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AUTHOR AND EDITOR INFORMATION

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Author: Lawrence Chan, MD, Department Head and Director of Skin Immunology Research, Professor, Departments of Dermatology and Microbiology/Immunology, University of Illinois College of Medicine

Lawrence Chan is a member of the following medical societies: Alpha Omega Alpha, American Academy of Dermatology, American Medical Association, American Society for Investigative Pathology, Federation of American Society of Experimental Biology, Illinois State Medical Society, and Society for Investigative Dermatology

Editors: Smeena Khan, MD, Private Practice, Adult and Pediatric Dermatology Associates; Richard P Vinson, MD, Assistant Clinical Professor, Department of Dermatology, Texas Tech University School of Medicine; Consulting Staff, Mountain View Dermatology, PA; Jeffrey Meffert, MD, Assistant Clinical Professor of Dermatology, Medicine, University of Texas Health Science Center-San Antonio; Catherine Quirk, MD, Clinical Assistant Professor, Department of Dermatology, Brown University; William D James, MD, Paul R Gross Professor of Dermatology, University of Pennsylvania School of Medicine; Vice-Chair, Program Director, Department of Dermatology, University of Pennsylvania Health System

Author and Editor Disclosure

Synonyms and related keywords: herpetiform pemphigus

INTRODUCTION

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Background

Pemphigus herpetiformis is a clinical variant of pemphigus that combines the clinical features of dermatitis herpetiformis with the immunopathologic features of pemphigus. Previously, pemphigus was described using various terms, including herpetiform pemphigus, acantholytic herpetiform dermatitis, pemphigus controlled by sulfapyridine, and mixed bullous disease. Because pemphigus herpetiformis is a clinical variant of pemphigus, it may be more appropriately described with a term that begins with the general group term (pemphigus), followed by a term for the variant subset (herpetiformis), similar to the terms for other pemphigus variants, such as pemphigus vulgaris, pemphigus foliaceus, pemphigus vegetans, and pemphigus erythematosus.

Pathophysiology

Pemphigus herpetiformis appears to be mediated by the immunoglobulin G (IgG) class of autoantibodies that target the skin epidermis desmoglein components. Most patients demonstrate autoantibodies to desmoglein 1, a desmosomal component predominantly located in the upper epidermis, while a minority of patients demonstrates autoantibodies to desmoglein 3, which is predominantly located in the lower epidermis. The ability of desmoglein 3 to induce an experimental model of pemphigus after transfer of splenocytes from desmoglein 3-immunized desmoglein 3-knockout mice to Rag-2 immunodeficient mice further supports the role of desmogleins as autoantigens. Histologically demonstrated eosinophil and/or neutrophil infiltration into the epidermis may be relevant pathogenically in the disease process.

In the neutrophil-dominant subset, epidermal cells secrete a neutrophil chemokine interleukin 8 (IL-8), which apparently is induced by IgG autoantibodies to desmoglein and may be responsible for the recruitment of neutrophils to the epidermis, resulting in the subsequent blistering process.

Frequency

United States

Pemphigus herpetiformis is a rare clinical variant of pemphigus. Frequency of occurrence remains undetermined.

International

Although frequency of occurrence is not determined, pemphigus herpetiformis has been reported in Europe, Japan, and the United States. In a large study conducted in Eastern Europe, 15 patients (7.3%) with pemphigus herpetiformis were found among 205 patients with pemphigus. In a smaller study conducted in Italy, 5 patients with pemphigus herpetiformis were found among 84 patients with pemphigus. Therefore, pemphigus herpetiformis accounts for approximately 6-7% of pemphigus in European populations.

Mortality/Morbidity

Pemphigus herpetiformis is not associated with significant mortality; however, the disease is associated with significant pruritus. Treatment regimens for the disease may cause significant adverse effects that must be monitored closely by the patient's physicians. Severe pruritus is noted in approximately one half of patients affected with pemphigus herpetiformis. At least 2 cases of pemphigus herpetiformis have been reported to occur in association with lung cancer. Whether this association was coincidental is not clear.

Race

Because pemphigus herpetiformis is rare, ethnic distribution is not determined yet. Because the disease occurs in the United States, Europe, and Asia, it does not appear to have a specific ethnic predominance.

Sex

Because pemphigus herpetiformis is rare, sex distribution has yet to be defined clearly. Studies in the literature do not appear to support a sex predilection.

Age

The age of onset for pemphigus herpetiformis ranges from 30-80 years, with a mean age of onset of 60 years.


CLINICAL

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History

Patients affected with pemphigus herpetiformis usually have a subacute onset of disease. Approximately one half of patients experience severe pruritus.

Physical

  • Patients affected with pemphigus herpetiformis usually present with erythematous, vesicular, bullous, or papular lesions.

  • Lesions often demonstrate a "herpetiform" pattern, which is manifested as a cluster of blisters on an inflammatory base.

  • Mucous membrane involvement is observed only occasionally. Oral erosion has been reported as a rare finding.

  • Occasionally, lesions resemble those found in dermatitis herpetiformis, bullous pemphigoid, linear IgA bullous dermatosis, pemphigus foliaceus, pemphigus erythematosus, or pemphigus vulgaris.

Causes

  • Pemphigus herpetiformis appears to be mediated by IgG autoantibodies targeting the interepidermal cell adhesion molecules desmoglein 1 or desmoglein 3. However, unlike typical pemphigus vulgaris, significant numbers of inflammatory cells, eosinophils, neutrophils, or mixed eosinophils and neutrophils infiltrate pemphigus herpetiformis lesional skin. The roles of inflammatory cells, particularly eosinophils, in the pathogenesis of pemphigus herpetiformis require further investigation.
  • Etiology in the neutrophil-dominant subset of pemphigus herpetiformis includes the following:
    • In a study of 2 patients, IgG autoantibodies that recognized desmoglein 1 (a predominant upper-epidermal protein) exclusively were found to co-localize with expression of IL-8 (a strong neutrophil chemokine) and neutrophilic infiltration at the upper epidermis of the patients' skin.
    • In the study of 2 patients, the purified IgG fraction of the patients' sera induced IL-8 secretion from normal cultured human keratinocytes. Purified IgG from one of these patients also induced the cytoplasmic expression of IL-8 in normal cultured human keratinocytes.
    • Thus, in the neutrophil-dominant subset of pemphigus herpetiformis, it seems that IgG autoantibodies targeting desmoglein 1 were responsible for neutrophil recruitment to the epidermis as a result of inducing epidermal-cell IL-8 expression and secretion. Once at the epidermis, infiltrating neutrophils may result in blisters by releasing their proteases.

  • In the eosinophil-dominant subset of pemphigus herpetiformis, eosinophilic involvement has not been investigated yet.
  • One report of a patient with pemphigus herpetiformis has been associated with use of medication (thiopronine). A detailed mechanism is not delineated.
  • One patient with pemphigus herpetiformis had a history of psoriasis and developed the pemphigus disease shortly after a course of ultraviolet light treatment, raising a possible role of ultraviolet light in the induction of pemphigus herpetiformis.
  • At least 2 reported patients with pemphigus herpetiformis had coexisting psoriasis, a chronic inflammatory dermatosis, raising a possible role of "epitope spreading" in the induction of pemphigus herpetiformis.


DIFFERENTIALS

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Bullous Pemphigoid
Dermatitis Herpetiformis
Pemphigus Erythematosus
Pemphigus Foliaceus
Pemphigus Vulgaris

Other Problems to be Considered

Linear immunoglobulin A bullous dermatosis


WORKUP

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Lab Studies

  • To establish a diagnosis of pemphigus herpetiformis, perform the following tests: histopathology on newly blistered skin, direct immunofluorescence (DIF) on periblistered skin, and indirect immunofluorescence (IIF) of the patient's sera on monkey esophagus substrate.

  • Histopathology: Histopathology documents the acantholytic process and inflammatory cell infiltration (eosinophils, neutrophils, or both) that characterize the disease.

  • Direct immunofluorescence
    • DIF documents the immunologic nature of the disease.

    • DIF usually detects the presence of IgG with or without C3 deposition around cell surfaces of keratinocytes in the patient's skin. The optimal location for the skin biopsy used in this study is adjacent to a blister or an inflammatory papule.

  • Indirect immunofluorescence
    • IIF confirms the presence in the patient's serum of IgG-circulating autoantibodies that bind to epidermal cell surfaces.

    • In some patients, IgG autoantibodies predominantly bind to the upper part of the epidermis; in other patients, IgG autoantibodies bind to the entire epidermis.

    • The titer of autoantibodies often parallels the clinical level of activity of the disease and often is helpful in following the patient's disease activity after the diagnosis has been established.

Imaging Studies

  • Patients who have associated pulmonary symptoms should undergo routine chest radiography. CT scanning may also be needed.

Other Tests

  • Immunoblotting
    • Immunoblotting documents specific skin desmosomal components, in a denatured form, that are recognized by the patient's IgG autoantibodies.

    • Most patients with pemphigus herpetiformis have IgG autoantibodies that recognize desmoglein 1, a desmosomal protein predominantly located in the upper epidermis.

    • In a minority of patients with pemphigus herpetiformis, IgG autoantibodies were detected to desmoglein 3, a desmosomal protein predominantly located in the lower epidermis.

  • Enzyme-linked immunosorbent assay
    • Similar to immunoblotting, enzyme-linked immunosorbent assay (ELISA) detects the specific protein component (usually in recombinant nondenatured form) recognized by the patient's IgG autoantibodies.

    • ELISA usually is more sensitive than immunoblotting in detecting the protein recognized by autoantibodies.

  • Immunoprecipitation: Immunoprecipitation has the same function as immunoblotting but is more difficult to perform. Immunoprecipitation detects the native form of the target antigen rather than the denatured form of the antigen.


TREATMENT

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Medical Care

Pemphigus herpetiformis is responsive to anti-inflammatory and immunosuppressive medications. Dapsone is the drug of choice if the patient tolerates the treatment.

Activity

No specific activity restrictions are indicated; however, advise patients to avoid injury during the active disease period.


MEDICATION

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Because pemphigus herpetiformis is a rare variant of pemphigus, comprehensive therapeutic studies of large numbers of patients have not taken place. The following treatment options are taken from the personal experiences of physician-investigators with a small number of patients.

In general, dapsone is the drug of choice. Other anti-inflammatory and immunosuppressive medications are also effective.

Drug Category: Anti-inflammatories

Since pemphigus herpetiformis lesions are characterized by prominent infiltration of inflammatory cells, anti-inflammatory medication may inhibit the functions of these cells, therefore improving disease conditions.

Drug NameDapsone (Avlosulfon)
DescriptionMechanism of action is similar to that of sulfonamides, in which competitive antagonists of PABA prevent formation of folic acid, inhibiting bacterial growth. Used alone or in conjunction with other anti-inflammatory medication or immunosuppressives for pemphigus herpetiformis.
Adult Dose100 mg PO qd or 50 mg PO bid
Pediatric Dose>10 years: 25-50 mg/d PO single dose or 25-50 mg/d PO bid; consult pediatrician before prescribing
ContraindicationsAbsolute: Documented hypersensitivity
Relative: G-6-PD deficiency (especially in African Americans, persons of Middle Eastern heritage, Asians), significant cardiopulmonary disease, significant hematologic disease, sulfa allergy (cautious use may be attempted; cross-reactivity is relatively rare and mild)
InteractionsTrimethoprim, probenecid, and folic acid antagonists (eg, pyrimethamine, methotrexate) increase levels; activated charcoal, PABA, and rifampin decrease levels; may increase hemolysis with sulfonamides and hydroxychloroquine
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsPerform weekly CBC counts (first mo), then perform CBC counts monthly (6 mo), then semiannually; discontinue if significant reduction in platelets, leukocytes, or hematopoiesis is seen; methemoglobin reductase deficiency, G-6-PD deficiency, or hemoglobin M because of high risk for hemolysis and Heinz body formation; patients exposed to other agents or conditions (eg, infection, diabetic ketosis) capable of producing hemolysis; peripheral neuropathy can occur (rare); phototoxicity may occur when exposed to UV light

Drug NameSulfapyridine
DescriptionSulfa drug with similar function to dapsone in controlling pemphigus herpetiformis. Competitive antagonist of PABA.
Adult Dose500 mg PO bid; increase by 1 g q 1-2 wk until disease is controlled; control may require 1-4 g/d
Pediatric Dose35 mg/kg PO bid, not to exceed 100 mg/kg/d; consult pediatrician before prescribing
ContraindicationsDocumented hypersensitivity; slow acetylators may require smaller doses or more gradual initial dosage adjustment
InteractionsBioavailability of digoxin is reduced by sulfapyridine; recommended interval of 2-3 h between administrations
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsIdiosyncratic reactions (eg, hypersensitivity pneumonitis, a lupuslike syndrome, pancreatitis, toxic hepatitis) may occur; agranulocytosis occurs rarely; immune and nonimmune hemolytic anemia develop; nonimmune hemolytic anemia is more common in G-6-PD–deficient patients; folate deficiency may occur secondary to impaired absorption; nephrolithiasis may occur as with other sulfa drugs; toxic epidermal necrolysis has been reported with medications containing sulfa groups; check CBC and LFT monthly for 5 mo, then q6wk thereafter

Drug NamePrednisone (Deltasone)
DescriptionImmunosuppressant for treatment of autoimmune disorders; may decrease inflammation by reversing increased capillary permeability and suppressing PMN activity. Stabilizes lysosomal membranes and also suppresses lymphocytes and antibody production. Taken alone, or in conjunction with other anti-inflammatory or immunosuppressive medications, is useful for controlling pemphigus herpetiformis.
Adult Dose20-60 mg PO qam; taper over 2-4 wk as symptoms resolve; alternatively, 0.5-2 mg/kg/d; taper as condition improves; single morning dose is safer for long-term use, but divided doses have more anti-inflammatory effect
Pediatric Dose4-5 mg/m2/d PO, or 0.05-2 mg/kg PO; taper over 2 wk as symptoms resolve; consult pediatrician before prescribing
ContraindicationsAbsolute: Systemic fungal infection, herpes simplex keratitis, hypersensitivity (usually with corticotropin, occasionally with IV forms)
Relative: Hypertension, active TB, CHF, prior psychosis, positive purified protein derivative test result, glaucoma, severe depression, diabetes mellitus, active peptic ulcer disease, cataracts, osteoporosis, recent bowel anastomosis, pregnancy
InteractionsIncreased levels occur with ketoconazole, erythromycin, clarithromycin, estrogens, and birth control pills; decreased levels occur with aminoglutethimide, phenytoin, phenobarbital, rifampin, cholestyramine, and ephedrine; levels of potassium-depleting diuretics (potentiates potassium loss and digitalis toxicity) and cyclosporine increase; levels of isoniazid, insulin (resistance is induced), and salicylates decrease; monitor anticoagulant therapy and theophylline levels
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsUse lower dose in hypothyroidism, liver disease, and obesity (decreased cortisol-binding globulin [CBG] and increased free fraction of steroid); pregnancy, hyperthyroidism, and concurrent estrogen therapy may increase CBG levels; abrupt discontinuation of glucocorticoids may cause adrenal crisis; hyperglycemia, edema, osteonecrosis, myopathy, peptic ulcer disease, hypokalemia, osteoporosis, euphoria, psychosis, myasthenia gravis, growth suppression, and infections may occur with glucocorticoid use; alternate-day therapy does not prevent bone loss (appropriate monitoring and prophylaxis for osteoporosis continues to evolve)

Drug Category: Immunosuppressives

Pemphigus herpetiformis is an autoimmune disease; immunosuppressives are useful in suppressing autoimmune response.

Drug NameAzathioprine (Imuran)
DescriptionAntagonizes purine metabolism and inhibits synthesis of DNA, RNA, and proteins. May decrease proliferation of immune cells, which results in lower autoimmune activity. Usually used as supplement to anti-inflammatory medication; is useful in controlling pemphigus herpetiformis.
Adult Dose1 mg/kg qd/bid (empiric) or by TPMT level; increase by 0.5 mg/kg q4wk until response, not to exceed 2.5 mg/kg/d
TPMT testing not entirely reliable; involves testing activity of TPMT activity in RBCs, which correlates with systemic TPMT activity; functional enzyme test has been shown to have variability between test sites, and kits may contain varying amounts of enzyme inhibitor; starting at low doses, monitoring for pancytopenia, then increasing the dose is an alternative; if clinical response is not good, patient may be a homozygote for high activity and may need increased dose; Wolverton does not recommend using this assay (Wolverton, Comprehensive Dermatologic Drug Therapy); some references recommend checking before treatment in all patients
TPMT <5 U: No treatment with azathioprine
TPMT 5-13.7 U: Not to exceed 0.5 mg/kg
TPMT 13.7-19 U: Not to exceed 1.5 mg/kg
TPMT >19 U: Not to exceed 2.5 mg/kg
Pediatric DoseSafety and efficacy not established
ContraindicationsAbsolute: Documented hypersensitivity, pregnancy or attempting pregnancy, clinically significant active infection
Relative: Concurrent use of allopurinol; prior treatment with alkylating agents (eg, cyclophosphamide, chlorambucil, melphalan, others [high risk of neoplasia])
InteractionsAllopurinol increases risk of pancytopenia; captopril/ACE inhibitors may increase risk of anemia and leukopenia; warfarin dose may need to be increased; pancuronium dose may need to be increased for adequate paralysis; live virus vaccines and cotrimoxazole increase risk of hematologic toxicity; rifampicin may cause transplants to possibly be rejected; clozapine may increase risk of agranulocytosis
PregnancyD - Unsafe in pregnancy
PrecautionsIncreased risk of neoplasia; caution in liver disease and renal impairment; hematologic toxicities may occur; rarely, patients may develop fever without associated infections; measure thiopurine methyltransferase level prior to treatment; periodically monitor CBC count and liver function


FOLLOW-UP

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Further Inpatient Care

  • The disease activities of pemphigus herpetiformis rarely require hospitalization. In a few patients, short-term hospitalization (<10 d) may be helpful.

Further Outpatient Care

  • The disease activities of pemphigus herpetiformis range from mild to moderate.

  • During the active disease period, provide follow-up care for patients on a monthly outpatient basis. These visits ensure that (1) patients are responding clinically to prescribed medications and (2) patients experience no serious adverse effects that require a change of medications.

  • Typically, follow-up visits are not needed for patients in clinical remission and not on treatment.

Deterrence/Prevention

  • For patients who are treated with systemic corticosteroid for longer than one month, a combined calcium and Vitamin D supplements should be instituted to prevent osteoporosis. The dosage and frequency of these supplements are stated in the 1996 recommendations established by the American College of Rheumatology Task Force.

Prognosis

  • The prognosis for pemphigus herpetiformis usually is excellent.


MISCELLANEOUS

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Medical/Legal Pitfalls

  • Failure to monitor patients receiving treatment with dapsone, since adverse effects may be severe

  • Failure to examine early signs of neuropathy, which is essential in patients receiving treatment with dapsone because of potential adverse effects

  • Failure to regularly obtain CBC counts, which is important in patients receiving treatment with dapsone to monitor potential adverse effects

  • Failure to investigate potential lung cancer associated with the disease when the patient has pulmonary symptoms


MULTIMEDIA

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Media file 1:  Histopathologic examination of a blister lesion obtained from a patient with pemphigus herpetiformis shows a subcorneal blistering process, acantholysis, and neutrophilic infiltrate.
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Media type:  Photo

Media file 2:  Direct immunofluorescence microscopy performed on a skin biopsy specimen obtained from a patient with pemphigus herpetiformis detects immunoglobulin G deposits on the epithelial cell surfaces but sparing the basal layers.
Click to see larger pictureClick to see detailView Full Size Image
Media type:  Photo


REFERENCES

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Pemphigus Herpetiformis excerpt

Article Last Updated: Sep 8, 2006