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AUTHOR AND EDITOR INFORMATION

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Author: Warren R Heymann, MD, Head, Division of Dermatology, Professor, Department of Internal Medicine, University of Medicine and Dentistry of New Jersey

Warren R Heymann is a member of the following medical societies: American Academy of Dermatology, American Society of Dermatopathology, and Society for Investigative Dermatology

Coauthor(s): Kathleen M Rossy, MD, Staff Physician, Department of Dermatology, New York Medical College, Metropolitan Hospital

Editors: Robert A Schwartz, MD, MPH, Professor and Head of Dermatology, Professor of Medicine, Professor of Pediatrics, Professor of Pathology, Professor of Preventive Medicine and Community Health, UMDNJ-New Jersey Medical School; Michael J Wells, MD, Associate Professor, Department of Dermatology, Texas Tech University Health Sciences Center; Paul Krusinski, MD, Director of Dermatology, Professor, Department of Internal Medicine, Fletcher Allen Health Care, University of Vermont; 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: AAE, Caldwell syndrome, acquired angioedema

INTRODUCTION

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Background

Acquired angioedema (AAE) is characterized by painless, nonpruritic, nonpitting swelling of the skin that is classified into 2 forms: acquired angioedema type I (AAE-I) and acquired angioedema type II (AAE-II). AAE-I is associated with other diseases, most commonly B-cell lymphoproliferative disorders. AAE-II is an autoimmune process defined by the presence of an autoantibody directed against the C1 inhibitor molecule (C1-INH).

Pathophysiology

The gene for C1-INH (SERPING1) has been mapped to chromosome 11 (11q12-q13.1). C1-INH is a multifunctional serine protease inhibitor that is normally present in high concentrations in plasma. It is the only plasma inhibitor of C1r and C1s, the activated proteases of the first component of complement. It is also the major plasma inhibitor of activated Hageman factor, the first protease in the contact system. Additionally, C1-INH is one of the major inhibitors of plasma kallikrein, the contact system protease that cleaves kininogen and releases bradykinin.

Presumably, uncontrolled activation of the contact system allows for release of kininlike mediators, resulting in vascular permeability with edema of subcutaneous and mucosal tissues. Although the issue of which vasoactive peptide is ultimately responsible for these changes remain controversial, direct evidence supports the importance of bradykinin in the clinical manifestations of angioedema. Other kinins may also be pathogenic. The specific trigger responsible for inducing the release of these vasoactive peptides is unclear. Factor XII activation (Hageman factor) may be secondary to phospholipid release from damaged or apoptotic cells and may be important in the generation of bradykinin from endothelial activation. This hypothesis encompasses the role of illness or tissue injury in the generation of bradykinin. The precise pathophysiology of AAE-I remains to be defined. Diminished levels of C1-INH are due to its increased catabolism.

In AAE-I, the associated disorders (usually lymphoproliferative malignancies) produce complement-activating factors, idiotype/anti-idiotype antibodies, or other immune complexes that destroy C1-INH function. Neoplastic lymphatic tissue has been found to play an active role in the consumption of C1-INH and the complement components of the classic pathway. The most commonly associated malignancy, B-cell lymphoma, has shown that anti-idiotypic antibody attached to immunoglobulin on the surface of B-cells causes C1-INH deficiency. Increased consumption of C1q followed by C2 and C4 results in subsequent release of vasoactive peptides that act on postcapillary venules.

In AAE-II, a normal 105-kd C1-INH molecule is synthesized in adequate amounts, but, because of an unknown event, a subpopulation of B cells secretes autoantibodies to the C1-INH molecule. This autoantibody, which may be any of the major immunoglobulin classes, binds to the reactive center of C1-INH. After binding to C1-INH and altering its structure, its regulatory capacity is diminished or abrogated.

In all reported cases of C1-INH deficiency caused by an autoantibody, C1-INH circulates in the blood in a form that has been cleaved by target proteases from its native molecule to a 95-kd fragment. Because of the higher affinity of the autoantibody for native C1-INH, the 95-kd antibody/C1-INH complex dissociates, and the freed antibody can bind to another native C1-INH molecule, allowing for the further depletion of C1-INH.

The distinction between AAE-I and AAE-II may be difficult to make at times and it is imperative to stress that overlap does occur. For instance, cases of monoclonal gammopathy of undetermined significance ( MGUS) have shown the monoclonal immunoglobulin itself to be the C1-INH antibody. Regarding malignancies and/or other diseases associated with AAE-I, it has been demonstrated that these patients may initially present with autoantibodies to C1-INH, or they may develop as the disease progresses.

Frequency

International

AAE is rare, with approximately 150 cases reported in the medical literature worldwide.

Mortality/Morbidity

Although mortality may occur because of laryngeal edema, it is more likely due to the complications of the associated disorder.

Race

Presumably, all races are affected.

Sex

Men and women may be affected.

Age

The onset of AAE is most common after the fourth decade of life, whereas the onset of hereditary acquired angioedema (HAE) is in the second decade.


CLINICAL

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History

  • A family history for hereditary angioedema is not obtained, which distinguishes AAE from HAE.

  • Regarding angioedema, symptoms are referable to 3 prominent sites: subcutaneous tissues (eg, face, hands, arms, legs, genitals, buttocks); abdominal organs (eg, stomach, intestines, bladder), which may manifest as nausea, vomiting, and/or colicky pain and mimic a surgical emergency; and the upper airway (eg, larynx), which may result in laryngeal edema.

  • Occasionally, patients may experience heat and pain in the affected areas.

  • Other symptoms may be related to underlying disorders, such as lymphoproliferative malignancies or connective tissue disease.

Physical

  • Physical signs include overt, noninflammatory swelling of the skin and mucous membranes.

  • Although urticaria does not usually occur, occasionally, erythema or mild urticarial eruptions may precede the edema.

Causes

AAE-I is most frequently associated with B-cell lymphoproliferative disease. To date, only 2 reports of a T-cell lymphoma associated with AAE-I have been documented. Other disorders have included multiple myeloma, chronic lymphocytic leukemia, myelofibrosis, Waldenström macroglobulinemia, non-Hodgkin lymphoma, MGUS, rectal carcinoma, essential cryoglobulinemia, erythrocyte sensitization, livedo reticularis, cold urticaria, lupus anticoagulant, and infection with Helicobacter pylori or Echinococcus granulosis. By definition, AAE-II is not associated with any specific disorder but rather by the presence of the autoantibody directed against C1-INH. However, the occasional existence of features of both AAE-I and AAE-II has been noted, most notably with a MGUS.

One case of AAE with C1-INH deficiency state was identified in association with liver transplantation. The status of the liver donor was unknown, but it is speculated that the donor may have been C1-INH deficient.

Another case of AAE was reported with acute upper airway angioedema in association with the local anesthetic articaine.


DIFFERENTIALS

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Angioedema, Hereditary
Drug Eruptions
Urticaria, Acute
Urticaria, Cholinergic
Urticaria, Chronic
Urticaria, Contact Syndrome
Urticaria, Dermographism
Urticaria, Solar
Urticarial Vasculitis

Other Problems to be Considered

ACE inhibitor–induced angioedema
Episodic angioedema with angioedema
Leukocytoclastic vasculitis
Urticaria, cold


WORKUP

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Lab Studies

  • AAE-I and AAE-II
    • Low C1-INH levels

    • Low C1q levels (except 1 reported case)

    • Low C4 levels

    • Low C2 levels

  • AAE-II - Positive immunoblot assay findings for 95-kd C1-INH cleavage product

Imaging Studies

  • Abdominal radiographs may demonstrate features of ileus. Other findings may be referable to an associated illness.

Other Tests

  • Other laboratory findings are related to associated illnesses.

Histologic Findings

Histologic features include reticular dermal, subcutaneous, or submucosal edema without infiltrating inflammatory cells. Vasodilation may be seen.


TREATMENT

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Medical Care

  • Depending on the symptoms and the site of the angioedema, intensive support may be necessary, including intravenous fluids.

  • When possible, the underlying disorder should be treated. The resolution of angioedema has been reported with the treatment of underlying disease, although recurrences have occurred despite appropriate treatment of the disorder.

  • In AAE-I, treatment of the associated lymphoproliferative process may result in correction of the abnormality.

Surgical Care

Intubation may be necessary in cases of laryngeal edema.


MEDICATION

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In AAE, therapy for acute attacks may be aborted with C1-INH concentrates or, if unavailable, fresh-frozen plasma. However, rapid catabolism of C1-INH occurs in AAE, so higher doses of C1-INH plasma concentrate may be needed.

Androgens, such as danazol or stanozolol, may be beneficial in AAE-I but are of no value in AAE-II. Prostate cancer and pregnancy preclude the use of androgens.

Antifibrinolytics, such as epsilon-aminocaproic acid and tranexamic acid, have been found to be more effective for long-term prophylaxis in those with AAE.

Immunosuppressive therapy directed toward decreasing autoantibody production may be of value in patients with AAE-II, which may be accomplished by the use of plasmapheresis with cyclophosphamide.

A recent paper reported effective treatment of 3 severe AAE cases with a series of 4 weekly injections with rituximab (a chimeric monoclonal antibody to CD 20). After treatment with rituximab, normalization of C1-INH and C4 levels and long-term remission of angioedema attacks was achieved.

New medications are currently being studied for the treatment of AAE. One such treatment is a synthetic kallikrein inhibitor (DX-88), which is thought to be able to stop the generation of bradykinin by inhibiting kallikrein activation. This drug allows for a decrease in the rate of C1-INH catabolism, allowing for C1-INH concentrate to be more effective.

Other new products in trial are genetically engineered C1 esterase inhibitor and bradykinin B2 receptor antagonist.

Drug Category: Alkylating agents

Some agents in this class have potent immunosuppressive activity.

Drug NameCyclophosphamide (Cytoxan, Neosar)
DescriptionChemically related to nitrogen mustards. As an alkylating agent, the mechanism of action of the active metabolites may involve cross-linking of DNA, which may interfere with growth of normal and neoplastic cells.
Adult Dose500-750 mg/m2
Pediatric DoseAdminister as in adults
ContraindicationsDocumented hypersensitivity; severely depressed bone marrow function
InteractionsAllopurinol may increase risk of bleeding or infection and enhance myelosuppressive effects; may potentiate doxorubicin-induced cardiotoxicity; may reduce digoxin serum levels and antimicrobial effects of quinolones; chloramphenicol may increase half-life while decreasing metabolite concentrations; may increase effect of anticoagulants; coadministration with high doses of phenobarbital may increase rate of metabolism and leukopenic activity; thiazide diuretics may prolong cyclophosphamide-induced leukopenia and neuromuscular blockade by inhibiting cholinesterase activity
PregnancyD - Unsafe in pregnancy
PrecautionsRegularly examine hematologic profile (particularly neutrophils and platelets) to monitor for hematopoietic suppression; regularly examine urine for RBCs, which may precede hemorrhagic cystitis; hematologic myelosuppression, primarily leukopenia, is most common adverse effect; thrombocytopenia and anemia occur less frequently; gastrointestinal adverse effects include anorexia, nausea, emesis, and stomatitis; urologic adverse effects include dysuria, urgency, hematuria, bladder fibrosis, and necrosis; death from hemorrhagic cystitis has occurred; encourage excessive fluid intake; interferes with oogenesis and spermatogenesis; may cause irreversible sterility in both sexes

Drug Category: Antifibrinolytic agents

Act through the inhibition of plasmin.

Drug NameAminocaproic acid (Amicar)
DescriptionLysine analog that inhibits fibrinolysis via inhibition of plasminogen activator substances; to a lesser degree, through antiplasmin activity.
Widely distributed. Half-life is 1-2 h. Peak effect occurs within 2 h. Hepatic metabolism is minimal. Can be used PO/IV.
Adult Dose8 g q4h IV, then 16 g/d in acute attacks
6-10 g/d PO maintenance
Pediatric Dose8-10 g/d PO
Not recommended in newborns
ContraindicationsDocumented hypersensitivity; evidence of active intravascular clotting process; coadministration with factor IX complex concentrates or anti-inhibitor coagulant complexes; injection in premature neonates (injectable product contains benzyl alcohol)
InteractionsCoadministration with estrogens may cause increase in clotting factors, leading to a hypercoagulable state; coadministration with tretinoin my increase risk of both venous and arterial thrombosis
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsDo not administer unless a definite diagnosis of hyperfibrinolysis has been made; caution in cardiac, hepatic or renal disease; because aminocaproic acid can be fatal in patients with DIC, important to differentiate between hyperfibrinolysis and DIC; thrombi that form during treatment are not lysed and effectiveness is uncertain; associated adverse effects are postural hypotension, thrombosis, and muscular pain and weakness; monitor CK levels; caution in patients with upper urinary tract bleeding; caution with rapid infusions; do not administer with factor IX complex concentrates or anti-inhibitor coagulant complexes; adverse effects include bradyarrhythmia, drug-induced myopathy, and hypotension

Drug NameTranexamic acid (Cyklokapron)
DescriptionAlternative to aminocaproic acid. Inhibits fibrinolysis by displacing plasminogen from fibrin.
Adult DoseUp to 8 g PO/IV for acute attacks
1-2 g PO for maintenance
3-4.5 g PO/IV qd divided tid/qid pc; continue for period long enough for at least 3-4 attacks to have normally occurred
Pediatric Dose12-25 mg/kg/dose (not to exceed 1.5 g) PO tid/qid for acute attack or as prophylaxis for 5 d
ContraindicationsDocumented hypersensitivity; active intravascular clotting process; acquired defective color vision; subarachnoid hemorrhage
InteractionsNot established
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsCaution in renal impairment; adverse effects are not common but include headaches, nausea, abdominal pain, and diarrhea; evidence of tumor formation in retina and liver found in experimental animal models after long-term use; although no evidence has supported these findings in humans, annual funduscopic examinations and LFT monitoring recommended q6mo if on long-term therapy; perform baseline ophthalmologic examination before initiating therapy; caution in history of thromboembolic disease and disseminated intravascular coagulation

Drug Category: Antigonadotropic agents

These agents have immunosuppressive properties.

Drug NameDanazol (Danocrine)
DescriptionIncreases levels of C4 component of complement and prevents attacks associated with angioedema.
Adult Dose200 mg PO bid/tid initially; if efficacious, taper dose by 50% over following 2-3 mo
Pediatric DoseNot established
ContraindicationsDocumented hypersensitivity; seizure disorders; renal or hepatic insufficiency; cardiac disease; breastfeeding; conditions influenced by edema; undiagnosed genital bleeding; porphyria; carcinoma of the breast
InteractionsDecreases insulin requirements and increases effects of anticoagulants; concomitant administration with carbamazepine may result in toxicity; coadministration with HMG-CoA reductase inhibitors may increase risk for rhabdomyolysis; cyclosporine and/or tacrolimus toxicity may increase if coadministered with danazol; concomitant use with carbamazepine may increase risk of carbamazepine toxicity; concomitant administration with cyclosporine or tacrolimus and anabolic steroids may result in increased cyclosporine or tacrolimus blood levels and toxicity; may result in increased lovastatin plasma concentrations when administered concurrently (use only if potential benefit justifies potential risk of developing myopathy/rhabdomyolysis)
PregnancyX - Contraindicated in pregnancy
PrecautionsCaution in renal, hepatic, or cardiac insufficiency and seizure disorders; peliosis hepatitis and benign hepatic adenoma have been observed with long-term therapy; thromboembolic events and pseudotumor cerebri reported; androgenlike effects, including weight gain, acne, hirsutism, edema, hair loss, voice change, and menstrual disturbances, occur; temporary alteration of lipoproteins may occur; consider the impact on the risk of atherosclerosis and coronary artery disease; serum total testosterone values may be falsely elevated if radioimmunoassay done to measure testosterone in women taking danazol

Drug NameStanozolol (Winstrol)
DescriptionSynthetic androgen with immunosuppressive properties. Increases levels of C1 esterase inhibitor and C4 component of the complement.
Adult Dose2 mg PO tid and reduce to maintenance dose of 2 mg/d or 2 mg qod after 1-3 mo
Pediatric Dose<6 years: 1 mg/d PO
6-12 years: 2 mg/d PO
>12 years: Administer as in adults
ContraindicationsDocumented hypersensitivity; nephrosis; breast or prostate cancer
InteractionsIncreases hypoprothrombinemic effects of oral anticoagulants and hypoglycemic effects of insulin and sulfonylureas
PregnancyX - Contraindicated in pregnancy
PrecautionsMay cause peliosis hepatitis, liver cell tumors, and blood lipid changes with increased risk of arteriosclerosis; caution in cardiac, renal, or hepatic disease or epilepsy; adverse effects include cholestatic jaundice syndrome and/or hepatic necrosis (causing death); may cause premature epiphyseal closure in children; caution in diabetic patients and pediatric patients; may cause suppression of clotting factors II, V, VII, and X and an increase in prothrombin time


FOLLOW-UP

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Prognosis

  • The prognosis is variable, but it predominantly depends on control of the underlying disorder.

  • Compared with the general population, patients with AAE have a higher incidence of B-cell malignancies.

  • Patients with AAE and a concurrent diagnosis of MGUS do not have an increased risk for progression to malignancy compared with patients with a sole diagnosis of MGUS.

Patient Education


MISCELLANEOUS

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Special Concerns

  • Tranexamic acid may be used during pregnancy.


REFERENCES

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Angioedema, Acquired excerpt

Article Last Updated: May 21, 2007