Pemphigus Explained

Pemphigus (or) is a rare group of blistering autoimmune diseases that affect the skin and mucous membranes.[1] The name is derived from the Greek root pemphix, meaning "blister".[2]

In pemphigus, autoantibodies form against desmoglein, which forms the "glue" that attaches adjacent epidermal cells via attachment points called desmosomes. When autoantibodies attack desmogleins, the cells become separated from each other and the epidermis becomes detached, a phenomenon called acantholysis. This causes blisters that slough off and turn into sores. In some cases, these blisters can cover a large area of the skin.[3]

Originally, the cause of this disease was unknown, and "pemphigus" was used to refer to any blistering disease of the skin and mucosa. In 1964, researchers found that the blood of patients with pemphigus contained antibodies to the layers of skin that separate to form the blisters.[4] [5] In 1971, an article investigating the autoimmune nature of this disease was published.[6] [7]

Types

The several types of pemphigus (pemphigus vulgaris, pemphigus foliaceus, intraepidermal neutrophilic IgA dermatosis, and paraneoplastic pemphigus) vary in severity. Skin lesions caused by pemphigus can lead to fatal infections, so treatment is extremely important.

Hailey-Hailey disease, also called familial benign pemphigus, is an inherited skin disease, not an autoimmune disease, so it is not considered part of the pemphigus group of diseases.[12]

Diagnosis

Pemphigus defines a group of autoimmune intraepithelial blistering diseases that are characterized by loss of normal cell-cell adhesion (acantholysis), and by the presence of pathogenic (predominantly IgG) autoantibodies reacting against epithelial adhesion molecules.[10] Pemphigus is further divided in two major subtypes: pemphigus vulgaris (PV) and pemphigus foliaceus (PF). However, several other disorders such as IgA pemphigus, IgE pemphigus, pemphigus herpetiformis, drug-induced pemphigus, Senear Usher syndrome, and endemic pemphigus foliaceus exist, and are recognized by a dermatologist from the appearance and distribution of the skin lesions. It is also commonly diagnosed by specialists practicing otolaryngology- head and neck surgery, periodontists, oral and maxillofacial surgeons, and eye doctors, as lesions can affect the eyes and mucous membranes of the oral cavity. Intraorally, it resembles the more common diseases lichen planus and mucous membrane pemphigoid.[13] Definitive diagnosis requires examination of a skin or mucous membrane biopsy by a dermatopathologist or oral pathologist. The skin biopsy is taken from the edge of a blister, prepared for histopathology and examined with a microscope. The pathologist looks for an intraepidermal vesicle caused by the breaking apart of epidermal cells (acantholysis). Thus, the superficial (upper) portion of the epidermis sloughs off, leaving the bottom layer of cells on the "floor" of the blister. This bottom layer of cells is said to have a "tombstone" appearance.

Definitive diagnosis also requires the demonstration of antidesmoglein autoantibodies by direct immunofluorescence on the skin biopsy. These antibodies appear as IgG deposits along the desmosomes between epidermal cells, a pattern reminiscent of chicken wire. Antidesmoglein antibodies can also be detected in a blood sample using the ELISA technique.

Classification

Pemphigus is a group of autoimmune blistering diseases that may be classified into these types:

Treatment

If not treated, pemphigus can be fatal, usually from overwhelming opportunistic infection of lesions. The most common treatment is the administration of oral steroids, especially prednisone, often in high doses. The side effects of corticosteroids may require the use of so-called steroid-sparing or adjuvant drugs. One of the most dangerous side effects of high-dosage steroid treatments is intestinal perforations, which may lead to sepsis. Steroids and other medications being taken to treat pemphigus may also mask the effects of the perforations. Patients on high dosages of oral steroids should closely monitor their gastrointestinal health. As lesions are usually terribly painful, pain medication[14] likely complicates and exacerbates the gastrointestinal issues caused by steroids.

Treatment options

All of these drugs may cause severe side effects, so patients should be closely monitored by doctors. Once the outbreaks are under control, dosage is often reduced, to lessen side effects.

A meta-analysis of the literature found insufficient evidence to determine the optimal treatment regimen for pemphigus vulgaris and pemphigus foliaceus, but it found that adding cyclophosphamid and azathioprine to a glucocorticoid regimen reduced the amount of glucocorticoid needed for treatment, and topical epidermal growth factor significantly reduced lesion healing time.[19]

If skin lesions do become infected, antibiotics may be prescribed. Tetracycline antibiotics have a mildly beneficial effect on the disease and are sometimes enough for pemphigus foliaceus. In addition, talcum powder is helpful to prevent oozing sores from adhering to bedsheets and clothes. Wound care and treatments are often akin to those used in burn units, including careful use of dressings that don't stick to the wounds, etc.

If paraneoplastic pemphigus is diagnosed with pulmonary disease, a powerful cocktail of immunosuppressant drugs is sometimes used in an attempt to halt the rapid progression of bronchiolitis obliterans, including methylprednisolone, ciclosporin, azathioprine, and thalidomide. Plasmapheresis may also be useful.

Animals affected

Pemphigus foliaceus has been recognized in pet dogs, cats, and horses, and is the most common autoimmune skin disease diagnosed in veterinary medicine. PF in animals produces clusters of small vesicles that quickly evolve into pustules. Pustules may rupture, forming erosions or become crusted. Left untreated, PF in animals is life-threatening, leading to not only loss of condition, but also secondary infection.

PV is a very rare disorder described in pet dogs and cats. Paraneoplastic pemphigus has been identified in pet dogs.

See also

External links

Notes and References

  1. Yeh SW, Ahmed B, Sami N, Ahmed AR . Blistering disorders: diagnosis and treatment. Dermatologic Therapy. 16. 3. 214–23. 2003. 14510878. 10.1046/j.1529-8019.2003.01631.x. free.
  2. Web site: Definition of PEMPHIGUS. www.merriam-webster.com. en. 2017-03-11.
  3. http://pemphigus.org/index.php?option=com_content&view=article&id=364&Itemid=100073/ International Pemphigus & Pemphigoid Foundation: What is Pemphigus?
  4. Beutner. EH. Jordon. RE. Demonstration of skin antibodies in sera of pemphigus vulgaris patients by indirect immunofluorescent staining. Proceedings of the Society for Experimental Biology and Medicine. November 1964. 117. 2. 505–510. 14233481. 10.3181/00379727-117-29622. 9443044.
  5. Web site: Dermatology Foundation: BEUTNER, JORDAN SHARE 2000 DERMATOLOGY FOUNDATION DISCOVERY AWARD . 2009-01-31 . https://web.archive.org/web/20080518082952/http://www.dermfnd.org/press01/beutner.html . 2008-05-18 . dead .
  6. 10.1111/1523-1747.ep12293273. Robert E. Jordon. Ernst H. Beutner. Robert E.. Jordon. W. Mitchell. Sams Jr.. Gustavo. Diaz. Ernst H.. Beutner. Negative Complement Immunofluorescence in Pemphigus. Journal of Investigative Dermatology. 1971. 57. 6. 407–410. 4108416. free.
  7. Serratos. BD. Rashid, RM. Nail disease in pemphigus vulgaris. Dermatology Online Journal. Jul 15, 2009. 15. 7. 2. 10.5070/D34X05D6VH . 19903430.
  8. Sampaio SA et al . Brazilian pemphigus foliaceus, endemic pemphigus foliaceus, or fogo selvagem (wild fire). Dermatologic Clinics. 12. 4. 765–776. 1994. 10.1016/S0733-8635(18)30140-2. 7805306.
  9. Saleh MA . Pemphigus in the Arab world. The Journal of Dermatology. 42. 1. 27–30. 2015. 25558949. 10.1111/1346-8138.12676. 5126848. free.
  10. 10.7241/ourd.20134.158 . Autoimmune epidermal blistering diseases . 2013 . Abreu Velez . Ana Maria . Calle . Juliana . Howard . Michael S. . Our Dermatology Online . 4 . 631–646 . free .
  11. 10.1067/s0190-9622(03)00851-x . A unique form of endemic pemphigus in northern Colombia . 2003 . Abrèu-Velez . Ana María . Hashimoto . Takashi . Bollag . Wendy B. . Tobón Arroyave . Sergio . Abrèu-Velez . Clara Eugenia . Londoño . Martha Luz . Montoya . Fernando . Beutner . Ernst H. . Journal of the American Academy of Dermatology . 49 . 4 . 599–608 . 14512903 .
  12. Web site: Hailey Hailey Disease Society . 2008-03-04 . https://web.archive.org/web/20121014124508/http://haileyhailey.com/WhatIsHHD.htm . 2012-10-14 . dead .
  13. Book: Sapp. J. Philip. Eversole. Lewis R.. Wysocki. George P.. Contemporary Oral and Maxillofacial Pathology. 1997. Mosby. 978-0-8016-6918-7. also here
  14. Rashid. RM. Candido, KD. Pemphigus pain: a review on management. The Clinical Journal of Pain. Oct 2008. 24. 8. 734–5. 18806540. 10.1097/AJP.0b013e31817af6fc. 21201391.
  15. http://www.bad.org.uk/public/leaflets/bad_patient_information_gateway_leaflets/pemphigus/treated/steroid.asp British Association of Dermtologists, Steroid sparing (or adjuvant) drugs
  16. Ahmed AR, Spigelman Z, Cavacini LA, Posner MR . Treatment of pemphigus vulgaris with rituximab and intravenous immune globulin. New England Journal of Medicine. 355. 17. 1772–9. 2006. 17065638. 10.1056/NEJMoa062930 . free.
  17. Joly P, Mouquet H, Roujeau JC, etal . A single cycle of rituximab for the treatment of severe pemphigus. New England Journal of Medicine. 357. 6. 545–52. 2007. 17687130. 10.1056/NEJMoa067752. free.
  18. Murrell DF et al . Diagnosis and management of pemphigus: Recommendations of an international panel of experts. Journal of the American Academy of Dermatology. 82. 3. 575–585. 2020. 29438767. 10.1016/j.jaad.2018.02.021. 7313440.
  19. Martin. Linda K. Agero. Anna Liza. Werth. Victoria. Villanueva. Elmer. Segall. Janet. Murrell. Dedee F. 2009-01-21. Interventions for pemphigus vulgaris and pemphigus foliaceus. Cochrane Database of Systematic Reviews. 1. CD006263. en. 10.1002/14651858.CD006263.pub2. 19160272. 34912494 . 1465-1858.