Hypersensitivities, Drug Eruptions, Vasculitides, and Miscellaneous Inflammatory Disorders



Hypersensitivities, Drug Eruptions, Vasculitides, and Miscellaneous Inflammatory Disorders


Cathleen K. Case

Kelli Turgeon-Daoust






I. OVERVIEW

There are two opposite sides to immunity: host protection and injury. The immune response to an antigen is designed to protect the host. Disorders of the immune system include hypersensitivity, autoimmunity, and immunodeficiency. These response mechanisms produce a wide range of clinical conditions from local reactions to lifethreatening diseases. The primary biological effects of the immune response are the humoral (antibody) and cellular recognition and elimination of infectious agents and other foreign antigens. If there is re-exposure to the same antigen in a previously sensitized individual, there may be an exaggerated or “hypersensitivity” reaction. This is a misdirected immune response that results in local tissue injury or systemic manifestations, which may include shock and death. Immune responses that result in tissue injury or other pathophysiologic changes are called allergic/immunopathologic (hypersensitivity) reactions. There are four types of hypersensitivity reactions.

A. Causes of tissue injury

1. Release of vasoactive substances; primary and secondary mediators

2. Phagocytosis or lysis of cells

3. Activation of components of the complement system

4. Release of proteolytic enzymes, cytokines, and other mediators of tissue injury and inflammation from recruited inflammatory cells









TABLE 18-1 Four Types of Hypersensitivity Reaction






































Type


Mediators


Mechanism


Response Time


Appearance


Associated Conditions


Type I (immediate, anaphylactic)


IgE, histamine, tryptase, and leukotrienes


IgE, produced in excessive amounts, interacts with mast cells to cause release of histamine and other vasoactive mediators of hypersensitivity


Usually 15-30 min; may have delayed onset of 10-12 h


Wheal and flare


Anaphylaxis, asthma, urticaria, and angioedema


Type II (cytotoxic)


IgM or IgG, complement


Antibody is bound to antigen on cell surface, triggering complement activation, cell lysis, and cytotoxicity


Minutes to hours


Lysis and necrosis


Transfusion reaction, some drug reactions, and druginduced pemphigus


Type III (immune complex)


Immune complex IgG or IgM


Antigen-antibody immune complexes are deposited in tissue, activating mast cells, neutrophils, and phagocytes and triggering complement cascade


3-10 h


Erythema and edema, and necrosis


Serum sickness, Arthus reaction, vasculitis, and systemic lupus erythematosus


Type IV (delayed/cell mediated)


Antigen-specific T cells, monocyte chemotactic factor, interleukin-2, interferon-gamma, TNF-alpha, and TNF-beta


Activated antigen-specific helper T cells stimulate release of cytokines and chemokines, which attract and activate macrophages, eosinophils, and neutrophils; cytotoxic T cells cause damage directly


1-3 d; up to 4 wk for some reactions


Erythema and induration


Allergic contact dermatitis, tuberculin reaction, granuloma formation secondary to infection and foreign antigens (tuberculosis, leprosy), and fixed drug eruption


B. Hypersensitivity reactions, their mediators, and associated conditions (Table 18-1)

This chapter focuses on urticaria, angioedema, and anaphylaxis, certain drug reactions, cutaneous small-vessel vasculitis (CSVV), and other hypersensitivity syndromes, including:

1. Erythema multiforme (EM)

2. Stevens-Johnson syndrome (SJS)

3. Toxic epidermal necrolysis (TEN)

4. Erythema nodosum (EN)

5. Pyoderma gangrenosum (PG)


URTICARIA, ANGIOEDEMA, AND ANAPHYLAXIS


I. OVERVIEW

Approximately 1 in 5 people will experience urticaria. Urticaria may be more common in atopic individuals and is usually classified as acute or chronic; however, the majority of cases are acute lasting from hours to a few weeks. Chronic urticaria is defined as episodes of urticaria lasting for more than 6 weeks; however, all urticaria begins in an acute phase. Occasionally, acute urticaria is associated with deeper less well-demarcated edema referred to as angioedema.

Allergic angioedema can be associated with anaphylaxis including life-threatening bronchoconstriction and hypotension. The eyelids and lips are most typically affected by angioedema. The cause of acute urticaria may be identified and generally self-limiting; the cause of chronic urticaria may be determined in only 5% to 20% of cases.

A. Definition

1. Urticaria, also called hives or wheals, is a common and distinctive cutaneous reaction pattern involving the superficial dermis. It is usually transient, demonstrating localized edema caused by dilatation and increased permeability of the capillaries and marked by the development of wheals. A wheal or hive is a welldemarcated, erythematous or white, nonpitting, edematous papule or plaque that is usually pruritic. The lesions are polymorphous and often form annular, arciform, or polycyclic plaques (Figures 18-1 and 18-2). The lesions change shape and size during the few hours or days they are present. Urticaria can be acute or chronic, and the physical urticarias depend on an external or exogenous factor. Chronic urticaria is defined as episodes of urticaria lasting for more than 6 weeks; however, all urticaria begins in an acute phase.

2. Angioedema (angioneurotic edema) is a hive-like swelling caused by increased vascular permeability in the subcutaneous tissue of the skin and mucosa and submucosal layers of the respiratory and gastrointestinal (GI) tracts. Hives and angioedema can occur simultaneously and may have the same etiology. Angioedema is usually located on the eyes, as seen in Figure 18-3, and mouth (Figure 18-4) but may also occur on the hands and feet or in the throat. Laryngeal edema does not usually occur with urticaria or simple angioedema. There are multiple syndromes of angioedema including idiopathic, allergic, and medication-induced angioedema; hereditary angioedema (HAE); and acquired angioedema (AAE). The presence or absence of hives is used to characterize the different syndromes of angioedema.

3. Anaphylaxis is a severe, potentially fatal, systemic allergic reaction that occurs suddenly after contact with an allergy-causing substance.







FIGURE 18-1. Large edematous plaques of urticaria. (From Elder, D. E. (2012). Atlas and synopsis of Lever’s histopathology of the skin. Philadelphia, PA: Wolters Kluwer.)

B. Etiology

1. Urticaria

a. Most cases of acute urticaria are IgE-mediated type I hypersensitivity reactions. Circulating antigens such as foods, drugs, or inhalants react with cell membrane-bound IgE to release histamine. IgE antigen on the mast cell surface unites with the antigen of food, drug, stinging insect venom, or pollen and causes an immediate and large release of histamine and other vasoactive mediators from mast cells.

b. Complement-mediated acute urticaria may be caused by administration of whole blood, plasma, immunoglobulins, and drugs or by insect stings. Type III hypersensitivity reactions occur with deposition of insoluble immune complexes in vessel walls (Arthus reactions). The complexes are composed of IgG or IgM, the trapped complexes activate complement, and the process releases histamine from mast cells. A frequent reason for acute urticaria is viral infections of the upper respiratory tract, which increases mast cell reactivity.






FIGURE 18-2. Typical hives of different sizes. (From Anderson, M. K. (2012). Foundations of athletic training. Philadelphia, PA: Wolters Kluwer.)






FIGURE 18-3. Urticaria with angioedema around the eyes. (From Goodheart, H. P. (2003). Goodheart’s photoguide of common skin disorders (2nd ed.). Philadelphia, PA: Lippincott Williams & Wilkins.)

c. Nonimmunologic release of histamine occurs when pharmacologic mediators, such as acetylcholine, opiates, polymyxin B, or strawberries, react directly with
cell membrane-bound mediators to release histamine. Aspirin and other nonsteroidal anti-inflammatory drugs (NSAIDs) can cause nonimmunologic release of histamine; these patients may have a history of allergic rhinitis or asthma. The physical urticarias may be induced by both direct stimulation of cell membrane receptors and immunologic mechanisms.






FIGURE 18-4. Angioedema of the lip, tense swelling of the dermis and subcutaneous tissue. (Neville, B., Damm, D., White, D., & Waldron, W. (1991). Color atlas of clinical oral pathology. Philadelphia, PA: Lea & Febiger. Used with permission.)

d. Patients with history of hives lasting more than 6 weeks may be classified as having chronic urticaria. The lesional morphology is similar to acute hives, any skin surface can be affected, and the lesions last less than 24 hours. Angioedema occurs in 50% of cases of chronic urticaria. Chronic urticaria patients are likely to exhibit physical urticaria, is usually nonallergic, and is usually idiopathic. Angioedema associated with chronic urticaria is different from HAE in that it rarely affects the larynx. Table 18-2 displays the clinical classification of urticaria/angioedema.

e. A partial list of the etiologic classification of urticaria is found in Table 18-3.

2. Angioedema

a. Most cases of angioedema are idiopathic. Angioedema will often occur with hives, and angioedema without wheals is seen with drug reactions and C1 inhibitor deficiency.

b. Severe allergic type I immediate hypersensitivity IgE-mediated reactions can cause acute angioedema. Angioedema can occur with other symptoms of anaphylaxis including hypotension and respiratory distress.

c. Drugs such as contrast dyes, NSAIDs, aspirin, indomethacin, and ACE inhibitors can cause angioedema with nonimmunologic mechanism.

d. AAE results from an acquired C1 inhibitor deficiency considered to be an autoimmune disease. HAE is an inherited C1 inhibitor deficiency and results from lack of the functional C1 esterase inhibitor.

3. Anaphylaxis

a. Immediate-type hypersensitivity reactions may occur locally or systemically causing mild symptoms or sudden death from anaphylactic shock. Food allergies, including allergy to tree nuts and peanuts, and crustaceans are common causes of serious anaphylactic reactions. Other common causes include antibiotics, especially penicillins; other drugs and chemicals, including radiographic contrast agents; and hymenoptera stings.








TABLE 18-2 Clinical Classification of Urticaria















Clinical Class


Duration


Ordinary urticaria (acute and chronic)


3-36 h


Physical urticaria


Adrenergic (stress)


Aquagenic


Cholinergic


Cold


Delayed pressure


Dermatographism


Exercise-induced urticaria (anaphylaxis)


Solar


Vibratory angioedema


30 min to 2 h except delayed pressure urticaria that may last longer than 2 h


Contact urticaria


1-2 h









TABLE 18-3 Etiologic Classification of Urticaria










































Etiology


Examples


Food


Fish, shellfish, nuts, eggs, strawberries, cow’s milk, wheat, and yeast


Food additives


Salicylates, benzoates, penicillin, and sulfites


Drugs


Penicillin, aspirin, sulfonamides, and drugs that cause a nonimmunologic release of histamine (morphine, codeine, dextran, polymyxin, curare, quinine)


Infections


Chronic bacterial infections (sinus, dental, urinary tract), fungal infections, viral infections (hepatitis B prodrome, infectious mononucleosis, coxsackie), intestinal worms, and malaria


Inhalants


Pollens, mold spores, animal dander, house dust, and aerosols


Internal disease


Systemic lupus erythematosus, hyperthyroidism, autoimmune thyroid disease, carcinomas, lymphomas, leukocytoclastic vasculitis, polycythemia vera, rheumatic fever, and transfusion reaction


Physical stimuli (physical urticarias)


Listed in Table 18-4


Nonimmunologic contact urticaria


Plants (nettles), animals (caterpillars, jellyfish), and medications (cinnamic aldehyde, dimethyl sulfoxide)


Uncertain mechanism


Ammonium persulfate used in hair bleach, chemicals, foods, textiles, wood, saliva, cosmetics, perfumes, and bacitracin


Skin diseases


Mastocytosis, dermatitis herpetiformis, pemphigoid, and amyloidosis


Hormones


Pregnancy and premenstrual flare (progesterone)


Genetic


Hereditary angioedema, familial cold urticaria, and vibratory urticaria


C. Incidence

1. Estimates of the lifetime occurrence of urticaria range from less than 1% to as high as 30% of the population. Hives can occur at any age, is a worldwide disease, and may be more common in atopic patients.

2. Angioedema frequently occurs with acute urticaria, which is more common in children and young adults. Chronic urticaria is more common in women in the third to fifth decades of life; there is no consensus on the prevalence of chronic urticaria.

3. Most cases of angioedema are idiopathic. It can occur at any age but is most common in the 40- to 50-yearold age group, women being more affected than men. Angiotensin-converting enzyme inhibitors (ACEIs) are the number one drug cause of acute angioedema; the incidence may be higher in Black Americans. HAE affects between 1 in 10,000 and 1 in 50,000 persons and begins in late childhood or early adolescence.

4. True incidence of anaphylaxis is unknown; lifetime prevalence is 1% to 2% for the population as a whole.


D. Pathologic processes

1. There are several types of stimuli that cause urticaria, which include immunologic, nonimmunologic, physical, and chemical. Several are listed in Table 18-3.

2. The mast cell is the primary effector cell in urticaria. Release of mast cell mediators causes inflammation and mast cell degranulation that results in the release of histamine and inflammatory mediators, as well as an accumulation and activation of other cells including eosinophils, neutrophils, and, possibly, basophils. Histamine causes endothelial cell contraction that allows vascular fluid to leak between the cells through vessel walls, causing tissue edema and wheal formation.

3. When histamine is injected into the skin, there is vasodilation causing local erythema, a peripheral flare characterized by erythema beyond the border of local erythema (axon reflex), and a wheal produced by leakage of fluid from the postcapillary venules.

4. Angioedema is a hive-like swelling in the subcutaneous tissue of skin, mucosa, and submucosal layers of the respiratory and GI tracts. The reaction is similar to that of urticaria in the upper dermis. Hives and urticaria may have the same etiology and often occur simultaneously.

5. Anaphylaxis can be mediated by immunologic (IgEmediated and non-IgE-mediated [e.g., IgG and immune complex complement-mediated]) and nonimmunologic factors, which include events resulting in sudden mast cell and basophil degranulation in the absence of immunoglobulins.

E. Considerations across the life span

1. Urticaria, angioedema, and anaphylaxis can occur at any age.


II. ASSESSMENT

The diagnosis of urticaria is often one of exclusion. It is essential to rule out the presence of serious illnesses of which recurring hives and/or edema can be a symptom. Examples of such illnesses may include hepatitis, hyperthyroidism, lymphomas, lupus, and cancers of the rectum, kidneys, and GI tract.

A. History and physical examination

1. History and physical exams are the most important parts of the initial evaluation and should include an evaluation of the following factors.

a. Association with any specific substance or activity: drug ingestion or exposure; respiratory infection; food and drink; exposure to pollens and chemicals; physical location of work, travel, hobby, or home; and medications, supplements, or homeopathic compounds.

b. Appropriate description of the character of the primary lesion in urticaria is important, usually an edematous and erythematous papule or plaque.

c. Location of the lesions—itchy lesions that come and go, located anywhere on the skin.

d. Length of response—individual hives do not usually last for more than 24 hours. Note time of onset, appearance, day, year, and season. Duration of individual lesions: less than 1 hour, physical urticaria and typical hives; less than 24 hours, typical hives; longer than 25 hours, and that burn or resolve with purpura require a biopsy to exclude urticarial vasculitis.

e. Assessment of previous incidence of symptoms related to common causes of urticaria. Table 18-3 lists possible causes. Drugs are common causes in adults, and viral respiratory or streptococcal infections are common causes in children.

f. Evaluation of recent exposure to possible allergens.

g. Assessment of common subtypes of urticaria (Table 18-2).

h. Evaluate the role that occupation can play in establishing the diagnosis of urticaria.

i. Differentiation of angioedema from urticaria is of utmost importance related to the life-threatening possibilities associated with angioedema. Urticarial lesions are superficial and widespread, while lesions associated with angioedema are deep, and the eyelids and lips are the areas most typically affected. Urticaria and angioedema frequently occur at the same time. Any patient with recurrent angioedema or abdominal pain without wheals should be evaluated for HAE.

j. Evaluate for physical urticaria by stroking the arm with a tongue blade to test for dermatographism. This may indicate one of the physical urticarias.

k. Anaphylaxis almost always involves the skin and/or mucous membranes with a combination of erythema, urticaria, angioedema, or pruritus. Adults will present with cutaneous and respiratory symptoms and children may show more respiratory symptoms.

B. Skin findings

1. A wheal or hive is a well-demarcated, erythematous or white, nonpitting, edematous papule or plaque that is usually pruritic. The lesions of urticaria change shape and size during the few hours or days they are present. The central area (wheal) can be pale compared to the surrounding erythematous area (flare). Wheals are sharply marginated and predominantly flat topped. Their color varies from light pink to dark red depending on the amount of fluid present between the skin surface and the underlying dilated vascular bed. Wheals frequently have a dimpled surface because of the anchoring effect of hair follicles as fluid fills the papillary dermis surrounding them. The physical urticarias have unique characteristics and are outlined in Table 18-4.

a. The evolution of urticaria is dynamic and lesions are transient.

b. Hives result from local capillary vasodilation and dermal edema; the edema is in the superficial dermis.

c. Lesions vary in size from 2 to 4 mm seen in cholinergic urticaria up to a giant hive that may cover an entire extremity.

d. Lesions will be round, oval, polycyclic, or incomplete rings. Color may be solid red or white, or white in center with red border. Purpura within individual lesions may indicate urticarial vasculitis.









TABLE 18-4 The Physical Urticarias











































































Urticaria


Relative Frequency


Precipitant


Local Symptoms


Systemic Symptoms


Symptomatic dermatographism


Most frequent


Stroking skin


Irregular, pruritic wheals


None


Delayed dermatographism


Rare


Stroking skin


Burning, deep swelling


None


Pressure urticaria


Frequent


Pressure


Diffuse, tender swelling


Flulike symptoms


Solar urticaria


Frequent


Various light wavelengths


Pruritic wheals


Wheezing, dizziness, and syncope


Familial cold urticaria


Rare


Change in skin temperature from cold air


Burning wheals


Tremor, headache, arthralgia, and fever


Essential cold urticaria


Frequent


Cold contact


Pruritic wheals


Wheezing and syncope


Heat urticaria


Rare


Heat contact


Pruritic wheals


None


Cholinergic urticaria


Very frequent


General overheating of the body


Papular, pruritic wheals


Syncope, diarrhea, vomiting, salivation, and headaches


Aquagenic urticaria


Rare


Water contact


Papular, pruritic wheals


None reported


Vibratory angioedema


Very rare


Vibrating against skin


Angioedema


None reported


Exercise-induced anaphylaxis


Rare


Exercise; in some cases, ingestion of certain foods


Pruritic wheals


Respiratory distress and hypotension


e. Thicker plaques with fluid in dermis and subcutaneous tissue are considered angioedema.

f. Hives are generally ITCHY; however, intensity may vary.

g. Purpura within a wheal may indicate urticarial vasculitis and will need biopsy.

2. The reaction of angioedema is deeper than wheals and produces more diffuse swelling. The swelling is painful and burning but not pruritic.

a. Lips, palms, soles, trunk, limbs, and genitalia are commonly affected.

b. There may be involvement of respiratory or GI tracts producing dyspnea, dysphagia, abdominal pain, and diarrhea.

c. Angioedema may develop as a result of trauma.

3. The physiologic responses to the release of anaphylaxis mediators include smooth muscle spasm in the respiratory and GI tracts, vasodilation, increased vascular permeability, and stimulation of sensory nerve endings.

a. These physiologic events lead to some or all of the classic symptoms of anaphylaxis: flushing; urticaria/angioedema; pruritus; bronchospasm; laryngeal edema; abdominal cramping with nausea, vomiting, and diarrhea; and feeling of impending doom.

C. Differential diagnosis

1. Urticarial stage of bullous pemphigoid

2. Dermatitis herpetiformis

3. Drug eruptions

4. Erythema multiforme

5. Papular urticaria

6. Polymorphic eruption of pregnancy

7. Urticaria pigmentosa

8. Urticarial vasculitis

D. Diagnostic tests

1. Complete blood count (CBC) with differential.

2. Liver and thyroid function tests.

3. Urine analysis.

4. Erythrocyte sedimentation rate (ESR).

5. If the history provides evidence that warrants additional tests, consider test for hepatitis A, B, and C; infectious mononucleosis; thyroid antibodies; and antinuclear antibody (ANA).

6. Biopsy for urticarial lesions with purpuric center or for lesions that last for more than 36 hours to evaluate for urticarial vasculitis. Also, biopsy if there is fever, arthralgia, elevated ESR, or petechiae.

7. Sinus x-rays may be considered for evaluation of chronic urticaria if there is a corresponding history.

8. If HAE is suspected, C4 level can be a screening test.


III. COMMON THERAPEUTIC MODALITIES

A. Systemic therapy for urticaria and associated angioedema

1. First-line therapy is (nonsedating) second-generation H1 antagonists to inhibit mast cell mediators.

a. Cetirizine 10 mg nightly or twice daily

b. Loratadine 10 mg daily or twice daily

c. Fexofenadine 120 to 180 mg daily

2. First-line therapy may include first-generation H1 (sedating) antihistamines and/or H2 receptor antagonists if symptoms are not controlled after a week or two of treatment.

a. Diphenhydramine 10 to 25 mg four times daily.

b. Hydroxyzine HCl 10 to 25 mg four times daily.

c. Doxepin 10 to 25 mg nightly.

d. H2 receptor antagonists include cimetidine 400 mg twice daily, ranitidine 150 mg twice daily, or famotidine 20 mg twice daily.

3. Second-line therapy may include systemic corticosteroid.

a. Prednisone 0.5 to 1 mg/kg daily for short course may provide relief for severe cases.

4. Third-line therapy may include leukotriene receptor agonists and can be combined with antihistamines.

a. Montelukast 10 mg daily

b. Zafirlukast 20 mg twice daily

c. Zileuton 600 mg four times a day


5. Treatment of choice for angioedema associated with anaphylaxis is epinephrine given intramuscularly (IM) (1:1,000 solution) when intravenous is not available. Diphenhydramine 50 mg can also be given IM. The IM route is better and more quickly absorbed than subcutaneous.

B. Nonpharmacologic interventions

1. Identify and eliminate underlying cause.

a. Avoid common triggers such as aspirin, NSAIDs, food additives, heat, and alcohol.

b. Whether urticaria is acute or chronic, consider stopping vitamins, laxatives, antacids, toothpaste, cigarettes, cosmetics and all toiletries, chewing gum, household cleaning solutions, and aerosols.

c. Chronic hives are not caused by food allergies; however, some individuals find that hives are worsened after eating certain foods. Consider stopping fruits, tomatoes, nuts, eggs, shellfish, chocolate, milk, cheese, bread, diet drinks, and junk food.

2. Avoid eliciting stimuli.

a. Take cool showers or baths, apply cool compresses (except with cold urticaria), wear loose fitting clothes, and avoid strenuous activity.

b. Swimming in cold water is the most common cause of severe cold urticaria reaction. Patients should be advised never to jump into a cold body of water, and water activities should be done under supervision.

c. Strategies to reduce stress can be helpful.

C. Medication therapy monitoring

1. The role of pharmacotherapy is symptom management, and control of pruritus is critical in helping patients find relief.

2. Antihistamine therapy usually starts with nonsedating antihistamines; however, if symptoms are not managed well, sedating antihistamines will be needed.

3. All patients, especially the elderly, should be educated on possible side effects including sedation, dry mouth, urine retention, and dizziness.

4. Start with low dose to monitor tolerance.

D. Other nursing interventions

1. Discuss skin care with patients recommending emollients and bathing not too hot or cold.

2. Emollients with anti-itch properties such as menthol, phenol, and pramoxine can be helpful especially for spot treatment and comfort.

3. Quality-of-life issues for patients with chronic urticaria should be acknowledged and addressed especially around relief of pruritus. Disease management needs to be prompt, and an individual approach is necessary due to the complex nature of urticaria. In addition, the management must be a close working cooperation with the patient.

4. When the cause of acute urticaria is promptly avoided, symptoms resolve rapidly. Reassure patients with acute urticaria that most cases resolve within 6 weeks; patients are often frustrated and fearful especially with chronic urticaria. The evolution from acute to chronic urticaria is not well understood, and the prognosis for resolution after 6 months is unclear.

E. Complementary alternative medicine

1. Certain foods can act as natural antihistamine:

a. Foods high in vitamin C such as carrots, mangoes, spinach, and tomatoes.

b. Foods high in vitamin A such as oranges, lemons, tangerines, limes, and grapefruit.

c. Pineapples can also be considered as an alternative and natural antihistamine. Bromelain is an enzyme found in high concentration in pineapple. Adding pineapples to daily diet can act as an alternative way to prevent and treat hive outbreaks.



IV. HOME CARE AND FOLLOW-UP

Patients with chronic urticaria may need referral to allergist, immunologist, or urticaria specialist if the cause cannot be found and the urticaria is interfering with quality of life. Allergy testing may be helpful for urticaria evaluation, but it is imperative for individuals who have had an anaphylactic episode. In general, patients with urticaria can be cared for on an outpatient basis unless their urticaria is severe and does not respond to antihistamine therapy or if they progress to laryngeal angioedema and/or anaphylactic shock or have comorbidities that require inpatient therapy.



VASCULITIS


I. OVERVIEW

Vasculitis is a nonspecific term that encompasses and a large and heterogeneous group of disorders characterized by inflammation of blood vessels. The process can involve the walls of any size or type of vessel causing damage that results in tissue necrosis. Cutaneous vasculitis may be limited to the skin, there may be secondary systemic involvement, or it may be a cutaneous manifestation of a systemic disease. There is no uniform classification system for vasculitis, although some classify according to the type of cell within the vessel walls (neutrophil, lymphocyte, or histiocyte), the type of circulating immune complexes, and the size and type of primary vessel involved (venule, arteriole, artery, or vein). The International Chapel Hill Consensus Conference of the Nomenclature of Systemic Vasculitides (CHCC2012) recently updated their system that specifies the name that should be used for a specifically defined disease process, used when a patient fulfills a definition. The spectrum of this group of diseases is too large for the context of this text, and therefore, the focus will be on some of the more common vasculitides affecting small vessels. This will include CSVV/leukocytoclastic vasculitis (LCV) and Henoch-Schönlein purpura (HSP).

A. Definition

1. All vessel sizes of venous and arterial systems can be involved. Small vessels include arterioles, capillaries, and postcapillary venules that are found in the superficial and middermis of the skin. Medium-sized vessels include the main visceral arteries and veins, and small arteries and veins within the deep dermis and subcutaneous tissue. Large vessels include the aorta, major branches and corresponding veins, and other named arteries such as the temporal artery.

2. Table 18-5 lists the main vasculitides classified by vessel size.

3. CSVV has in the past been referred to as LCV and hypersensitivity vasculitis and is the most commonly seen form of small-vessel necrotizing vasculitis. The condition may be limited to the skin or may involve different organs.

4. HSP is acute LCV that occurs mainly in children between ages 2 and 10; however, adult cases are reported. HSP is characterized by deposits of IgA immune complexes in venules, capillaries, and arterioles. HSP is the most common systemic vasculitis in children.

B. Etiology

1. Generally, there is hypersensitivity to various antigens including drugs, chemicals, microorganisms, and endogenous antigens. This results in the formation of immune complexes that are deposited in the vessel walls. There are many diseases that may be associated with hypersensitivity vasculitis; however, in many cases, the cause is not determined. These include the following:

a. Hepatitis B and C virus

b. Other infections

c. Drugs








TABLE 18-5 Classification of Vasculitides Based on Vessel Size

























Predominant Caliber of Affected Vessel


Classification


Subclassification


Small


Cutaneous smallvessel vasculitis


Idiopathic Henoch-Schönlein purpura Acute hemorrhagic edema of infancy Erythema elevatum diutinum


Small and medium sized


Secondary


Cryoglobulinemic ANCA associated


Infections and septic vasculitis Inflammatory disorders (SLE, rheumatoid arthritis, Sjogren syndrome) Drug exposure Neoplasms


Microscopic polyangiitis Wegener granulomatosis Churg-Strauss syndrome


Medium sized


PAN


Systemic form


Benign cutaneous form


Large


Temporal arteritis Takayasu arteritis



ANCA, antinuclear cytoplasmic antibodies; PAN, polyarteritis nodosa; SLE, systemic lupus erythematosus.

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Mar 9, 2021 | Posted by in NURSING | Comments Off on Hypersensitivities, Drug Eruptions, Vasculitides, and Miscellaneous Inflammatory Disorders

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