Walmart Continuing Education Managing Consequences of the Allergic Response:
Walmart Continuing Education Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic Disease Expiry Date: April 8, 2012 Author: Tom Smiley, BSc. Pharm., PharmD. CCCEP File # 899-0309 The Canadian Council on Continuing Education in Pharmacy has approved this program for 1.75 CEUs. Update for Pharmacists Update for Pharmacists Table of Contents MANAGING CONSEQUENCES OF THE ALLERGIC RESPONSE: Dear Manitoba Pharmacists: FOCUS ON ASTHMA AS A MODEL OF ATOPIC DISEASE . . . . . . . . 4 How is Asthma Control Defined? . . . . . . . . . . . . . . . . . . . . . . 9 Peak Expiratory Flow Meters for Patients feel that pharmacists are the most trusted health care professionals. Monitoring of Asthma Control . . . .With . . . . . this ................9 Case . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 4 responsibility comes our duty to maintain and grow our knowledge base so that we are able to provide exceptional our patients. Characterizing the Epidemiology and pharmaceutical care to Spirometry . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 10 Etiology of Atopic Conditions . . . . . . . . . . . . . . . . . . . . . . . . . 4 At Wal-Mart Pharmacy, our valued LivingSmart Pharmacists quarterly continuing Treatment ofreceive Asthma Based on Level of Control. . . . . . . . . . . . 10 The Pathophysiology of Allergic Reactions . . . . . . . . . . . . . . . 4 education modules on up to date topics on a regular basis. It is a pleasure for us to Fast-acting Bronchodilator on Demand . . . . . . . . . . . . . . . . . 10 share some of these CEU modules with you. We hope you are able to utilize this .wealth Atopic vs. Non-atopic Asthma . . . . . . . . . . . . . . . . . . . . . . . . . 5 of knowledge to improve your patient’s health outcomes, and together, we will be able Controller Therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 10 to grow our profession to new heights. Asthma Symptoms as a Consequence of Allergic Triggers . . . . 6 Best Regards, Triggers of Allergic Responses – Asthma, Allergic Rhinitis . . . . 6 Focus on Leukotriene Receptor Antagonists . . . . . . . . . . . . . . 11 Laurie Kaminsky, B.Sc.Pharm Immunotherapy for Prevention of Professional Services Allergy-Mediated SymptomsManager . . . . . . . . . . –. . Western . . . . . . . . . Canada ......7 Wal-Mart Canada Corp. Asthma Action Plans and Resources . . . . . . . . . . . . . . . . . . . . 11 How does immunotherapy work? . . . . . . . . . . . . . . . . . . . . . . . 7 Vijay Akileswaran, B.Sc.Pharm Use of Allergen Extract Immunotherapy Professional Services Manager in– Eastern Canada Specific Allergic Conditions ...........................8 Wal-Mart Canada Corp. Risks Associated Louise Hostewith Allergen Immunotherapy . . . . . . . . . . . . 8 Director, Professional Services Omalizumab: A Biological Response Modifier for Wal-Mart Canada Corp. Treatment of Allergic Asthma . . . . . . . . . . . . . . . . . . . . . . . . . . 8 Anaphylaxis – An Overview . . . . . . . . . . . . . . . . . . . . . . . . . . 12 Pharmacologic Management of Acute Anaphylaxis . . . . . . . . . 12 Precautions for People at Risk for Anaphylaxis . . . . . . . . . . . . 13 Summary . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14 REFERENCES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14 QUIZ . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15 Current Levels of Asthma Management – Challenges and Opportunities . . . . . . . . . . . . . . . . . . . . . . . . . 9 Accreditation requirements: A mark of 70% or greater is required on the quiz questions to earn the accredited number of CEUs. A participant who fails a post-test may have one opportunity to re-do the test without being advised which questions were incorrect the first time. Following the second attempt, whether a pass or fail, the correct answers and rationale will be provided to the participant. Disclosure Statement: The Author and Expert Reviewers declare no real or perceived conflict with the sponsor company. Learning Objectives After successful completion of this continuing education lesson pharmacists will be better able to: • Discuss the epidemiology, etiology and pathophysiology associated with atopic conditions • Describe different allergy/asthma triggers and methods for avoidance • Recommend immunization strategies and omalizumab therapy for attenuation of allergy and asthma symptoms in patients meeting appropriate criteria • Aid patients in assessment of asthma control and understanding of asthma severity • Recommend appropriate stepwise therapy for asthma • Recommend appropriate treatment of anaphylaxis 2 2 Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic Disease Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic Disease Update for Pharmacists Update for Pharmacists Table of Contents MANAGING CONSEQUENCES OF THE ALLERGIC RESPONSE: FOCUS ON ASTHMA AS A MODEL OF ATOPIC DISEASE . . . . . . . . 4 Case . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 4 Characterizing the Epidemiology and Etiology of Atopic Conditions . . . . . . . . . . . . . . . . . . . . . . . . . 4 The Pathophysiology of Allergic Reactions . . . . . . . . . . . . . . . 4 Atopic vs. Non-atopic Asthma . . . . . . . . . . . . . . . . . . . . . . . . . 5 Asthma Symptoms as a Consequence of Allergic Triggers . . . . 6 Triggers of Allergic Responses – Asthma, Allergic Rhinitis . . . . 6 Immunotherapy for Prevention of Allergy-Mediated Symptoms . . . . . . . . . . . . . . . . . . . . . . . . . . . 7 How is Asthma Control Defined? . . . . . . . . . . . . . . . . . . . . . . 9 Peak Expiratory Flow Meters for Monitoring of Asthma Control . . . . . . . . . . . . . . . . . . . . . . . . . 9 Spirometry . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 10 Treatment of Asthma Based on Level of Control. . . . . . . . . . . . 10 Fast-acting Bronchodilator on Demand . . . . . . . . . . . . . . . . . . 10 Controller Therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 10 Focus on Leukotriene Receptor Antagonists . . . . . . . . . . . . . . 11 Asthma Action Plans and Resources . . . . . . . . . . . . . . . . . . . . 11 Anaphylaxis – An Overview . . . . . . . . . . . . . . . . . . . . . . . . . . 12 How does immunotherapy work? . . . . . . . . . . . . . . . . . . . . . . . 7 Pharmacologic Management of Acute Anaphylaxis . . . . . . . . . 12 Use of Allergen Extract Immunotherapy in Specific Allergic Conditions . . . . . . . . . . . . . . . . . . . . . . . . . . . 8 Precautions for People at Risk for Anaphylaxis . . . . . . . . . . . . 13 Risks Associated with Allergen Immunotherapy . . . . . . . . . . . . 8 Omalizumab: A Biological Response Modifier for Treatment of Allergic Asthma . . . . . . . . . . . . . . . . . . . . . . . . . . 8 Summary . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14 REFERENCES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14 QUIZ . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15 Current Levels of Asthma Management – Challenges and Opportunities . . . . . . . . . . . . . . . . . . . . . . . . . 9 Accreditation requirements: A mark of 70% or greater is required on the quiz questions to earn the accredited number of CEUs. A participant who fails a post-test may have one opportunity to re-do the test without being advised which questions were incorrect the first time. Following the second attempt, whether a pass or fail, the correct answers and rationale will be provided to the participant. Disclosure Statement: The Author and Expert Reviewers declare no real or perceived conflict with the sponsor company. Learning Objectives After successful completion of this continuing education lesson pharmacists will be better able to: • Discuss the epidemiology, etiology and pathophysiology associated with atopic conditions • Describe different allergy/asthma triggers and methods for avoidance • Recommend immunization strategies and omalizumab therapy for attenuation of allergy and asthma symptoms in patients meeting appropriate criteria • Aid patients in assessment of asthma control and understanding of asthma severity • Recommend appropriate stepwise therapy for asthma • Recommend appropriate treatment of anaphylaxis 2 Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic Disease Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic Disease 3 Update for Pharmacists Update for Pharmacists MANAGING CONSEQUENCES OF THE ALLERGIC RESPONSE: FOCUS ON ASTHMA AS A MODEL OF ATOPIC DISEASE Case Julie is a 25 year old lady who is pregnant with her first child. Julie has seasonal allergies as well as allergies to dust and moulds. She also has asthma. Julie’s husband gets hayfever in the fall of the year but does not have asthma. Julie wants to do whatever she can to reduce her child’s risk for allergies. She is wondering if her child will have allergies no matter what she does. Characterizing the Epidemiology and Etiology of Atopic Conditions The incidence of immunoglobulin E (IgE)-mediated medical conditions such as asthma, allergic rhinitis, and atopic dermatitis are rising in Canada and around the world.1, 2 It is interesting to note, however, that the prevalence of these allergy-mediated conditions varies widely across Canada and between different countries. 2 This suggests that the causes of these conditions are multifactorial, with atopy but one of many factors involved in pathogenesis.3 Allergic conditions have been referred to as “polygenic,” meaning that several genes on different chromosomes are involved in causing these disorders. Although a family history of allergic disease is a strong predisposing factor, the rapid increase in prevalence of atopic conditions cannot be explained by this factor alone.3 Many theories have been offered in an attempt to explain the increase in prevalence of atopic conditions. These have been based on the following epidemiologic observations: • Increase in atopic conditions has occurred in industrialized Western countries. • Prevalence is higher in urban than in rural areas. • Prevalence is higher in privileged socioeconomic groups and smaller families. There is an increasing prevalence of asthma associated with fast-paced industrialization in developing countries. Potential consequences of the development of Western societies causing increased risk for atopy may include increased exposure to allergens and to both outdoor and indoor pollution as well as changing lifestyle factors such as diet, body weight, antibiotic use, and stress.2 One hypothesis suggests increased use of topical corticosteroids may play a role, noting that the use of these agents and the increase in prevalence of atopic diseases were coincidental.4 In summary, it is apparent that for expression of atopic disorder to occur, a complex interaction of genes with environmental factors is required.3 Case (continued) Julie is wondering if there is anything specific she can do to reduce her child’s chance of getting asthma and/or allergies. Will breastfeeding help? Should they get rid of their dog? Is there any preventive medication that can be given? Clinical Practice Pearl: Parents who are themselves atopic may be concerned about the possibility of their child inheriting the condition. The Canadian Pediatric Asthma Consensus Guidelines have recommended actions that may protect against development of allergy and asthma:5 • Do not expose fetus or infant to environmental tobacco smoke. Passive exposure to tobacco smoke is one of the strongest domestic and environmental risk factors for developing recurrent coughing/wheezing or asthma symptoms at any age during childhood.6 • The guidelines suggest that “Promotion of exclusive breastfeeding for at least four months seems reasonable.” However, recent evidence suggests that while exclusive breastfeeding seems to reduce risk for wheezing episodes in children less than four years of age (often associated with respiratory infections), the effect on risk of developing asthma in the long-term is not clear.7 For families where both parents are atopic, there is maternal asthma, or both parents have asthma, the guidelines recommend against the presence of a cat or dog in the house. However, a recent meta-analysis suggests that while dogs may increase asthma risk in an atopic individual, cat exposure may actually be protective.8 More studies with exact measurement of exposure are required to clarify this issue. The Pathophysiology of Allergic Reactions The onset of increased IgE levels and eosinophilia is preceded by a series of events as follows:9 Antigen is taken up by mucosal dendritic cells (often Langerhans’ cells in the airways) and presented to T lymphocytes (often in a draining lymph node). • T lymphocytes are of the T helper 1 (Th1) or T helper 2 (Th2) type. T lymphocytes with the Th2 cytokine profile increase synthesis of interleukin 4 (IL-4) and interleukin 13 (IL-13) which in turn promote IgE synthesis by B lymphocytes.(see Figure 1). In phase 1, IgE fixates to mast cells and basophils (see Figure 1)9 Pathways favouring the Th1 cytokine profile inhibit B lymphocyte production of IgE (see Figure 1). • When the person with allergy is re-exposed to the allergen the second and third phases occur. Cross-linking of IgE bound to mast cells trigger the release of vasoactive mediators (e.g., histamine, leukotrienes, prostaglandin D2 and kinins) from the mast cells (see Figure 1). For an overview of the effects of some of these mediators on allergic rhinitis and asthma please refer to Table 1. • IgE-induced mast cell degranulation is followed by a third or late-phase reaction, a second wave of hypersensitivity responses occurring many hours after the acute reaction, and dependent upon increased eosinophil levels. This phase is associated with hyper-responsiveness to inhaled irritants and allergens.10 Consequences of the Allergic Response: Focus on Asthma a Model of Atopic Disease 3 4Managing Managing Consequences of the as Allergic Response: Focus on Asthma as a Model of Atopic Disease Update for Pharmacists Update for Pharmacists Figure 1: The Pathophysiology of Allergic Responses (Adapted from Ref. 5) Allergens Dendritic Cell (airway) Dendritic Cell (lymph node) Interferon γ Inhibits B lymphocyte production of IgE Th1 B lymphocytes Th0 IgE Synthesis IL4, IL 13 Promotes B lymphocyte production of IgE Th2 Allergens Prostaglandin D2 Mast Cell Leukotrienes Table 1: Mediators of Signs and Symptoms of Asthma and Allergic Rhinitis9 Mediator Histamine Leukotrienes Signs and Symptoms Allergic Rhinitis Itch Sneeze Rhinorrhea Obstruction Possible rhinorrhea Obstruction Kinins Obstruction Prostaglandins Obstruction Endothelin Itch Sneeze Rhinorrhea Asthma Bronchoconstriction Plasma protein exudation Mucus secretion Bronchoconstriction Plasma protein exudation Mucus secretion Bronchoconstriction Cough Bronchoconstriction (PG E2, PG D2) Antibronchoconstrictor (PG E2) Cough (PG E2) Bronchoconstriction Kinin Histamine Atopic vs. Non-atopic Asthma The strongest predisposing factor for the development of asthma is atopy (hereditary allergy). A common first presentation of asthma in a child would be associated with a positive family history of asthma and allergy to tree and grass pollen, house dust mites, household pets, and moulds.11 Case 1 (continued): Julie’s child Jimmy is now 2 years old and Julie has heard him wheezing this week. Jimmy also has a runny nose. Julie wants to know if she should assume he has asthma. The diagnosis of asthma in preschool children is difficult because wheezing early in life can occur in more than half of all children.12 Most wheezing episodes are associated with viral respiratory illness. Therefore, it is very important that parents with young children who have had a wheeze do not automatically jump to the conclusion that their child has asthma. Approximately 60% of children with infantile wheeze will be healthy at school age.6 Preschool wheezing can be divided into four categories:6 • Transient wheezing – Wheezing during the first 2-3 years of life, but not after the age of three years. • Nonatopic wheezing – Mainly triggered by viral infection and tends to resolve later in childhood. 4 Managing Consequences of the Allergic Response: FocusDisease on Asthma as a Model of Atopic Disease Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic 5 Update for Pharmacists • Persistent asthma – Wheezing associated with the following: • Clinical manifestations of atopy (eczema, allergic rhinitis and conjunctivitis, food allergy), blood eosinophilia, and/ or elevated total immunoglobulin E (IgE). • Specific IgE-mediated sensitization to foods in infancy and early childhood, and subsequently to common inhaled allergens. • Inhalant allergen sensitization prior to three years of age, especially with sensitization and high levels of exposure to specific perennial allergens in the home. • A parental history of asthma. • Severe intermittent wheezing – Infrequent acute wheezing episodes associated with the following: • Minimal morbidity outside of time of respiratory tract illness. • Atopic characteristics, including eczema, allergic sensitization and peripheral blood eosinophilia. Atopic asthma is likely to persist whereas non-atopic asthma is most likely to resolve before adulthood. A clinical index for the diagnosis of asthma has been used to help predict which children will likely go on to have persistent asthma.5, 13 Stringent index: 3 or more episodes of wheeze during the first 3 years of life with: • parental history of at least one of the major risk factors: i. asthma ii. eczema or • 2 of 3 minor risk factors: i. eosinophilia ii. wheezing without colds iii. allergic rhinitis Loose index: any wheezing during the first 3 years of life plus: • 1 major or 2 minor risk factors Asthma Symptoms as a Consequence of Allergic Triggers Asthma affects approximately 8.4% of Canadians.14 The Adult Asthma Consensus Guidelines Update 2003 supports the following definition of asthma:15 • Characterized by paroxysmal or persistent symptoms such as dyspnea, chest tightness, wheezing, sputum production, and cough associated with variable airflow limitation and airway hyper-responsiveness to endogenous or exogenous stimuli. • Inflammation and its effects on airway structure are considered to be the principle mechanisms promoting the development and maintenance of asthma symptoms. Clinical Practice Pearl: Atopic dermatitis (eczema) is a common precursor to the development of asthma. Parents of children with atopic dermatitis should be educated about the signs and symptoms of asthma. Update for Pharmacists Similar to other atopic conditions, the prevalence of asthma has increased over the past number of years to epidemic proportions in Canada and the rest of the industrialized world. It is the most common chronic disease in children.12 Studies have shown that atopic dermatitis is a common precursor to the development of asthma.16 In atopic (i.e., allergic) asthma, the inhalation of specific allergens produces immediate bronchoconstriction that improves spontaneously over an hour or is easily reversed by a �-agonist. A second bronchoconstriction response often occurs 4-12 hours later (known as the late asthmatic response). This response is often more severe, more prolonged, and more difficult to reverse with bronchodilators. Corticosteroids can block the late asthmatic response but bronchodilators do not.11 If long-term airway inflammation resulting in asthma is not controlled, airway remodeling (thickening of the airway wall basement membrane) may occur. This refers to changes in structure of the amount and composition of the extracellular matrix in the airway wall. This may result in airflow obstruction becoming only partially reversible.11 Asthma and allergic rhinitis are no longer viewed as having distinct causes.2 Both nose and lower airways respond to stimulation by irritant substances. While increased blood flow is the main contributor to exacerbations of nasal obstruction in allergic rhinitis, smooth muscle constriction and airway narrowing is the primary cause of symptoms in asthma. Although eosinophilia is a characteristic feature of both diseases, in allergic rhinitis the mucosal eosinophilic response is strongly related to the antigenic load. In asthma, bronchial eosinophilia is prominent. In both asthma and allergic rhinitis there is epithelial accumulation of mast cells displaying allergen-induced activation, which results in the production of pro-inflammatory mediators including histamine, cytokines, prostaglandins, leukotrienes, tryptase, and kinins. Each of these mediators cause symptoms in asthma and allergic rhinitis (see Table 1). These pro-inflammatory mediators are important targets for current and future therapies. Triggers of Allergic Responses – Asthma, Allergic Rhinitis Studies have shown that early and persistent exposure aeroallergen sensitization confers a higher risk for development of asthma and allergic rhinitis compared to later development of sensitivity.17 Allergen exposure leads to sensitization and the triggering of symptoms.1 Studies where a potential allergen is removed before sensitization can occur have had conflicting results. The complete removal of a potential aeroallergen can be difficult to achieve and sustain, and this should be balanced with controlling symptoms through pharmacotherapy.6 Strategies that have been recommended for avoidance of allergy triggers are outlined in Table 2. Consequences of the Allergic Response: Focus on Asthma a Model of Atopic Disease 5 6Managing Managing Consequences of the as Allergic Response: Focus on Asthma as a Model of Atopic Disease Update for Pharmacists Update for Pharmacists Table 2: Allergens: Recommended Avoidance Strategies* Allergen Grass, tree, weed and flower pollen Dust mites (present in house dust) Moulds (may be present in damp basements, closets, bathrooms, and upholstered furniture, and other places) House pets (animal dander can stay in carpets and furniture for 4 - 6 weeks and remain in air for months after the animal leaves) Drugs Food allergens Smoke from tobacco and fires – environmental factors can trigger allergies (allergic rhinitis and asthma) Recommended Actions To Avoid Triggers • Use an air conditioner and keep doors and windows shut as much as possible. • Vacation in areas where pollen counts are low. • Limit outdoor activities when pollen counts are high. • Bathe or shower and change clothes after being outdoors during allergy season. • Dry clothes in a vented dryer instead of outside, where pollen may collect. • Use a cover for the bed mattress and box spring that is allergen- impermeable (does not allow allergens through material). • Use pillow cases that are allergen-impermeable and airtight. • Wash bedding in hot water at least 55o C (130o F) at least once a week. Dry in a hot dryer. • Clean surfaces with a damp cloth at least weekly. • Don’t use carpets or select carpets with low pile. • Choose vinyl, leather, or plain wooden furniture instead of fabric-upholstered furniture. • Vacuum floors at least weekly with a vacuum cleaner with integral HEPA filter and double-thickness bags. • Limit clutter and knickknacks that collect dust. Keep dust-accumulating objects in closed cupboards. • Keep relative humidity in home low (<50%); use a dehumidifier if necessary. • Replace curtains with blinds or easily washable curtains. • Remove stuffed toys from bedrooms or hot wash/freeze them. • Use a cleaning solution that contains 5% bleach to clean the tub and shower area and any other places where mould and mildew grow (should be done by a non-allergic individual). • Keep humidity in home below 50% to reduce mould growth. • Dry sheets and clothing in a vented dryer, as mould s may collect if hung outside to dry. • Refrain from walking in uncut fields, working with compost or dry soil, and raking leaves. • Removal of the pet from the home is the most effective approach. Where removal is not possible: • Keep pets out of the main living areas and bedrooms. • Brush pet outdoors to remove loose hair and allergens and wash pet at least once a week (to be done by non-allergic individual). • Keep the pet outside as much as possible. • Install a high-efficiency particulate air cleaner (HEPA) in the home. • When necessary, find a good home for the pet. • Cats tend to cause more problems than dogs. • Remove carpeting or vacuum frequently. • Avoid drugs that have been identified as allergens (such as ASA, NSAIDS). Non-selective betablockers (e.g., propranolol) should not be used by people with asthma. • Identify and avoid food allergens (most common: eggs, milk, peanuts, shellfish, fish, soy, and wheat). • Keep home smoke-free. • Avoid areas where smoking is allowed. • Encourage family members and/or caregivers to quit smoking. • Use airtight stove/fireplaces if wood must be burned. • Do not burn leaves in autumn. * Adapted from reference Immunotherapy for Prevention of Allergymediated Symptoms role of immunotherapy in allergic diseases varies according to the atopic condition. How Does Immunotherapy Work? In order to understand the most recently accepted theory of the mechanism of action of SIT, we need to build on the pathophysiological process outlined in Figure 1. In addition to Th1 and Th2 cells, a third type of T-cell referred to as regulatorysuppressor T-cells (TReg cells) has been identified.19 These cells have immunosuppressive function and cytokine profiles distinct from either Th1 or Th2 cells. They are able to inhibit the development of allergic Th2 responses and play a major role in allergen SIT. Recent evidence suggests that production of TReg cells and suppressive cytokines IL-10 and TGF-� (transforminggrowth factor beta cells) are induced by SIT.19 These, in turn, Prevention is always the best strategy for management of disease. The immune reaction which is stimulated by allergy triggers as described in Table 2, and results in symptoms of asthma and allergic rhinitis can be attenuated by immunotherapy. Specific immunotherapy or SIT (subcutaneous injection of small amounts of allergen) inhibits the progress of IgE-mediated allergic diseases such as asthma and allergic rhinitis.18 It is an interesting approach to management of allergies that addresses the cause of hypersensitivity to antigens at the cellular level. The 6 Managing Consequences of the Allergic Response: FocusDisease on Asthma as a Model of Atopic Disease Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic 7 Update for Pharmacists Update for Pharmacists suppress proliferative and cytokine responses against the major allergens and their T-cell-recognition sites.19 associated benefits and risks, including the importance of adhering to the immunotherapy schedule.12 Use of Allergen Extract Immunotherapy in Specific Allergic Conditions Risks Associated with Allergen Immunotherapy Case 1 (continued) Jimmy is now four years old and has allergic rhinitis. Julie has heard that allergen immunotherapy can help Jimmy with his symptoms and potentially even prevent him from getting asthma. Is that true? Allergen immunotherapy is effective in the management of allergic asthma, allergic rhinitis, and stinging insect hypersensitivity.20 It may also prevent the development of asthma in children with allergic rhinitis.20 Clinical study suggests that SIT consisting of house dust mite preparation is able to improve eczema in patients with atopic dermatitis and reduces the need for topical corticosteroids. This indication for allergen immunotherapy is still under investigation.18 Clinical indications for allergen immunotherapy include the following:20 • In patients with allergic asthma: • Symptoms of asthma after natural exposure to aeroallergens, demonstrable evidence of clinically relevant specific IgE antibodies, and one of the following: • Poor response to pharmacotherapy or allergen avoidance • Unacceptable adverse effects of medication • Desire to avoid long-term pharmacotherapy and reduce the cost of medication • Coexisting allergic rhinitis and allergic asthma • In patients with allergic rhinitis: • Symptoms of allergic rhinitis after natural exposure to aeroallergens, demonstrable evidence of clinically relevant specific IgE antibodies (i.e., skin-testing and/or immunological assay) and one of the following: • Poor response to pharmacotherapy or allergen avoidance • Unacceptable adverse effects of medications • Desire to avoid long-term pharmacotherapy and reduce the cost of medication • Coexisting allergic rhinitis and asthma • Possible prevention of asthma in children • In patients with reactions to Hymenoptera (ants, bees, wasps) stings: • History of a systemic reaction to a Hymenoptera sting (especially if the reaction was associated with respiratory or cardiovascular symptoms) and demonstrable evidence of clinically relevant specific IgE antibodies • Age > 16 years, history of a systemic reaction limited to the skin, and demonstrable evidence of clinically relevant specific IgE antibodies • History of a systemic reaction to imported fire ant and demonstrable evidence of clinically relevant specific IgE antibodies When speaking with patients about allergen immunotherapy options, health professionals need to educate patients around the In general, the risk of fatal and nonfatal systemic reactions after administration of allergenic extract is very low. Circumstances which may increase such risk include:20 • Unstable steroid-dependent asthma • Any medical condition that would compromise a patient’s ability to withstand a systemic anaphylactic reaction. This would include uncontrolled hypertension (because use of epinephrine to treat systemic symptoms could be dangerous), unstable angina or recent myocardial infarction • Patients who are unable to communicate. They may not be able to report signs or symptoms of systemic reaction • A high level of allergic reactivity based on diagnostic tests (usually immediate hypersensitivity skin tests) • A history of previous systemic reactions to allergen immunotherapy • Starting a new vial of extract • Asthmatic symptoms present immediately before receiving an injection of allergenic extract • Concomitant treatment with �-adrenergic blocking agents • Administration of pollen extracts • Rate of increase in the dose of allergenic extract that is too rapid considering the patient’s degree of hypersensitivity Treatment of anaphylaxis resulting from administration of allergenic extracts is essentially the same as the treatment of anaphylaxis from other causes (epinephrine is the treatment of choice). Most severe reactions develop within 20 to 30 minutes after the immunotherapy injection, and rarely an anaphylactic reaction may be delayed for longer than one hour. Therefore, most health professionals administering immunotherapy will have their patients wait one-half hour in the office after administration of the injection. Case (continued) Julie has found her asthma worsening lately and has had difficulty keeping her symptoms controlled. Her environment hasn’t changed, she is compliant with her prescribed therapy and the severity of her asthma is moderate to severe. She has heard of a “biologic” that can help people with asthma. She would like you to tell her more about it. Omalizumab: A Biological Response Modifier for Treatment of Allergic Asthma Omalizumab is a recombinant humanized monoclonal antibody indicated for treatment of moderate to severe persistent asthma in persons 12 years or older who have had a positive skin test or in vitro reactivity to a perennial aeroallergen and whose symptoms are inadequately controlled with inhaled corticosteroids. 21 It improves asthma symptoms by binding to the IgE molecule and inhibiting the binding of IgE to its receptor on mast cells and basophils (see Figure 1), thereby preventing the release of the allergy symptoms mediators such as histamine. 21 Consequences of the Allergic Response: Focus on Asthma a Model of Atopic Disease 7 8Managing Managing Consequences of the as Allergic Response: Focus on Asthma as a Model of Atopic Disease Update for Pharmacists Clinical Practice Pearl: Patients who have moderate to severe asthma and consistently have poor control despite adherence to treatment principles have an opportunity to improve quality of life through treatment with omalizumab. Studies have consistently shown that omalizumab reduces the incidence and frequency of clinically significant asthma exacerbations and reduces inhaled corticosteroid requirements in patients with moderate to severe allergic asthma.22 The drug has also been shown to improve asthma symptoms and lung function and to improve asthma-related quality of life in these patients.22 In patients with severe asthma, omalizumab has been shown to significantly reduce the level of exacerbations and the level of severe exacerbations resulting in hospitalization or emergency care in patients deemed to be at high risk because of recent emergency treatment or prior intubation.22 Use of omalizumab is associated with side effects that include injection site reactions (45%), viral (24%) and upper respiratory tract infections (19%), headache (15%), sinusitis (16%), and pharyngitis (10%). The occurrence of adverse events resulting in clinical intervention (e.g., discontinuation of omalizumab treatment) in clinical studies was 0.1% or less.21 Current Levels of Asthma Management – Challenges and Opportunities It is very evident that a large care gap exists between current and optimal levels of asthma care. A large gap also exists in patients’ perceptions of good asthma control. In a survey of 893 Canadian patients with asthma (The Reality of Asthma in Canada or TRAC survey), 53% had uncontrolled asthma as per criteria outlined below and 47% had controlled asthma.23 Only 3% of patients actually thought they had uncontrolled asthma and 45% believed that making one or two emergency trips to the hospital was just a normal part of having the condition.23 Only 11% of patients had written action plans and only one-half used them regularly.24 Approximately 61% of physicians surveyed in the TRAC study admitted not using current Canadian asthma guidelines most or all of the time.24 These findings represent an opportunity for pharmacists and all health professionals to educate patients around appropriate management of asthma, assessment of control and development of action plans. Pharmacists are ideally positioned to play a critical role in the collaborative education of patients. How is Asthma Control Defined? The Adult Asthma Consensus Guidelines Update 2003 offer the following as criteria for the control of asthma:15 • Daytime symptoms less than 4 days per week • Night-time symptoms less than one night per week • Normal physical activity • Mild, infrequent exacerbations • No absenteeism from school or work due to asthma • Fewer than 4 doses per week of a fast-acting �2-agonist (apart from one dose/day before exercise) • Forced expiratory volume in one second or peak expiratory flow at 90% of personal best or greater Update for Pharmacists • Diurnal variability (difference between highest and lowest value) in peak expiratory flow (PEF) of less than 10-15% during the day. The checklist above can be used with patients to determine if their asthma is controlled. If any of the criteria above do not apply, then a patient’s asthma is not controlled. Alternatively, a 30-second asthma test™ has been developed to help patients quickly determine if their asthma is controlled. Figure 2: The 30-Second Asthma Test25 ❏ I use my blue inhaler (reliever medication) 4 or more times a week (except one dose/day for exercise). ❏ I cough, wheeze or have a tight chest because of my asthma (4 or more days per week). ❏ Coughing, wheezing or chest tightness wakes me at night (1 or more times a week). ❏ I stop exercising because of my asthma (in the past 3 months). ❏ I miss work or school because of my asthma (in the past 3 months). If you answered yes to one or more of the questions above, talk with your doctor or certified asthma educator about how you can better manage your asthma. Peak Expiratory Flow Meters for Monitoring of Asthma Control Peak flow monitors measure the peak expiratory flow rate. They can be used to:26 • Help determine the severity of asthma • Check response to treatment during an acute asthma episode • Monitor progress in treatment of chronic asthma and provide objective information for any possible adjustments in therapy • Detect worsening in lung function, thereby avoiding a possible exacerbation in asthma with early intervention Predicted “normal” peak flow is determined by height, age and gender. However, asthma control is best followed by comparing daily peak flow readings with “personal best” reading. The personal best is the highest peak flow number a patient can achieve over a 2-3 week period when asthma is under control.26 Peak flow should be recorded twice daily for two to three weeks, using the same peak flow meter. It is important to understand that personal best values in children will change as they grow and as disease status changes. The following steps should be followed when using a peak flow meter: • The device must read zero or be at base level to begin • Take reading standing up whenever possible • Patient should inhale as deeply as possible • Meter should be placed in mouth and lips closed around the mouthpiece • Patient must blow out as hard and as fast as possible • Patient must not cough, spit or let tongue block the mouthpiece 8 Managing Consequences of the Allergic Response: FocusDisease on Asthma as a Model of Atopic Disease Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic 9 Update for Pharmacists Update for Pharmacists • The process repeated two additional times with the highest of the three readings documented • Be sure to remind the patient to clean the meter as recommended by the manufacturer Peak flow readings are generally interpreted as follows: • Peak Expiratory flow rate (PEFR) of 80-100% of personal best reflects controlled asthma • PEFR of 50-80% of personal best means caution and a temporary increase in asthma medication is indicated • PEFR below 50% of personal best means “danger”/ Follow instructions of Asthma Care Plan • Results of peak flow monitoring should be linked (along with asthma symptoms) to an appropriate asthma action care plan Peak flow meters must be checked regularly for accuracy and reproducibility of results. This can be accomplished by asking patients to take their meter to clinic visits so that readings can be compared with spirometry.27 • A patient who is less than 80% of personal best is not well controlled. A patient who is less than 60% of personal best is in the “danger zone” and should immediately attend an emergency department of a hospital. Clinical Practice Pearl: Peak flow monitors are recommended particularly for those people with asthma who are poor perceivers of worsening asthma for which they have required hospital emergency treatment. For others, monitoring symptoms and use of rescue medication is the most important means for evaluating asthma control. Spirometry Spirometry is performed with a spirometer in a clinical setting to measure lung volumes. The following is some terminology used:28 • Vital capacity (VC) is the volume of air blown off after maximal inspiration to full expiration. • Forced Expiratory Volume (FEV) is associated with exhalation into the spirometer as forcefully and completely as possible after maximal inspiration. The total volume of air blown is known as the Forced Vital Capacity (FVC). • The total volume of air blown in the first second of this activity (as measured by the spirometer) is known as the Forced Expiratory Volume in the first second (FEV1). In general, healthy people can exhale at least 75-80% of their FVC (i.e., FEV1/FVC) ratio in one second. Pulmonary disorders generally fall into two categories: those that restrict the lungs and thorax and those that obstruct them. In a general sense, obstructive disease limits airflow during expiration while restrictive disease limits airflow during inspiration. Spirometry is used to confirm a diagnosis of asthma. A 12% (preferably 15%) or greater improvement in FEV1 from baseline 15 minutes after use of an inhaled short-acting �2-agonist, or a 20% or greater improvement after 10-14 days of ingested prednisone, when symptoms are stable, indicates a reversible airflow obstruction scenario consistent with asthma.28 clinic where the apparatus is available. Portable peak flow meters are much more convenient for airflow monitoring. Although spirometry can help to confirm a diagnosis of asthma, its value is far more important in relating the subjective patient reported symptoms to an objective measure of lung function. Treatment of Asthma Based on Level of Control Treatment of asthma is based upon an individual’s current asthma control, escalated if needed to gain control, only after addressing other reasons for poor control, and reduced to the least amount required to maintain asthma control.29 Attention should always be paid to environmental control (i.e., identifying asthma triggers and avoiding/preventing exposure). Assessment of asthma control, triggers, compliance with treatment regimens, inhaler technique and co-morbidities should take place on a regular basis. Although the triggers of asthma are often atopic in nature, evidence points to control of airway inflammation and bronchoconstriction as the most effective approach to treatment. Fast-acting Bronchodilator on Demand: All individuals with asthma should have access to a fast-acting bronchodilator for use as needed to treat acute symptoms. Inhaled fast-acting β2-agonists are the preferred class and route of reliever medication. These include: • Several short-acting β2-agonists: salbutamol, terbutaline, and fenoterol; • One long-acting β2-agonist; formoterol. Formoterol should only be used as a reliever in individuals on regular inhaled corticosteroid (ICS) therapy in adults and children aged 12 years and over, preferably in the same inhaler device (i.e., combination budesonide/formoterol preparation).29 Controller Therapy: • Regular controller therapy is indicated in children 6 years and over and adults who have one or more indicators of poor control. • Pharmacologic therapy should be determined based upon an individual’s current asthma control, escalated if needed to gain control, only after addressing other reasons for poor control, and reduced to the least amount required to maintain asthma control. • Prescribed controller therapy should take into account both current control and future risk for severe exacerbations.29 For the 2010 Canadian Respiratory Guidelines update: Recommendations for the management of asthma in children (6 years and over) and adults, visit http://www.respiratoryguidlines. ca/sites/all/files/cts_asthma_slim_jim_2010.pdf. All alterations in medication therapy should be considered a trial, and effectiveness should be re-evaluated after a reasonable period of time. After optimal asthma control is achieved, medications should be reduced to the minimum necessary to maintain control. Spirometry is also helpful for monitoring asthma status. A detailed account of therapies used in the treatment of However, this is often impractical given the need to attend a asthma other than leukotriene receptor antagonists which directly Managing Consequences of the Allergic Response: Focus on Asthma a Model of Atopic Disease 9 10 Managing Consequences of the as Allergic Response: Focus on Asthma as a Model of Atopic Disease Update for Pharmacists target leukotriene mediation of asthma symptoms prompted by immune response, is beyond the scope of this lesson. Please refer to previous continuing education lessons on asthma management for more information. Focus on Leukotriene Receptor Antagonists Leukotriene Receptor Antagonists (LTRAs) act by preventing the binding of the cysteinyl leukotrienes (LTC4, LTD4, LTE4) to their binding sites in the human airway. Leukotrienes are released from cells such as mast cells and eosinophils and cause inflammation, bronchoconstriction, mucous secretion, vascular permeability, and eosinophil recruitment. Currently available LTRAs include montelukast and zafirlukast. • LTRAs are a less effective option for monotherapy in mild asthma for those patients who cannot or will not use ICS.15 In a systematic review which compared the effects of LTRAs and ICS, patients treated with LTRAs were 60% more likely to suffer an asthma exacerbation that required a course of oral prednisone than patients using ICS.30 Patients using ICS also had better symptom control and lung function. LTRAs should not be used as monotherapy for moderate to severe asthma. • LTRAs are also a less effective option than LABA for add-on therapy to ICS when low-dose ICS alone does not control asthma in adults.15 • Montelukast (10 mg for adults, 5 mg for 6-14 years of age, and 4 mg for 2-5 years of age) is an alternative to as-needed salbutamol for prevention of exercise-induced bronchoconstriction in adult and pediatric patients 2 years of age and older. • LTRAs may be used as an additive therapy to ICS in an attempt to reduce the dose of ICS while maintaining control (especially in children). • LTRAs must not be used instead of short-acting �2-agonists for treatment of acute asthma attacks. • Montelukast and zafirlukast are associated with adverse effects which include infrequent episodes of headache, nausea, diarrhea and abdominal pain.31 Rare cases of Churg-Strauss syndrome (eosinophilic vasculitis) have been reported after stopping or reducing doses of oral corticosteroids while taking a LTRA.27 Churg-Strauss syndrome is characterized by symptoms which can include worsened asthma, fever, weight loss, maculopapular rash, purpura, rhinitis, cough, shortness of breath, chest pain, diarrhea, abdominal pain and prostatitis. • Montelukast may be used in children 2 years of age and over, while zafirlukast is not indicated for children under 12 years of age. • Montelukast has not been documented to interact with other drugs that would require dose adjustment. Zafirlukast inhibits action of the cytochrome P450 2C9 isoenzyme system. This is the likely mechanism for a 35% increase in prothrombin time observed in a warfarin/zafirlukast drug interaction study.32 Therefore INR should be monitored closely if this drug combination is used. • Other drugs metabolized by the cytochrome P450 2C9 should be monitored closely with use of zafirlukast. These include tolbutamide, phenytoin, and carbamazepine. Erythromycin and theophylline may decrease plasma levels of zafirlukast, while ASA (650 mg four times daily) may result in increased plasma levels of the drug. Increased levels Update for Pharmacists of zafirlukast may increase risk for adverse effects which may include headache, nausea, diarrhea, abdominal pain. • In patients with stable alcoholic cirrhosis, the clearance of zafirlukast is reduced by approximately 50-60.32 Zafirlukast is not recommended for use by patients with hepatic impairment of any kind. If liver dysfunction is suspected at any time (e.g., right upper quadrant abdominal pain, enlarged liver, nausea, fatigue, lethargy, pruritus, jaundice), zafirlukast should be discontinued.32 Asthma Action Plans and Resources The Canadian Thoracic Society Asthma Management Continuum – 2010 Consensus Summary for children six years of age and over, and adults states that “written action plans are a key component of care for all patients with asthma.” The written plans referred to are often called “asthma action plans.”15 They allow patients to understand when to alter medication management (e.g., increase doses of medications and/or add oral prednisone therapy) and when to seek emergency help according to the severity of symptoms. The action plan should be created by the doctor or asthma-care specialist responsible for the patient’s asthma care. Since a minority of patients report utilizing an asthma action plan, this is an excellent awareness-raising opportunity for pharmacists. • Examples of action plans based on symptoms only (i.e., do not require a patient to have a peak flow meter) can be found on the Internet at the Asthma Society of Canada website at http://www.asthma.ca/adults/control/pdf/ AsthmaActionPlan_ENG.pdf. • If a patient has a peak flow meter, action plans found at the Canadian Lung Association website at http://www.lung. ca/_resources/asthma_action_plan.pdf • The action plan found at Family Physician Airways Group of Canada at http://www.fpagc.com/AsthmaActionPlan2004. pdf is also available. All action plans include the message to go to emergency if peak expiratory flow rate is 60% of personal best or lower. Clinical Practice Pearl: The Lung Association offers management tips and a number of asthma management tools including an asthma diary which allows patients to record asthma symptoms, medication use and peak flow readings in their publication “The Asthma Handbook.” It can be found at http://www. lung.ca/pdf/handbook_web.pdf These tools can all be downloaded and serve as excellent resources for pharmacists to educate patients about their condition. Asthma patients without action plans should be encouraged to take one of the templates with them to their principle asthma care provider at their next appointment. The following are recommendations from the Canadian Asthma Consensus Report on elements of patient asthma education. These elements could be ticked off as you complete patient education as part of an asthma clinic and with your clients on an individual basis. ❏ Rationale and methods for identifying and avoiding irritants and relevant allergens. ❏ Education about airway inflammation and bronchospasm. 10 Managing Consequences of the Allergic Response: FocusDisease on Asthma as a Model of Atopic Disease Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic 11 Update for Pharmacists ❏ Description of the rationale, correct use and side effects of preventive medications and bronchodilators. ❏ Discussion of potential concerns or barriers to medication use. ❏ Demonstration and practice of inhaler/spacer technique and monitoring using symptoms or PEF meters. ❏ Description of criteria for control and steps to take when control deteriorates (i.e., a written Asthma Action Plan). ❏ Discussion of the action plan and an attempt to improve the patient’s and family’s understanding and willingness to implement the plan when it is needed. ❏ Demonstration of techniques for successful communication with health care professionals. ❏ Emphasis on the need for regular follow-up. ❏ Discussion of intolerance to sulfites or ASA. ❏ Specific information on food allergy. ❏ Discussion, when relevant, of conditions such as pregnancy. If asthma is not controlled, review the following: ❏ Inhaler technique ❏ Potential barriers to compliance • Cost • Side effects • Concerns • Forgetfulness ❏ Asthma trigger exposure ❏ Other drugs: e.g., NSAIDs, beta-blockers ❏ Other potentially aggravating diseases: e.g., gastroesophageal reflux disease (GERD), rhinosinusitis Anaphylaxis – An Overview The difference between survival and death of a patient with severe allergy with or without associated asthma may ultimately depend on a health professional’s and patient’s ability to immediately recognize and appropriately treat an anaphylactic reaction. Even when initially there are mild symptoms, the potential for progression to a severe and even irreversible outcome must be recognized.33 Any substance has the potential to cause anaphylaxis.34 The most common causes of IgE-mediated anaphylaxis are insect stings, medications, latex, peanuts and tree nuts (e.g., walnuts, hazelnuts, almonds, cashews, pecans, and pistachios), shellfish, fish, milk, eggs and wheat. Common anaphylactoid reactions include those associated with NSAID use, opiates, and radiocontrast agents.34 Anaphylaxis is a systemic, generalized reaction; therefore, a wide variety of clinical signs and symptoms may be present, including:34 • Skin – flushing, erythema, pruritus, urticaria, angioedema, maculopapular rash • Gastrointestinal – nausea, vomiting, abdominal pain, diarrhea • Neurologic – dizziness, weakness, seizures, syncope • Ocular – pruritus, conjunctival injection (dilated vessels causing redness of the eye), lacrimation • Upper airway – nasal congestion, sneezing, hoarseness, stridor, oropharyngeal or laryngeal edema, cough, obstruction • Lower airway – dyspnea, bronchospasm, tachypnea, accessory muscle use, cyanosis, respiratory arrest • Cardiovascular – Tachycardia, hypotension, arrhythmias, myocardial ischemia/infarction, cardiac arrest Update for Pharmacists Symptoms usually appear within minutes but can occasionally occur as long as one hour after exposure to the offending antigen. Signs and symptoms resolve within hours of treatment. However, in 20% of cases a second phase of symptoms occurs. These “second-phase” symptoms occur at a mean of ten hours after the initial reaction but may occur up to 38 hours later. Approximately one-third of these reactions are more severe, one-third are of the same severity, and one-third are less severe than the initial reaction.33 Clinical Practice Pearl: Although many authors recommend administration of corticosteroids to prevent or minimize the second phase (demonstrated beneficial in trials), there have been several documented cases of patients receiving corticosteroid therapy who went on to experience severe biphasic reactions. Therefore, patients must be prepared for a second reaction with epinephrine-based treatment regardless of corticosteroid administration.33 Pharmacologic Management of Acute Anaphylaxis Parenteral epinephrine given intramuscularly (IM) is the cornerstone of management for acute anaphylaxis (see Table 4).34 Administration of epinephrine is also indicated in the treatment of life-threatening asthma attacks.35 The strong vasoconstrictor action of epinephrine acts quickly to counteract vasodilation and resultant capillary permeability. Epinephrine relaxes the bronchioles through its action on smooth muscle, thereby relieving wheezing and dyspnea. It also relieves angioedema and hives.35 Epinephrine injection is available commercially in an auto-injector format (EpiPen®,EpiPen Jr.® and Twin-Ject®). The following are some instructions for the appropriate use of this product:35 • The patients or someone at the scene who is familiar with the use of the EpiPen® or EpiPen Jr.® (e.g., a parent or teacher) should use the product at first sign of a recognized anaphylactic reaction. Emergency help should then be summoned for follow-up care at the nearest hospital. • Both the adult and “junior” version of the auto-injector deliver a single dose of 0.3 mL; the adult version contains epinephrine 1:1000 (delivering 0.3 mg) and the junior version contains epinephrine 1:2000 (delivering 0.15 mg).35 Clinical Practice Pearl: Parents need to be made aware that once their child weighs 30 kg or more, they should switch to the 0.3 mg dose of epinephrine. There is a common tendency to prescribe EpiPen Jr.® for anyone under 12 years of age. • Patients should be informed that there will be some liquid left in the auto-injector after the injection is given, as only 0.3 mL of the 2 mL contained in the injector is actually administered. • Patients must be careful to store the auto-injector at room temperature (between 15oC and 30o C.) It must not be left Managing Consequences of the Allergic Response: Focus on Asthma a Model of Atopic Disease 11 12 Managing Consequences of the as Allergic Response: Focus on Asthma as a Model of Atopic Disease Update for Pharmacists Update for Pharmacists in extreme temperatures such as in the car during a heat wave or a cold snap. • If the solution in the auto-injector has turned brown, is discoloured, or contains a precipitate, it must not be used. • It is recommended that two Epipen® auto-injectors or one Twinject® be kept handy at all times, as a second dose may be needed should a second-phase reaction occur. Epinephrine should be injected only in the thigh as outlined in the package insert. Figure 3: Patient Instructions for Use of EpiPen and EpiPen Jr35 How do I use the EpiPen and EpiPen Jr auto-injectors? (See package inserts for illustrations): 1. Pull off the grey safety release. 2. Inject EpiPen or EpiPen Jr into your outer thigh, even through clothing if necessary. Do not inject EpiPen or EpiPen Jr into your hands, feet, or buttock. Swing and push black tip firmly into outer thigh so it “clicks” AND HOLD on thigh for several seconds. 3. Massage the injected area for 10 seconds. 4. Seek medical attention immediately. 5. If you are able, go to the emergency room immediately after using EpiPen auto-injector. Even after you have sought medical help, stay where you can call 911 or within easy access of a hospital for the next 48 hours. If bronchospasm is present, inhaled �2-agonists such as salbutamol are useful. Corticosteroids (e.g., methylprednisolone 125 mg IV or prednisone 50 mg PO) have been found useful in minimizing second-phase reactions. Patients who are hypotensive should receive intravenous fluid support with crystalloid or colloid, and severe cases may require vasopressor agents such as dopamine or high-dilution epinephrine (1:10,000). Precautions for People at Risk for Anaphylaxis Allergen avoidance is the most reliable method for preventing anaphylaxis (see Table 2). Patients with documented allergies should wear identification such as a MedicAlert ™ bracelet. With MedicAlert™, in the event of an emergency, the caregiver is alerted to the possible cause of the incident and a 24-hour hotline provides callers with immediate access to the patient’s medical record. Health professionals can order MedicAlert™ application forms online at https://www.medicalert.ca/en/health/order.asp or by phoning 800-668-1507 between the hours of 9am and 5pm EST. Patients can also apply directly online at https://www. medicalert.ca/en/join/ An excellent organization to refer patients and parents of children with allergies to is Anaphylaxis Canada, which can be found online at http://www.anaphylaxis.org/index.asp . This website addresses issues associated with living with anaphylaxis and provides links to services that would commonly be required for people at risk for anaphylactic reactions. Table 4: Pharmacologic Management of Acute Anaphylaxis Reaction34 Drug Epinephrine 1:1000, IM Diphenhydramine IV, IM, or PO Ranitidine IV or PO Corticosteroids: Methylprednisolone IV or prednisone PO Frequency of Administration Immediately, then every 5-15 min. as needed* Once patient’s condition is stabilized with epinephrine and fluids, then every 4-6 hrs prn Once patient’s condition is stabilized with epinephrine and fluids, then every 8 hrs prn Once patient’s condition is stabilized with epinephrine and fluids, then every 6 hrs prn Dose (Adult) 0.3 - 0.5 mL 25 - 50 mg Dose (Child) 0.01 mL/kg (up to 0.3 mL) 1.25 mg/kg 50 mg IV or 150 mg PO 1.25 mg/kg IV or 2 mg/kg PO methylprednisolone 125 mg IV or prednisone 50 mg PO 1 mg/kg IV or 1 mg/kg PO * Until resolution or signs of palpitation, tremor, uncomfortable apprehension and anxiety occur. 12 Managing Consequences of the Allergic Response: FocusDisease on Asthma as a Model of Atopic Disease Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic 13 Update for Pharmacists Update for Pharmacists Summary Pharmacists are an important source of education for the atopic patient. Patients with a family history of allergy are at higher risk for all atopic conditions. People who have children with atopic dermatitis or allergic rhinitis should be vigilant for signs of asthma in their child. Avoidance of potential allergens is the cornerstone for management of conditions associated with atopy. Immunotherapy is a strategy that is associated with great relief for many patients. Pharmacists should ensure that patients understand how to assess their level of asthma control and the potential that exists for better quality of life through optimal asthma management. The continuum care promoted by the Canadian Asthma Consensus Update forofPharmacists Guidelines 2003 update, coupled with a raised awareness of asthma monitoring and effective pharmacist and allied health professional communication and intervention is essential to helping patients gain and maintain control of their asthma symptoms. Education of patients that includes development of a care plan and understanding of their disease state is an important role for pharmacists. Pharmacists are an important resource for patients at risk for anyphylactic reactions. Ensuring patients understand how and when to use emergency epinephrine products is a critical education piece for pharmacists to convey. REFERENCES 1. 2. 3. 4. 5. 6. 7. 8. 9. 10. 11. 12. 13. 14. 15. 16. 17. Eichenfield LF, Hanifin JM, Beck LA et al. Atopic dermatitis and asthma: parallels in the evolution of treatment. Pediatrics 2003;111(3):608-616. Habbick BF, Pizzichini MM, Taylor B, Rennie D, Senthilselvan A, Sears MR. Prevalence of asthma, rhinitis and eczema among children in 2 Canadian cities: the International Study of Asthma and Allergies in Childhood. CMAJ 1999;160(13):1824-1828. Arshad SH. Primary prevention of asthma and allergy. J Allergy Clin Immunol 2005;116(1):3-14. Pampura AN. Prevalence of atopic diseases and the use of topical corticosteroids. Is there any connection? Med Hypotheses 2005;64(3):575-578. Becker A, Berube D, Chad Z et al. Canadian Pediatric Asthma Consensus guidelines, 2003 (updated to December 2004): introduction. CMAJ 2005;173(6 Suppl):S12-S14. Bacharier LB, Boner A, Carlsen KH et al. Diagnosis and treatment of asthma in childhood: a PRACTALL consensus report. Allergy 2008;63(1):5-34. Greer FR, Sicherer SH, Burks AW. Effects of early nutritional interventions on the development of atopic disease in infants and children: the role of maternal dietary restriction, breastfeeding, timing of introduction of complementary foods, and hydrolyzed formulas. Pediatrics 2008;121(1):183-191. Takkouche B, Gonzalez-Barcala FJ, Etminan M, Fitzgerald M. Exposure to furry pets and the risk of asthma and allergic rhinitis: a meta-analysis. Allergy 2008;63(7):857-864. Howarth PH. ABC of allergies. Pathogenic mechanisms: a rational basis for treatment. BMJ 1998;316(7133):758-761. Oettgen HC, Geha RS. IgE in asthma and atopy: cellular and molecular connections. J Clin Invest 1999;104(7):829-835. Self TH. Asthma. Applied Therapeutics: The Clinical Use of Drugs , 23.1-23.43. 2005. Lippincott, Williams & Wilkins. Becker A, Watson W, Ferguson A, Dimich-Ward H, Chan-Yeung M. The Canadian asthma primary prevention study: outcomes at 2 years of age. J Allergy Clin Immunol 2004;113(4):650-656. Castro-Rodriguez JA, Holberg CJ, Wright AL, Martinez FD. A clinical index to define risk of asthma in young children with recurrent wheezing. Am J Respir Crit Care Med 2000;162(4 Pt 1):1403-1406. Health Canada. Respiratory Disease in Canada. Canadian Cataloguing in Publication Data 2005; ISBN 0-663-30968-5. Lemiere C, Bai T, Balter M et al. Adult Asthma Consensus Guidelines Update 2003. Can Respir J 2004;11(Suppl A):9A-18A. Bergmann RL, Edenharter G, Bergmann KE et al. Atopic dermatitis in early infancy predicts allergic airway disease at 5 years. Clin Exp Allergy 1998;28(8):965-970. Warner JO. A double-blinded, randomized, placebo-controlled trial of cetirizine in preventing the onset of asthma in children with atopic dermatitis: 18 months’ treatment and 18 months’ posttreatment follow-up. J Allergy Clin Immunol 2001;108(6):929-937. 18. Werfel T, Breuer K, Rueff F et al. Usefulness of specific immunotherapy in patients with atopic dermatitis and allergic sensitization to house dust mites: a multi-centre, randomized, dose-response study. Allergy 2006;61(2):202-205. 19. Akdis M, Blaser K, Akdis CA. T regulatory cells in allergy: novel concepts in the pathogenesis, prevention, and treatment of allergic diseases. J Allergy Clin Immunol 2005;116(5):961-968. 20. Joint Council of Asthma Allergy and Immunology. Practice parameters for allergen immunotherapy. Ann Allergy 90, S1-S540. 2006. 21. Xolair Product Monograph. Compendium of Pharmaceuticals and Specialties . 2009. 22. Bousquet J, Cabrera P, Berkman N et al. The effect of treatment with omalizumab, an anti-IgE antibody, on asthma exacerbations and emergency medical visits in patients with severe persistent asthma. Allergy 2005;60(3):302308. 23. McIvor RA, Boulet LP, FitzGerald JM, Zimmerman S, Chapman KR. Asthma control in Canada: no improvement since we last looked in 1999. Can Fam Physician 2007;53(4):673-7, 672. 24. FitzGerald JM, Boulet LP, McIvor RA, Zimmerman S, Chapman KR. Asthma control in Canada remains suboptimal: the Reality of Asthma Control (TRAC) study. Can Respir J 2006;13(5):253-259. 25. The Lung Association. Asthma Management: The Asthma Handbook. http:// www.lung.ca/pdf/handbook_web.pdf . 2009. Accessed Mar. 17, 2009 26. American Academy of Asthma AaI. Tips to remember: What is a Peak Flow Meter? http://www.aaaai.org/patients/publicedmat/tips/whatispeakflowmeter.stm . 2009. Accessed March 15, 2009 27. Boulet LP, Becker A, Berube D, Beveridge R, Ernst P. Canadian Asthma Consensus Report, 1999. Canadian Asthma Consensus Group. CMAJ 1999;161(11 Suppl):S1-61. 28. Barreiro TJ, Perillo I. An approach to interpreting spirometry. Am Fam Physician 2004;69(5):1107-1114. 29. Lougheed MD, Lemiere C, Dell SD, et al. Canadian Thoracic Society Asthma Management Continuum – 2010 Consensus Summary for children six years of age and over, and adults. Can Respir J 2010;17:15-24. 30. Ducharme FM. Inhaled glucocorticoids versus leukotriene receptor antagonists as single agent asthma treatment: systematic review of current evidence. BMJ 2003;326(7390):621. 31. McCormack D. Adult Asthma. Therapeutic Choices , 626-639. 2007. Canadian Pharmacists Association. 32. Astra Zeneca. Accolate product monograph. 2009. 33. The diagnosis and management of anaphylaxis: an updated practice parameter. J Allergy Clin Immunol 2005;115(3 Suppl 2):S483-S523. 34. Ellis AK, Day JH. Diagnosis and management of anaphylaxis. CMAJ 2003;169(4):307-311. 35. Epipen product monograph. Compendium of Pharmaceuticals and Specialties. 2009. Managing Consequences of the Allergic Response: Focus on Asthma a Model of Atopic Disease 13 14 Managing Consequences of the as Allergic Response: Focus on Asthma as a Model of Atopic Disease Quiz Dear Pharmacist: Below and on the back cover are the questions for the Wal-Mart Continuing Education lesson Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic Disease. Please complete the answer card on the back cover by circling the correct answer to each question and drop the completed card in the mail, or fax it to: The Manitoba Society of Pharmacists at 1-204-956-6686. The answer card can also be submitted online at www.msp.mb.ca. Please keep a photocopy for your records. You will be notified of your results within four to six weeks of receipt of your answer card. QUIZ 1. Which of the following statements about the epidemiology and etiology of atopic conditions is true? a. Family history of allergy-related disease is the sole determinant of a child’s risk for IgE-mediated disease. b. The incidence of IgE-mediated medical conditions is more prevalent in underprivileged areas. c. Prevalence of IgE-mediated disease is higher in urban than in rural areas. d. Outdoor pollution, but not indoor pollution plays a role in prevalence of IgE-mediated disease. 5. A patient tells you that his asthma is in good control. When you ask, he says he has only been to emergency once this year because of his asthma. Which of the following statements about asthma control and perception of asthma control is true according to The Reality of Asthma in Canada (TRAC) survey? a. About 80% of survey participants had their asthma under control. b. Almost one-half patients surveyed thought that one to two trips to emergency is normal for patients with asthma. c. Less than one-half patients surveyed perceived their asthma was under control. d. Answers a and b are correct. The Manitoba Society of Pharmacists 202-90 Garry St. Winnipeg, MB R3C 4H1 A young lady is considering immunotherapy to reduce future allergy symptoms. Which of the following statements about immunotherapy is FALSE? a. All patients with asthma are candidates for immunotherapy. b. Patients receiving immunotherapy against hymenoptera stings should be older than 16 years of age. c. People with uncontrolled hypertension should not receive immunotherapy, d. Risk for reactions to immunotherapy is greater when a new vial of extract is opened. _______________________________ 4. _______________________________ A young mother comes to you and says she has noticed her child wheezing on and off, especially when she has a cold, during her first three years. Which of the following is your best response? a. Don’t assume she has asthma. Many children have transient wheezing during the first few years. b. Wheezing is not common until after three years old in most children. She will likely be diagnosed with asthma. c. She will only get asthma if she first has allergic rhinitis. d. Mother should take her daughter to the doctor for allergy tests and possible immunotherapy. From___________________________ 3. Place Postage Here 2. Which of the following allergy symptom mediators promote bronchoconstriction? a. kinins b. leukotrienes c. endothelin d. all of the above Answer Card This is the answer card for the 2010 Wal-Mart Continuing Education lesson Managing Consequences of the Allergic Response: Focus on Asthma as a Model of Atopic Disease. Please circle the correct response to each question (there is only one correct answer for each question), complete the information at the bottom of the card and drop the completed card in the mail, or fax it to: The Manitoba Society of Pharmacists at 1-204-956-6686. The answer card can also be completed and submitted online at www.msp.mb.ca. Please keep a photocopy of your completed Answer Card for your records. Thank you. Quiz Answers 1. 2. 3. 4. 5. 6. 8. 9. 10. a b c d a b c d a b c d a b c d a b c d a b c d a b c d a b c d a b c d 6. A gentleman tells you that his doctor has told him he he now needs a long-acting β2-agonist addition to the short-acting β2-agonist and inhaled corticosteroid (ICS) controller he is currently using. Why would the doctor have prescribed the additional treatment for him? a. His Peak Expiratory Flow diurnal variation is 8%. b. His peak flow meter reading was 91% of personal best. c. He has daytime symptoms twice per week on average. d. He has been using his short-acting β2-agonist once daily on average for the last month. 7. A doctor asks you what dose of omalizumab he should order for an adult patient. Which of the following is your most appropriate response? a. Dose should be started at 150 mg SC every 4 weeks and titrated upwards as needed. b. Dose in adults should be 375 mg every 2 weeks. c. Dose should be based on symptoms. d. Dose should be based on serum IgE concentration and body weight. 8. A physician would like your opinion on whether to use montelukast or zafirlukast as add-on therapy for an atopic individual who has severe asthma. Which of the following statements about these two agents is true? a. Zafirlukast is not metabolized by the Cytochrome P450 system while montelukast is. b. Zafirlukast but not montelukast is associated with increased risk for Churg-Strauss syndrome. c. Montelukast is indicated for children while zafirlukast is indicated for only those older than 12 years. d. Answers b and c are correct 9. A patient tells you that he has heard a second phase reaction after an initial anaphylactic reaction may occur. He wants to know how long after the first reaction the second may occur. a. Approximately 1-2 hours later b. Up to 5 hours later c. 10 hours to 38 hours later d. Up to 3 days later 10. A patient wants to know more about the epipen® auto-injector. Which of the following statements is FALSE? a. If liquid is brown-coloured, auto-injector should be discarded. b. It is recommended to leave auto injector in the car so it is readily available on trips. c. Two auto injectors or one TwinJect should be available at all times. d. Epinephrine should only be injected in the thigh. Pharmacist Information Name:_ ________________________________________________________ Membership Number:_ ____________________________________________ Address:________________________________________________________ ______________________________________________________________ Tel:__________________________________ Fax:______________________ License Number:_ ________________________________________________ WAL 48000 Printed by Leech Printing 188155
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