Asthma: Review Open Access
Asthma: Review Open Access
Asthma: Review Open Access
http://www.aacijournal.com/content/7/S1/S2
REVIEW
Open Access
Asthma
Harold Kim1,2,3*, Jorge Mazza1,3
Abstract
Asthma is the most common respiratory disorder in Canada. Despite significant improvement in the diagnosis and
management of this disorder, the majority of Canadians with asthma remain poorly controlled. In most patients,
however, control can be achieved through the use of avoidance measures and appropriate pharmacological
interventions. Inhaled corticosteroids (ICSs) represent the standard of care for the majority of patients. Combination
ICS/long-acting beta2-agonists (LABA) inhalers are preferred for most adults who fail to achieve control with ICS
therapy. Allergen-specific immunotherapy represents a potentially disease-modifying therapy for many patients
with asthma, but should only be prescribed by physicians with appropriate training in allergy. Regular monitoring
of asthma control, adherence to therapy and inhaler technique are also essential components of asthma
management. This article provides a review of current literature and guidelines for the appropriate diagnosis and
management of asthma.
Introduction
Asthma remains the most common chronic respiratory
disease in Canada, affecting approximately 10% of the
population [1]. Although asthma is often believed to be
a disorder localized to the lungs, current evidence indicates that it may represent a component of systemic airway disease involving the entire respiratory tract, and
this is supported by the fact that asthma frequently
coexists with other atopic disorders, particularly allergic
rhinitis [2].
Despite significant improvements in the diagnosis and
management of asthma over the past decade, as well as
the availability of comprehensive and widely-accepted
national and international clinical practice guidelines for
the disease, asthma control in Canada remains suboptimal. Results from the recent Reality of Asthma Control
(TRAC) in Canada study suggest that over 50% of Canadians with asthma have uncontrolled disease [3]. Poor
asthma control contributes to unnecessary morbidity,
limitations to daily activities and impairments in overall
quality of life [1].
This article provides an overview of diagnostic and
therapeutic guideline recommendations from the Global
Initiative for Asthma (GINA) and the Canadian Thoracic Society and as well as a review of current literature
1
University of Western Ontario, London, Ontario, Canada
Full list of author information is available at the end of the article
Definition
Asthma is defined as a chronic inflammatory disease of
the airways. The chronic inflammation is associated
with airway hyperresponsiveness (an exaggerated airwaynarrowing response to triggers, such as allergens and
exercise), that leads to recurrent symptoms such as
wheezing, dyspnea (shortness of breath), chest tightness
and coughing. Symptom episodes are generally associated with widespread, but variable, airflow obstruction
within the lungs that is usually reversible either spontaneously or with appropriate asthma treatment [4].
Pathophysiology
Asthma is associated with T helper cell type-2 (Th2)
immune responses, which are typical of other atopic
conditions. Various allergic (e.g., dust mites, cockroach
residue, furred animals, moulds, pollens) and non-allergic (e.g., infections, tobacco smoke, cold air, exercise)
triggers produce a cascade of immune-mediated events
leading to chronic airway inflammation. Elevated levels
of Th2 cells in the airways release specific cytokines,
including interleukin (IL)-4, IL-5, IL-9 and IL-13, that
promote eosinophilic inflammation and immunoglobulin
E (IgE) production by mast cells. IgE production, in
turn, triggers the release of inflammatory mediators,
such as histamine and cysteinyl leukotrienes, that cause
2011 Kim and Mazza; licensee BioMed Central Ltd. This is an open access article distributed under the terms of the Creative
Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and
reproduction in any medium, provided the original work is properly cited.
Kim and Mazza Allergy, Asthma & Clinical Immunology 2011, 7(Suppl 1):S2
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Diagnosis
The diagnosis of asthma involves a thorough medical
history, physical examination, and objective assessments
of lung function (spirometry preferred) to confirm the
diagnosis (see Table 1). Bronchoprovocation challenge
testing and assessing for markers of airway inflammation
may also be helpful for diagnosing the disease,
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particularly when objective measurements of lung function are normal despite the presence of asthma symptoms [4,6,7].
Medical history
Table 1 Diagnosis of asthma based on medical history, physical examination and objective measurements [4,6,7]
Medical history
Assess for classic symptoms of asthma:
Wheezing
Breathlessness
Chest tightness
Cough (with our without sputum)
Assess for symptom patterns suggestive of asthma:
Recurrent/episodic
Occur/worsen at night or early in the morning
Occur/worsen upon exposure to allergens (e.g., animal dander, pollen, dust mites) or irritants (e.g., exercise, cold air, tobacco smoke,
infections)
Respond to appropriate asthma therapy
Assess for family or personal history of atopic disease (particularly allergic rhinitis)
Physical Examination
Examine for wheezing on auscultation
Examine upper respiratory tract and skin for signs of other atopic conditions
Objective Measurements
Perform spirometry (preferred) to confirm the diagnosis
Diagnostic criteria:
FEV1 (after bronchodilator): 12% and 200 mL
Consider PEF as an alternative if spirometry is unavailable
Diagnostic criteria:
PEF (after bronchodilator): 20% and 60 L/min
Diurnal variation: >20%
If spirometry (or PEF) is normal, but symptoms are present consider:
Challenge testing (e.g., methacholine, histamine, mannitol, exercise)
Non-invasive markers of airway inflammation (exhaled nitric oxide, sputum eosinophilia)
Trial of appropriate asthma therapy
Allergy testing
Perform skin tests to assess allergic status and identify possible triggers
FVC: forced vital capacity; FEV1: forced expiratory volume in 1 second; PEF: peak expiratory flow
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Kim and Mazza Allergy, Asthma & Clinical Immunology 2011, 7(Suppl 1):S2
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The measurement of inflammatory markers such as sputum eosinophilia (amount of eosinophils in the sputum)
or levels of exhaled nitric oxide (a gaseous molecule
produced by some cells during an inflammatory
response) can also be useful for diagnosing asthma. Evidence suggests that exhaled nitric oxide levels may be
better able to identify asthmatic patients than basic lung
function testing, and may also be useful for monitoring
patient response to asthma therapy [7]. Although these
tests have been studied in the diagnosis and monitoring
of asthma, they are not yet widely used in Canada. With
further clinical evidence and use, these markers of airway inflammation will likely become more commonly
available.
Allergy skin testing
Treatment
The primary goal of asthma management is to achieve
and maintain control of the disease in order to prevent
exacerbations (abrupt and/or progressive worsening of
asthma symptoms that often require immediate medical
attention and/or the use of oral steroid therapy) and
reduce the risk of morbidity and mortality. The level of
asthma control should be assessed at each visit using
the criteria in Table 2, and treatment should be tailored
to achieve control. In most asthma patients, control can
be achieved through the use of both avoidance measures
and pharmacological interventions. The pharmacologic
agents commonly used for the treatment of asthma can
be classified as controllers (medications taken daily on a
long-term basis that achieve control primarily through
anti-inflammatory effects) and relievers (medications
used on an as-needed basis for quick relief of
Table 2 Criteria for assessing asthma control [4,6]
No exacerbations
Fewer than 3 doses per week of a rapid-acting beta2-agonist
bronchodilator
Daytime symptoms < 3 days per week
No nighttime symptoms
Normal physical activity
No absenteeism from work or school
FEV1 or PEF at least 90% of personal best
FEV1: forced expiratory volume in 1 second; PEF: peak expiratory flow
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bronchoconstriction and symptoms). Controller medications include ICSs, leukotriene receptor antagonists
(LTRAs), long-acting beta2-agonists (LABAs) in combination with an ICS, and anti-IgE therapy. Reliever medications include rapid-acting inhaled beta2-agonists and
inhaled anticholinergics [4,6,7]. Allergen-specific immunotherapy may also be considered in most patients with
allergic asthma, but must be prescribed by physicians
who are adequately trained in the treatment of allergies
[11,12]. Systemic corticosteroid therapy may also be
required for the management of acute asthma exacerbations. A simplified, stepwise algorithm for the treatment
of asthma is provided in Figure 1.
When asthma control has been achieved, ongoing
monitoring is essential to establish the minimum maintenance doses required to maintain control. However,
because asthma is a variable disease, treatment may
need to be adjusted periodically in response to loss of
control (as indicated by failure to meet the control criteria in Table 2) [4]. It is also imperative that all asthma
patients be empowered to take an active role in the
management of their disease. This can be accomplished
by providing patients with a personalized written action
plan for disease management and by educating the
patient about the nature of the disease, the role of medications, the importance of adhering to controller therapy, and the appropriate use of inhaler devices [7].
Avoidance measures
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Avoidance measures
Rapid-acting beta2-agonist
as needed
Combination ICS/LABA
or ICS/LTRA
Figure 1 A simplified, stepwise algorithm for the treatment of asthma. ICS: inhaled corticosteroid; LTRA: leukotriene receptor antagonist; LABA:
long-acting beta2-agonist; IgE: immunoglobulin E Note: Treatments can be used individually or in any combination.
associated with an increased risk of asthma-related morbidity and mortality, formoterol should only be used as
a reliever in patients 12 years of age or older who are
on regular controller therapy with an ICS [4,6,7].
Short-acting anticholinergic bronchodilators, such as
ipratropium bromide, may also be used as reliever therapy. However, these agents appear to be less effective
than inhaled rapid-acting beta2-agonists and, therefore,
should be reserved as second-line therapy for patients
who are unable to use SABAs. They may also be used in
addition to SABAs in patients experiencing moderate to
severe asthma exacerbations. Furthermore, chronic,
short-acting anticholinergic bronchodilator therapy is
not recommended for use in children [6].
Controller medications
Inhaled corticosteroids (ICSs)
ICSs are the most effective anti-inflammatory medications available for the treatment of asthma and represent the mainstay of therapy for most patients with the
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recommended when used in combination with ICS therapy. The combination of a LABA and ICS has been
shown to be highly effective in reducing asthma symptoms and exacerbations, and is the preferred treatment
option in adolescents or adults whose asthma is inadequately controlled on low-dose ICS therapy, or in children over 6 years of age who are uncontrolled on
moderate ICS doses [6]. Although there is no apparent
difference in efficacy between ICSs and LABAs given in
the same or in separate inhalers, combination ICS/
LABA inhalers are preferred because they preclude use
of the LABA without an ICS, are more convenient and
may enhance patient adherence. Three combination
ICS/LABA inhalers are available in Canada: salmeterol/
fluticasone (Advair), budesonide/formoterol (Symbicort)
and mometasone/formoterol (Zenhale). Combination
budesonide/formoterol has recently been approved for
use in Canada as a single inhaler for both daily maintenance (controller) and reliever therapy in individuals 12
years of age and older. It should only be used in patients
whose asthma is not adequately controlled with low-tomoderate ICS doses or whose disease severity warrants
treatment with combination therapy [4,6].
Anti-IgE therapy
The LTRAs montelukast and zafirlukast are also effective for the treatment of asthma and are generally considered to be safe and well tolerated. However, because
these agents are less effective than ICS treatment when
used as monotherapy, they are usually reserved for
patients who are unwilling or unable to use ICSs.
LTRAs can also be used as add-on therapy if asthma is
uncontrolled despite the use of low-to-moderate dose
ICS therapy. It is important to note, however, that
LTRAs are considered to be less effective than LABAs
as add-on therapy in adults [4,6]. In children, however,
the data are less clear and, therefore, the childs symptoms and the presence of comorbidities may help direct
treatment. For example, if a child with asthma also has
allergic rhinitis, the addition of montelukast should be
considered. If, however, the child has persistent airway
obstruction, the addition of a LABA may be preferred.
Systemic corticosteroids
As mentioned earlier, LABA monotherapy is not recommended in patients with asthma as it does not impact
airway inflammation and is associated with an increased
risk of morbidity and mortality. LABAs are only
Theophylline
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Table 3 Overview of the main controller therapies used for the treatment of asthma.
Usual Adult Dose
Ciclesonide (Alvesco)
Fluticasone (Flovent
HFA, Flovent Diskus)
ICSs
Beclomethasone (Qvar,
generics)
DPI (maintenance): 100/6 g or 200/6 g, 12 puffs od or bid; max 4 Not indicated for children under 12 years of age
puffs/day
DPI (maintenance and reliever): 100/6 g or 200/6 g, 12 puffs bid
or 2 puffs od; plus 1 puff as needed for relief of symptoms (no more
than 6 puffs on any single occasion); max 8 puffs/day
Fluticasone/salmeterol
(Advair MDI, Advair
Diskus)
Mometasone/
formoterol (Zenhale)
Montelukast (Singulair)
Zafirlukast (Accolate)
LTRAs
Anti-IgE therapy
Omalizumab (Xolair)
ICS: inhaled corticosteroid; MDI: metered dose inhaler; DPI: dry powder inhaler; LTRA: leukotriene receptor antagonists; IgE: immunoglobulin E; od: once daily; bid: twice
daily; sc: subcutaneously
allergic asthma, it is not universally accepted by all clinical practice guideline committees due to the potential
for serious anaphylactic reactions with this form of therapy [11].
A Cochrane review of 75 randomized controlled trials
examining the use of allergen-specific immunotherapy
in asthma management confirmed its efficacy in reducing asthma symptom scores and medication requirements, and improving airway hyperresponsiveness [12].
Similar benefits have been noted with sublingual immunotherapy [13], which is expected to be approved in
Canada in the near future. Evidence also suggests that
allergen-specific immunotherapy may prevent the onset
of asthma in atopic individuals [14].
At present, allergen-specific immunotherapy should be
considered on a case-by-case basis. It can be used prior
to a trial of ICS therapy in patients with very mild
Kim and Mazza Allergy, Asthma & Clinical Immunology 2011, 7(Suppl 1):S2
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Conclusions
Asthma is the most common respiratory disorder in
Canada, and contributes to significant morbidity and
mortality. A diagnosis of asthma should be suspected in
patients with recurrent cough, wheeze, chest tightness
and dyspnea, and should be confirmed using objective
measures of lung function (spirometry preferred).
Allergy testing is also recommended to identify possible
triggers of asthma symptoms.
In most patients, asthma control can be achieved
through the use of avoidance measures and appropriate
pharmacological interventions. ICSs represent the standard of care for the majority of asthma patients. For
those who fail to achieve control with low-to-moderate
ICS doses, combination therapy with a LABA and ICS is
the preferred treatment choice in most adults. LTRAs
can also be used as add-on therapy if asthma is uncontrolled despite the use of low-to-moderate dose ICS
therapy, particularly in patients with concurrent allergic
rhinitis. Anti-IgE therapy may be useful in select cases
of difficult to control asthma. Allergen-specific immunotherapy is a potentially disease-modifying therapy, but
should only be prescribed by physicians with appropriate training in allergy. All patients with asthma should
have regular follow-up visits during which criteria for
asthma control, adherence to therapy and proper inhaler
technique should be reviewed.
Key take-home messages
A clinical diagnosis of asthma should be suspected in
patients with intermittent symptoms of wheezing,
coughing, chest tightness and breathlessness.
Objective measurements of lung function, preferably
using spirometry, are needed to confirm the diagnosis.
All asthma patients should be prescribed a rapid-acting bronchodilator to be used as needed for relief of
acute symptoms.
ICS therapy is the standard of care for most patients
with asthma.
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Kim and Mazza Allergy, Asthma & Clinical Immunology 2011, 7(Suppl 1):S2
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11.
12.
13.
14.
15.
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doi:10.1186/1710-1492-7-S1-S2
Cite this article as: Kim and Mazza: Asthma. Allergy, Asthma & Clinical
Immunology 2011 7(Suppl 1):S2.