The page number in the footer is not for bibliographic referencingwww.tandfonline.com/ojfp 31 Introduction Asthma is a chronic inflammatory disease of the airways, associated with bronchial hyper-responsiveness and reversible airflow obstruction. It is one of the most common chronic diseases in the world. It is estimated that approximately 300 million people worldwide suffer from asthma. Estimates of the prevalence of asthma range from 7% in France and Germany, to 11% in the USA, and 15-18% in the UK. Approximately 20% of patients suffer from severe asthma, of which 20% is inadequately controlled.1 Furthermore, asthma is reportedly increasing worldwide, as communities in the developing world adopt Western lifestyles and become urbanised. The World Health Organization recognised asthma as being of major public health importance in 2013.2 The magnitude of the burden of asthma may be underap- preciated. This is partly owing to health systems, such as primary healthcare services that are overwhelmed by communicable respiratory diseases, such as pneumonia or tuberculosis.3 The burden of asthma is underappreciated in countries like South Africa, where the burden of respiratory diseases such as pneumonia, tuberculosis and human immunodeficiency virus (HIV)-associated lung disease is well known.3 Asthma is the eighth leading contributor to the burden of disease in South Africa, and is the second most important chronic disease after HIV/acquired immune deficiency syndrome.3,4 Despite the availability of medication, asthma remains poorly controlled in many patients.3,5 The emphasis in asthma treatment is on achieving effective control. The Global Initiative for Asthma’s goals are to achieve and maintain control of the symptoms, maintain pulmonary function as close to normal as possible, and to prevent exacerbations and mortality.6 Improper or inadequate implementation of the guidelines is a major reason for poor asthma management in South Africa.3 Challenges to successful implementation include factors within the healthcare system and the individual behaviour of healthcare providers, as well as that of patients or caregivers. Moreover, socio-economic and structural barriers that impair access to healthcare services remain important obstacles.3 A large number of patients have not yet benefited from advances in asthma treatment, and are still insufficiently controlled, placing severe limits on daily life, and placing them at risk of asthma-related morbidity and mortality.7 Asthma is the most common chronic inflammatory disease, with resistance in the intrapulmonary airways due to abnormalities of airway function.8 Pathological components of asthma can be described as cellular inflammation, including bronchitis, and the remodelling of the structural elements of the airway wall.9 This includes inflammation of the airway, constriction of the airway via smooth muscle contraction, the hypersecretion of mucus, bronchial hyper- responsiveness, and additional narrowing of the airway due to mucosal oedema and sloughing of the epithelial cells.10 Figure 1 provides a diagrammatic overview of the pathophysiology of asthma.8 Precipitating factors Several trigger factors can contribute to an asthma attack. Avoiding these factors can help to reduce asthma exacerbations and asthma severity.11 Table I presents the precipitating factors of asthma, with examples of asthma triggers.12 Abstract Asthma is a chronic inflammatory disease that causes hyper-responsiveness of the bronchial tree, with reversible airflow obstruction. The condition places a significant burden on our healthcare system. Chronic asthma can cause remodelling of the airway. Patients suffering from asthma should be aware of its signs and symptoms, as well as factors that can precipitate an asthmatic attack. Asthma is mostly classified as either acute or chronic. The diagnosis of asthma is based on identification of both a characteristic pattern of respiratory symptoms and variable expiratory airflow limitation. Treatment is based on how the patient presents, and includes bronchodilators, inhaled corticosteroids and mast cell stabilisers. This article provides an overview of the diagnosis, characterisation and treatment of asthma. Keywords: asthma, bronchodilator, inhaled corticosteroid, β2 agonist, peak expiratory flow, spirometry, SABA, LABA S Afr Fam Pract ISSN 2078-6190 EISSN 2078-6204 © 2015 The Author(s) REVIEW South African Family Practice 2015; 57(4):31-36 Open Access article distributed under the terms of the Creative Commons License [CC BY-NC-ND 4.0] http://creativecommons.org/licenses/by-nc-nd/4.0 Approach to asthma in adults N Schellack1*, A Truter2 and PN Ntuli3 1BCur, BPharm, PhD(Pharmacy), Associate Professor 2BPharm, Department of Pharmacy, Faculty Health Sciences, Sefako Makgatho Sciences Hospital 3BPharm, Dr George Mukhari Academic Hospital *Corresponding author: Natalie Schellack, natalie.schellack@smu.ac.za S Afr Fam Pract 2015;57(4):31-3632 The page number in the footer is not for bibliographic referencingwww.tandfonline.com/ojfp 32 Signs and symptoms Acute asthma Acute asthma, also referred to as asthma exacerbations, is an episodic asthma attack that progresses rapidly. Therefore, early recognition and rescue medication is of high importance.13 The signs of an acute asthma attack include an increased heart rate, tachypnoea, cyanotic or pale skin, expiratory and inspiratory wheezing, a hyperinflated chest and a dry hacking cough. During an acute asthma attack, patients can experience anxiety, severe dyspnoea, tightness of the chest, or a burning sensation and shortness of breath. Also, they may be unable to speak a full sentence and can be in acute distress.12 Chronic asthma Chronic asthma is a lifelong condition that varies in nature from daily to intermittent symptoms, and patients need to be permanently managed and treated. Signs and symptoms may persist during exercise, or when exposed to an allergen. The signs of chronic asthma include a dry hacking cough, expiratory wheezing or signs of allergic rhinitis and/or eczema. Episodes of dyspnoea, coughing at night, tightness of the chest, wheezing or stridor are the symptoms of chronic asthma.12 Inhaled allergens ↑ Proinflammatory mediators: • Histamine • Eicosanoids • Reactive O2 species Asthma triggers Acute inflammation Occupational challenge Exercise Acute inflammation (+) IgE Activation of mast cells and macrophages Constriction of the airway, ↑ mucus secretion and vasodilation Exudative mucus plugs with inflammatory and epithelial cells Persistent involvement Activation of eosinophils, CD4 (derived lymphocytic T cells), basophils, neutrophils and macrophages Acute plasma protein leakage Late-phase inflammation (6-9 hours) • Both central and peripheral airway structures are inflamed • Involvement of all types of airway cells (eosinophils, T cells, mast cells, macrophages, epithelial cells, fibroblasts and bronchial smooth muscle cells) • Regulation of airway inflammation, with initiation of a process of remodelling • Release of cytokines and growth factors Chronic inflammation (+) (+) CD4: cluster of differentiation 4, IgE: immunoglobulin E Figure 1: Diagrammatic representation of the pathophysiology of asthma8 Table I: Precipitating asthma factors12 Viral respiratory infections • Rhinovirus (most common) • Other: Respiratory syncytial virus, parainfluenza virus, coronavirus and influenza viruses Environmental factors • Air pollution: Ozone, sulphur dioxide and tobacco smoke • Allergens: Airborne pollen, furry animals, fungal spores, house dust mites and cockroaches Occupational factors • Industrial inhalants and irritants: Hay, mould, Arabic gum, spices, flour dust and chemicals, i.e. azo dyes, polyvinyl chloride, formaldehyde, ethylenediamine and anhydrides Food additives • Preservatives: Sulphites and benzalkonium chloride • Metabisulphites: In wine, beer and dried fruit Medication • Cyclo-oxygenase inhibitors: Aspirin and nonsteroidal-anti- inflammatory drugs • Non-selective β blockers Nutritional and exercise-related factors • Obesity • Vitamin D insufficiency in children • Exercise in a cold, dry climate Psychological factors • Stress, anxiety and depression Gastroenterology factors • Gastro-oesophageal reflux disease Approach to asthma in adults 33 The page number in the footer is not for bibliographic referencingwww.tandfonline.com/ojfp 33 Classification It is important to classify the severity of a patient’s asthma before implementing the initial treatment. This will assist in reviewing management of the condition once periodic assessment for asthma control has been established. Making the diagnosis of asthma is based on the identification of both a characteristic pattern of respiratory symptoms and variable expiratory airflow limitation.6 The following needs to be considered: • Whether or not the symptoms of recurrent airway obstruction are present, based on a history and the examination: This refers to a history of coughing, recurrent wheezing, recurrent difficulty in breathing, recurrent chest tightness, symptoms occurring or worsening at night or with exercise, a viral infection, exposure to allergens and irritants, changes in the weather, hard laughing or crying, stress or other factors. • The use of spirometry in all patients > 5 years of age, to determine whether or not the airway obstruction is at least partially reversible. • Other causes of obstruction. Table II shows the four categories of severity of asthma, which may be classified into one of two groups, namely mild intermittent or chronic persistent asthma. Daytime symptoms include coughing, wheezing and a tight chest, and night-time symptoms include coughing, wheezing, a tight chest and nocturnal wakening.11 Diagnosis An objective measurement of airflow is required to clinically diagnose asthma. Bronchodilator responsiveness, increased day- to-day or periodic variability, or bronchial challenge testing for bronchial hyper-responsiveness are components that need to be demonstrated in order to make a diagnosis of asthma. The identification and assessment of these components is of great value in improving the understanding and management of asthma.9 The approach to diagnosing asthma should start with a patient with recurrent respiratory symptoms prompted by sporadic symptoms of wheezing, coughing, breathlessness, sputum or tightness of the chest. Any alternative diagnosis should be excluded.8 The diagnostic algorithm for asthma is shown in Figure 2, in which step-by-step procedures can be followed to diagnose and then treat asthma.12 The spirometer is used for an objective lung function test called spirometry, and can be used to confirm airway obstruction. By adding a bronchodilator, i.e. a short-acting β2 agonist, reversibility of obstruction can be demonstrated, if present.8 The spirometry test measures the forced expiratory volume in one second (FEV1) and the forced vital capacity (FVC), i.e. the maximum volume of air that can be exhaled. The ratio of FEV1/ FVC can then be calculated. The patient should be told to take in the largest breath possible, and to seal his or her lips around the mouthpiece of the spirometer. He or she then has to blow the air out as fully and as rapidly as possible. The FEV1/FVC ratio in a normal adult population is usually greater than 0.80. Airflow Table II: Classification of asthma severity11 Intermittent Chronic persistent Mild l Mild ll Moderate lll Severe lV Daytime symptoms ≤ 2 per week Daytime symptoms 3-4 per week Daytime symptoms ≥ 4 per week Daytime symptoms are continuous Night-time symptoms ≤ 1 per month Night-time symptoms 2-4 per month Night-time symptoms ≥ 4 per month Night-time symptoms are frequent PEF ≥ 80% PEF ≥ 80% PEF 60-80% PEF ≤ 60% PEF: peak expiratory flow or Peak flow monitoring or a trial of therapy Spirometry before and after an inhaled, rapid-acting bronchodilator Alternative options: Less accurate Normal • Consider an alternative diagnosis, and/or • Peak flow monitoring, and/or • Bronchial hyper-responsiveness testing • The introduction of treatment (only for patients with a high likelihood of asthma. Diagnosis should be confirmed at a later stage) Consistent with asthma • Administer a short-acting β2 agonist, as needed, to relieve symptoms • Start anti-inflammatory therapy, e.g. a low-dose inhaled corticosteroid • Look for triggers by history and occupational exposure, and consider allergy testing • Consider any relevant co-morbid conditions Re-evaluate the diagnosis, control and treatment at a follow-up visit FVC, FEV1 and the FEV1/FVC ratio Spirometry results Preferred option: High level of accuracy Symptoms were identified that are deemed to be consistent with asthma FEV1: forced expiratory volume 1, FVC: forced vital capacity Figure 2: A diagnostic algorithm for asthma12 S Afr Fam Pract 2015;57(4):31-3634 The page number in the footer is not for bibliographic referencingwww.tandfonline.com/ojfp 34 obstruction is diagnosed in values of less than 0.80. Following the administration of a bronchodilator, an FEV1/FVC ratio of less than 0.70 identifies airway obstruction associated with chronic obstructive pulmonary disease (COPD).8 If the spirometry results are nondiagnostic for a patient who has a normal FEV1/FVC ratio, but asthma is still suspected, further objective tests are available to confirm the presence of this condition. The next step is to promote peak flow monitoring, using a measuring device called a peak flow meter (Figure 2). The fastest rate of expired flow is measured in this test. The patient should be advised to take the deepest breath possible, and then to blow it out as fast and hard as possible into the peak flow meter.8 The normal values of peak expiratory flow (PEF) for men aged 15-85 years with a height measurement between 160 cm and 190 cm is 420-670 ml/minute, and for women aged 15-85 years with a height measurement between 152 cm and 183 cm, 310-470 ml/minute.13 The two parameters supporting the diagnosis and confirmation of asthma using the peak flow meter are: • A periodic variation in PEF of more than 20%, or with twice daily readings of more than 10% at each reading. • An improvement of at least 60 ml/minute or at least 20% after inhalation of a rapid-acting bronchodilator.8 Management approach The effective management of asthma involves the ability to step up the treatment when asthma control is not achieved, or to step it down once good asthma control has been established. Therefore, patients should be reviewed frequently until the desired level of control is achieved.11,14 Table III provides parameters that may be used to define good asthma control.14 This can be further classified (Table IV) as controlled, partly controlled or uncontrolled asthma, for a given week. The patient must be assessed for adherence and the level of his or her asthma control. Complete control of asthma is possible, and should be achieved with minimal side-effects.11 A patient with poor asthma control presents with the following factors, and should be assessed fo r a re-evaluation of the asthma treatment:14 • The use of β2 agonists three or more times a week. • Sporadic symptoms three or more times a week. • Nocturnal awakening one night per week due to symptoms. The following should be carried out with the patient in order to achieve asthma control:11 • Determine the reasons for poor adherence. • Clarify misunderstandings in terms of differences between relievers and controllers. • Check the inhaler technique. • Identify exposure to trigger factors at home or work. • Check for the presence of gastro-oesophageal (acid) reflux disease. • Assess for rhinitis and sinusitis. • Identify other medication that may aggravate asthma, such as aspirin, non-steroidal anti-inflammatory drugs and β blockers. • Identify other medical conditions, such as COPD, that may be aggravating the asthma. Stepwise approach The patient should be initiated on the step that is most appropriate to his or her level of disease. Figure 3 provides an overview of the stepwise approach that should be followed in the management of asthma in adults.4,15 The pharmacotherapeutic approach to the treatment of bronchial asthma may also be applied to other airway conditions that are associated with bronchoconstriction or bronchospasm, and a resultant decrease in pulmonary or respiratory function. Drug treatment should be aimed at relieving the major symptom, i.e. dyspnoea due to bronchoconstriction or bronchospasm, or to modify (“control”) the disease process through anti-inflammatory and anti-allergic action. Therefore, these therapeutic approaches should also be applied to the management of COPD, and the latter also applies to the treatment of allergic rhinitis.4,16 Table IV: Levels of asthma control11 Characteristics Controlled (all of the following) Partly controlled (any measurement present in any week) Uncontrolled Daytime symptoms ≤ 2 per week > 2 per week Three or more features of partially controlled asthma in any week Activities limited None Any Nocturnal symptoms and night awakenings None Any Need for reliever or rescue treatment ≤ 2 per week > 2 per week Lung function (PEF) Normal < 80% predicted or personal best Exacerbations None ≥ 1 per year One in any week PEF: peak expiratory flow Table III: Parameters that define effective asthma control14 Asthma control Check (ü) No daytime symptoms No night-time awakening due to asthma No need for rescue medication (acute attacks) No exacerbations No limitations on activities, including exercise Normal lung function No side-effects Approach to asthma in adults 35 The page number in the footer is not for bibliographic referencingwww.tandfonline.com/ojfp 35 The bronchodilators These drugs cause relaxation of the bronchial smooth muscle, and therefore facilitate bronchodilatation. The bronchial smooth muscle contains both muscarinic and β2-adrenergic receptors. This provides for two possible mechanisms of drug action, i.e. active bronchodilatation and passive bronchodilatation.15-17 The selective β2-receptor agonists These drugs are selective agonists at the β2-adrenergic receptors (also referred to as the β2 adrenoceptors) of the bronchial smooth muscle when they are inhaled directly into their biophase, i.e. when a localised effect is achieved on the smooth muscle of the lower respiratory tract. When administered intravenously, or even by mouth, they lose their selectivity and produce cardiac (β1 receptor) and other systemic effects as well. Salbutamol (also known as albuterol), fenoterol, hexoprenaline and terbutaline are examples of short-acting β2 agonists (SABAs). These drugs act as active bronchodilators by increasing the concentration of cyclic adenosine 3’, 5’-monophosphate (cAMP). Therefore, it can be said that they act as physiological antagonists of the spasmogens causing the bronchoconstriction. Patients should be monitored for tachycardia, palpitations, skeletal muscle tremors and an increase in arterial blood pressure. In contrast to the SABAs, which have an average onset of action of approximately half an hour or less, and a duration of action in the range of 4-6 hours, the long-acting β2 agonists (LABAs) have a slower onset and a more sustained duration of action, lasting up to 12 hours. Salmeterol and formoterol, as well as the newer arformoterol and indacterol, are examples of LABAs.15-17 Theophylline, a methylxanthine, is a systemic bronchodilator with a narrow therapeutic index. Therefore, therapeutic drug monitoring is required. It differs from the previously mentioned drugs in that it inhibits the enzyme, phosphodiesterase. This produces nonselective β-receptor effects through an increase in the cAMP concentration. It is a second-line drug. Caffeine is a methylxanthine as well, and may be used as an alternative to aminophylline to prevent apnoea of prematurity. Aminophylline is theophylline ethylenediamine, which is more water soluble and may be administered intravenously. In addition to their systemic β-adrenergic effects, the methylxanthines also have a stimulatory effect on the central nervous system, resulting in increased levels of alertness, and can cause gastric irritation.15-17 Mild intermittent asthma Regular preventer therapy Persistent poor control The continuous or frequent use of oral steroids Initial add-on therapy Step 1 Step 2 Step 4 Step 5Step 3 Inhaled short-acting β2 agonists, when required Add: Inhaled corticosteroid, according to the severity of the patient’s disease, i.e. a low-dose inhaled corticosteroid, 250-500 µg/day beclomethasone dipropionate equivalent Consider trials of: An increased inhaled corticosteroid, 500-1 000 µg/day beclomethasone dipropionate equivalent Add a fourth drug, e.g. a leukotriene receptor antagonist, slow-release theophylline or a β2-agonist tablet Use a daily steroid tablet, at the lowest possible dose to provide adequate control A high-dose inhaled corticosteroid, > 1 000 µg/day beclomethasone dipropionate equivalent Consider other treatments to minimise the use of steroid tablets Refer the patient for specialist care Add: Inhaled LABA, and assess for control of asthma If there’s a good response to the LABA, continue If the patient is adherent to the LABA, but with poor control, continue with the LABA, but increase the inhaled corticosteroid dose If there is no response to the LABA, stop the LABA, and increase the inhaled corticosteroid dose, 500-1 000 µg/ day beclomethasone dipropionate equivalent If there is still inadequate control, initiate a trial of other therapies, i.e. leukotriene receptor antagonists or slow-release theophylline LABA: long-acting β2 agonist Figure 3: Management of asthma in adults4,15 S Afr Fam Pract 2015;57(4):31-3636 The page number in the footer is not for bibliographic referencingwww.tandfonline.com/ojfp 36 The antimuscarinic drugs Ipratropium bromide is the short-acting drug of choice, since it does not cause thickening of the bronchial secretions. Blocking the muscarinic receptors inhibits acetylcholine-induced bronchoconstriction, and implies that the adrenergic stimulation of β2 adrenoceptors in the bronchial smooth muscle will not be opposed by parasympathetic outflow from the vagus nerves. This results in bronchodilatation. Therefore, ipratropium bromide is a passive bronchodilator. Tiotropium bromide is a long-acting muscarinic antagonist. Both drugs are of particular importance in the management of COPD, and they cause very few systemic side-effects because they are poorly absorbed following inhalation. Enhanced bronchodilatation may be achieved when combining ipratropium bromide with a short-acting, selective β2 agonist, such as salbutamol or fenoterol, owing to the synergism between their mechanisms of action.15-17 The disease modifiers The inhaled glucocorticosteroids The inhaled glucocorticosteroids, such as budesonide, beclomethasone, ciclesonide and fluticasone, are considerably safer for long-term use than the systemic corticosteroids. They alter the course of the disease process and are life saving in the long run. However, they do not manage acute bronchospasm, but decrease bronchial hyper-reactivity and the risk of a relapse. Nasal sprays are also available for the management of allergic rhinitis. In addition to budesonide, beclomethasone and fluticasone, mometasone and triamcinolone are available for the latter indication. Inhaled glucocorticosteroids may give rise to oral thrush, i.e. oral candidiasis. Therefore, patients are encouraged to rinse their mouths with clean water following the use of steroid inhalers. These drugs are the main anti- inflammatory agents used in the management of asthma.15-17 The leukotriene receptor antagonists The leukotriene receptor antagonists are effective in controlling exercise- and aspirin-induced asthma, and may also be used in the chronic treatment of asthma. Zafirlukast and montelukast are examples. They are competitive antagonists of the cysteinyl leukotriene receptor 1. They have the advantage of oral administration, and montelukast is even available as sprinkles and in a chewable tablet form for paediatric use.15-17 Zileuton is a 5-lipoxygenase inhibitor, and therefore acts as a leukotriene synthesis inhibitor. Zileuton has the added advantage of also inhibiting the formation of leukotriene B4. The so-called mast cell stabilisers, such as sodium cromoglycate (also known as cromolyn sodium) and ketotifen, may be used in (allergic) asthma prophylaxis, as well as for the prevention and treatment of allergic rhinitis. These drugs act by stabilising the plasma membranes of the mast cells. This prevents these cells from degranulating and releasing histamine and other spasmogens. The term “mast cell stabiliser” is actually somewhat limiting because sodium cromoglycate, and the closely related nedocromil sodium, have effects on a number of other cells that form part of the inflammatory response as well, while ketotifen also acts as an antagonist at the H1 receptors. 15-17 The novel monoclonal antibody, omalizumab, is an immuno- globulin E (IgE) antagonist that is administered subcutaneously once or twice a month. However, it may elicit allergic reactions, or even anaphylaxis itself, as it is a protein-therapeutic agent.17 Conclusion Asthma may be described as a condition of reversible airflow obstruction, and can be effectively managed with the right treatment. Patients should be diagnosed timeously and treated aggressively, with appropriate monitoring. Dosages of inhaled corticosteroids can be increased, depending on the patient’s response to treatment. Patients who are resistant to treatment should be referred to a respiratory specialist. Monoclonal antibodies might assist in reducing the IgE-mediated immune response elicited during an asthmatic attack. References 1. Peters SP, Ferguson G, Deniz Y, Reisner C. Uncontrolled asthma: a review of the prevalence, disease burden and options for treatment. Respir Med. 2006;100(7):1139-1151. 2. World Health Organization. Asthma. WHO [homepage on the Internet]. 2013. c2014. Available from: http://www.who.int/mediacentre/factsheets/ fs307/en/ 3. Zar HJ, Lalloo UG. Acute asthma treatment guidelines: reducing morbidity and mortality in South Africa. S Afr Med J. 2013;103(3):159-160. 4. Mash B, Rhode H, Pather M, et al. Quality of asthma care: Western Cape province, South Africa. S Afr Med J. 2009;99(12):892-896. 5. O’Byrne PM, Pedersen S, Schatz M, et al. The poorly explored impact of uncontrolled asthma. Chest. 2013;143(2):511-523. 6. Global Initiative for Asthma. Pocket guide for asthma management and prevention (for adults and children over 5 years). GINA [homepage on the Internet]. 2014. c2015. Available from: http://www.ginasthma.org/local/ uploads/files/GINA_Pocket_2014_Jun11.pdf 7. Mehuys E, Van Bortel L, De Bolle L, et al. Effectiveness of pharmacist inter vention for asthma control improvement. Eur Respir J. 2008;31(4):791-799. 8. Kaplan AG, Balter MD, Bell AD, et al. Diagnosis of asthma in adults. Can Med Assoc J. 2009;181(10):210-220. 9. Gibson PG, McDonald VM, Marks GB. Asthma in older adults. Lancet. 2010;376(9743): 803-813. 10. Buddiga P, Kaliner MA, Bashir MH, Baz M. Asthma in older adults. Medscape [homepage on the Interent]. 2013. c2015. Available from: http://emedicine. medscape.com/article/2001721-overview 11. Lalloo UG, Ainslie GM, Jack C, et al. Guidelines for the management of chronic asthma in adolescents and adults. S Afr Fam Pract J. 2007;49(5):19-31. 12. Kelly HW, Sorkness CA. Asthma. In: Dipiro JT, Talber RL, Yee GC, et al, editors. Pharmacotherapy: a patophysiologic approach. 8th ed. New York: McGraw- Hill; 2008. 13. Lalloo UG, Awotedu AA, Feldman C, et al. Guideline for the management of acute asthma in adults. S Afr Med J. 2013;103(3):189-198. 14. Levy ML, Thomas M, Small IR, et al. Summary of the 2008 BTS/SIGN British guideline on the management of asthma. Prim Care Respir J. 2009;18 Supp1:S1-S16. 15. Rossiter D, editor. South African medicines formulary. 11th ed. Cape Town: Health and Medical Publishing Group, 2014. 16. Schellack G, editor. Pharmacology in clinical practice: application made easy for nurses and allied health professionals. 2nd ed. Claremont: Juta and Company, 2010. 17. Brenner GM, Stevens CW. Pharmacology. 3rd ed. Philadelphia: Saunders, 2010.