation of blisters (bullae) in the space between the epidermal and dermal skin layers. It is classified as a type II hypersensitivity reaction, which involves formation of anti-hemidesmosome antibodies, causing a loss of keratinocytes to basement membrane adhesion.

Nikolsky's sign is a clinical dermatological sign, named after Pyotr Nikolsky (1858–1940), a Russian physician who trained and worked in the Russian Empire. The sign is present when slight rubbing of the skin results in exfoliation of the outermost layer. A typical test would be to place the eraser of a pencil on the roof of a lesion and spin the pencil in a rolling motion between the thumb and forefinger. If the lesion is opened, then the Nikolsky's sign is present/positive.

Pemphigus vulgaris is a rare chronic blistering skin disease and the most common form of pemphigus. Pemphigus was derived from the Greek word pemphix, meaning blister. It is classified as a type II hypersensitivity reaction in which antibodies are formed against desmosomes, components of the skin that function to keep certain layers of skin bound to each other. As desmosomes are attacked, the layers of skin separate and the clinical picture resembles a blister. These blisters are due to acantholysis, or breaking apart of intercellular connections through an autoantibody-mediated response. Over time the condition inevitably progresses without treatment: lesions increase in size and distribution throughout the body, behaving physiologically like a severe burn.

The desmogleins are a family of desmosomal cadherins consisting of proteins DSG1, DSG2, DSG3, and DSG4. They play a role in the formation of desmosomes that join cells to one another.

Desmoglein-1 is a protein that in humans is encoded by the DSG1 gene. Desmoglein-1 is expressed everywhere in the skin epidermis, but mainly it is expressed in the superficial upper layers of the skin epidermis.

Desmoglein-3 is a protein that in humans is encoded by the DSG3 gene. In the skin epidermis Desmoglein-3 is expressed in the basal lower layers of the epidermis, and dominates in terms of expression on mucosal surfaces compared to Desmoglein-1.

Pemphigoid is a group of rare autoimmune blistering diseases of the skin, and mucous membranes. As its name indicates, pemphigoid is similar in general appearance to pemphigus, but, unlike pemphigus, pemphigoid does not feature acantholysis, a loss of connections between skin cells.

Desquamative gingivitis is an erythematous (red), desquamatous (shedding) and ulcerated appearance of the gums. It is a descriptive term and can be caused by several different disorders.

Gestational pemphigoid (GP) is a rare autoimmune variant of the skin disease bullous pemphigoid, and first appears in pregnancy. It presents with tense blisters, small bumps, hives and intense itching, usually starting around the navel before spreading to limbs in mid-pregnancy or shortly after delivery. The head, face and mouth are not usually affected.

Discoid lupus erythematosus is the most common type of chronic cutaneous lupus (CCLE), an autoimmune skin condition on the lupus erythematosus spectrum of illnesses. It presents with red, painful, inflamed and coin-shaped patches of skin with a scaly and crusty appearance, most often on the scalp, cheeks, and ears. Hair loss may occur if the lesions are on the scalp. The lesions can then develop severe scarring, and the centre areas may appear lighter in color with a rim darker than the normal skin. These lesions can last for years without treatment.

Paraneoplastic pemphigus (PNP) is an autoimmune disorder stemming from an underlying tumor. It is hypothesized that antigens associated with the tumor trigger an immune response resulting in blistering of the skin and mucous membranes.

Impetigo herpetiformis is a form of severe pustular psoriasis occurring in pregnancy which may occur during any trimester.

Bullous impetigo is a bacterial skin infection caused by Staphylococcus aureus that results in the formation of large blisters called bullae, usually in areas with skin folds like the armpit, groin, between the fingers or toes, beneath the breast, and between the buttocks. It accounts for 30% of cases of impetigo, the other 70% being non-bullous impetigo.

Autoimmune skin disease in dogs are a group of diseases that occur in dogs that are caused by the body's immune system, where the body's white blood cells or body's antibodies attack its own tissues or extracellular protein of the skin.

Cutaneous manifestations of COVID-19 are characteristic signs or symptoms of the Coronavirus disease 2019 that occur in the skin. The American Academy of Dermatology reports that skin lesions such as morbilliform, pernio, urticaria, macular erythema, vesicular purpura, papulosquamous purpura and retiform purpura are seen in people with COVID-19. Pernio-like lesions were more common in mild disease while retiform purpura was seen only in critically ill patients. The major dermatologic patterns identified in individuals with COVID-19 are urticarial rash, confluent erythematous/morbilliform rash, papulovesicular exanthem, chilbain-like acral pattern, livedo reticularis and purpuric "vasculitic" pattern. Chilblains and Multisystem inflammatory syndrome in children are also cutaneous manifestations of COVID-19.

References

↑ Motta, Adriana; González, Luis Fernando; García, Gonzalo; Guzmán, Jennifer; Prada, Lorena; Herrera, Hugo; Rolon, Mariam (2022). "10. Vesiculobullous Inflammatory Diseases". Atlas of Dermatology: Inflammatory, Infectious and Tumoral Skin Diseases. Springer. pp. 284–285. ISBN 978-3-030-84106-5.
1 2 Freedberg, et al. (2003). Fitzpatrick's Dermatology in General Medicine. (6th ed.). Page 558–562. McGraw-Hill. ISBN 0-07-138076-0.
↑ Rapini, Ronald P.; Bolognia, Jean L.; Jorizzo, Joseph L. (2007). Dermatology: 2-Volume Set. St. Louis: Mosby. ISBN 978-1-4160-2999-1.
↑ NIH Publication No. 15–7083 (June 2015). "Questions and Answers about Pemphigus". National Institute of Arthritis and Musculoskeletal and Skin Disease. NIH. Retrieved 23 October 2015.{{cite web}}: CS1 maint: numeric names: authors list (link)
1 2 Fitzpatrick's Dermatology in General Medicine (8th ed.). McGraw-Hill. 2012. p. 592. ISBN 978-0-07-171755-7.
1 2 3 4 Dermatology (4th ed.). Elsevier. 2018. p. 500. ISBN 978-0-7020-6275-9.
↑ Medscape Reference

External links

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[Mott2022-1] Motta, Adriana; González, Luis Fernando; García, Gonzalo; Guzmán, Jennifer; Prada, Lorena; Herrera, Hugo; Rolon, Mariam (2022). "10. Vesiculobullous Inflammatory Diseases". Atlas of Dermatology: Inflammatory, Infectious and Tumoral Skin Diseases. Springer. pp. 284–285. ISBN 978-3-030-84106-5.

[Fitz2-2] 1 2 Freedberg, et al. (2003). Fitzpatrick's Dermatology in General Medicine. (6th ed.). Page 558–562. McGraw-Hill. ISBN 0-07-138076-0.

[Bolognia-3] Rapini, Ronald P.; Bolognia, Jean L.; Jorizzo, Joseph L. (2007). Dermatology: 2-Volume Set. St. Louis: Mosby. ISBN 978-1-4160-2999-1.

[4] NIH Publication No. 15–7083 (June 2015). "Questions and Answers about Pemphigus". National Institute of Arthritis and Musculoskeletal and Skin Disease. NIH. Retrieved 23 October 2015.{{cite web}}: CS1 maint: numeric names: authors list (link)

[:0-5] 1 2 Fitzpatrick's Dermatology in General Medicine (8th ed.). McGraw-Hill. 2012. p. 592. ISBN 978-0-07-171755-7.

[:1-6] 1 2 3 4 Dermatology (4th ed.). Elsevier. 2018. p. 500. ISBN 978-0-7020-6275-9.

[7] Medscape Reference

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Classification	D ICD-10 : L10.2 DiseasesDB : 31179
External resources	Orphanet : 79481