Respiratory Disorders Physiology Presentation by group 1 .pptx
1. WELCOME TO
Course Title: Pharmacology
Lecture Topic: Respiratory Disorders
Submitted to: Ma'am Rizwana Raheel
Submitted by: Group#1
Abera Siddique Ahtisham Farzand
Rimsha Waqar M. Umer
Sumbul Israr
2. LEARNING OUTCOMES:
Prefered Drugs Used To Treat Asthma.
Alternative Drugs Used To Treat Asthma.
Drugs Used To Treat Chronic Obstructive Pulmonary Disease.
Drugs Used To Treat Allergic Rhinitis.
Drugs Used To Treat Cough.
3. PREFERRED DRUGS USED TO TREAT ASTHMA
A. Goals of therapy:
Drug therapy for long-term control of asthma is designed to reverse and prevent airway
inflammation. The goals of asthma therapy are to decrease the intensity and frequency of
asthma symptoms, prevent future exacerbations, and minimize limitations in activity related to
asthma symptoms. First-line drug therapy based on classification of asthma is presented in
Figure 39.3.
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B. β2 -Adrenergic agonists
Inhaled β2 -adrenergic agonists directly relax airway smooth muscle. They are used for the
quick relief of asthma symptoms, as well as adjunctive therapy for long-term control of the
disease.
1. Quick relief:
Short-acting β2 agonists (SABAs) have a rapid onset of action (5 to 30 minutes) and provide
relief for 4 to 6 hours.
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They are used for symptomatic treatment of bronchospasm, providing quick relief of acute
bronchoconstriction. All patients with asthma should receive a SABA inhaler for use as needed.
β2 agonists have no anti-inflammatory effects, and they should not be used as monotherapy for
patients with persistent asthma. Monotherapy with SABAs may be appropriate for patients
with mild, intermittent asthma or exercise-induced bronchospasm.
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Direct acting β2-selective agonists include a/buterol [ai-BYOO-ter-all] and levalbuterol [leh-
vai-BYOO-ter-all]. These agents provide significant bronchodilation with little of the undesired
effect of a or β2 stimulation. Adverse effects, such as tachycardia, hyperglycemia,
hypokalemia, hypomagnesemia, and β2- mediated skeletal muscle tremors are minimized with
inhaled delivery versus systemic administration.
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2. Long-term control:
Salmeterol [sai-MEE-ter-all] and formoterol [for-MOE-ter-all] are long-acting β2-agonists
(LABAs) and chemical analogs of albuterol. Salmeterol and formoterol have a long duration of
action, providing bronchodilation for at least 12 hours. Use of LABA monotherapy is
contraindicated, and LABAs should be used only in combination with an asthma controller
medication, such as an inhaled corticosteroid (ICS).
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10. ICS remain the long-term controllers of choice in asthma, and LABAs are considered to be
useful adjunctive therapy for attaining control in moderate to severe asthma. Some LABAs are
available as a combination product with an ICS (see Figure 39.1 ). Although both LABAs are
usually used on a scheduled basis to control asthma, adults and adolescents with moderate
persistent asthma can use the ICS/formoterol combination for relief of acute symptoms.
Adverse effects of LABAs are similar to quick-acting β2-agonists.
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11. C. Corticosteroids
ICS are the drugs of choice for long-term control in patients with persistent asthma (Figure
39.3). Corticosteroids inhibit the release of arachidonic acid through inhibition of
phospholipase A2 thereby producing direct anti-inflammatory properties in the airways (Figure
39.4). To be effective in controlling inflammation, these agents must be used regularly.
Treatment of exacerbations or severe persistent asthma may require the addition of a short
course of oral or intravenous corticosteroids.
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14. Actions on lung:
ICS therapy directly targets underlying airway inflammation by decreasing the inflammatory
cascade (eosinophils, macrophages, and T lymphocytes), reversing mucosal edema, decreasing
the permeability of capillaries, and inhibiting the release of leukotrienes. After several months
of regular use, ICS reduce the hyperresponsiveness of the airway smooth muscle to a variety of
bronchoconstrictor stimuli, such as allergens, irritants, cold air, and exercise.
Lippincott Illustrated Review Pharmacology 7th Edition
15. Ill. ALTERNATIVE DRUGS USED TO TREAT ASTHMA
These drugs are useful for treatment of asthma in patients who are poorly controlled by
conventional therapy or experience adverse effects secondary to corticosteroid treatment. These
drugs should be used in conjunction with ICS therapy for most patients.
A. Leukotriene modifiers:
Leukotrienes (LT) 84 and the cysteinylleukotrienes, LTC4, LTD4, and LTE4, are products of
the 5-lipoxygenase pathway of arachidonic acid metabolism and part of the inflammatory
cascade.
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5-Lipoxygenase is found in cells of myeloid origin, such as mast cells, basophils, eosinophils,
and neutrophils. LTB4 is a potent chemoattractant for neutrophils and eosinophils, whereas the
cysteinyl leukotrienes constrict bronchiolar smooth muscle, increase endothelial permeability,
and promote mucus secretion. Zileuton [zye-LOO-ton] is a selective and specific inhibitor of 5-
lipoxygenase, preventing the formation of both LTB4 and the cysteinylleukotrienes.
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Zafirlukast [za-FIR-Ioo-kast] and montelukast [mon-te-LOO-kast] are selective antagonists of
the cysteinyl leukotriene-1 receptor, and they block the effects of cysteinyl leukotrienes (Figure
39.4). These agents are approved for the prevention of asthma symptoms. They should not be
used in situations where immediate bronchodilation is required. Leukotriene receptor
antagonists have also shown efficacy for the prevention of exerciseinduced bronchospasm.
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Pharmacokinetics:
These agents are orally active and highly protein bound. Food impairs the absorption of
zafirlukast. The drugs undergo extensive hepatic metabolism. Zileuton and its metabolites are
excreted in urine, whereas zafirlukast, montelukast, and their metabolites undergo biliary
excretion.
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B. Cromolyn:
Cromolyn [KRO-moe-lin] is a prophylactic anti-inflammatory agent that inhibits mast cell
degranulation and release of histamine. It is analternative therapy for mild persistent asthma
and is available as a nebulized solution. Because cromolyn is not a bronchodilator, it is not
useful in managing an acute asthma attack. Due to its short duration of action, this agent
requires dosing three or four times daily, which affects adherence and limits its use. Adverse
effects are minor and include cough, irritation, and unpleasant taste.
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C. Cholinergic antagonists
The anticholinergic agents block vagally mediated contraction of airway smooth muscle and
mucus secretion (see Chapter 5). Inhaled ipratropium [IP-ra-TROE-pee-um], a short-acting
quaternary derivative of atropine, is not recommended for the routine treatment of acute
bronchospasm in asthma, as its onset is much slower than that of inhaled SABAs. However, it
may be useful in patients who are unable to tolerate a SABA or patients with asthma-COPD
overlap syndrome.
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lpratropium also offers additional benefit when used with a SABA for the treatment of acute
asthma exacerbations in the emergency department. Tiotropium [tye-oh-TROE-pee-um], a
long-acting anticholinergic agent, can be used as an add-on treatment in adult patients with
severe asthma and a history of exacerbations. Adverse effects such as xerostomia and bitter
taste are related to local anticholinergic effects.
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D. Theophylline
Theophylline [thee-OFF-i-lin] is a bronchodilator that relieves airflow obstruction in chronic
asthma and decreases asthma symptoms. It may also possess anti-inflammatory activity,
although the mechanism of action is unclear. Previously, the mainstay of asthma therapy,
theophylline has been largely replaced with 132 agonists and corticosteroids due to its narrow
therapeutic window, adverse effect profile, and potential for drug interactions. Overdose may
cause seizures or potentially fatal arrhythmias.
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Theophylline is metabolized in the liver and is a CYP1 A2 and 3A4 substrate. It is subject to
numerous drug interactions. Serum concentration monitoring should be performed when
theophylline is used chronically.
E. Monoclonal antibodies
Omalizumab [OH-ma-LIZ -oo-mab] is a monoclonal antibody that selectively binds to human
immunoglobulin E (lgE).
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This leads to decreased binding of lgE to its receptor on the surface of mast cells and basophils.
Reduction in surface-bound lgE limits the release of mediators of the allergic response. The
monoclonal antibodies mepolizumab [MEP-oh-LIZ-ue-mab], benralizumab [ben-ra-LIZ-ue-
mab], and reslizumab [res-LIZ-ue-mab] are interleukin-5 (IL-5) antagonists. IL-5 is the major
cytokine involved in recruitment, activation, and survival of eosinophils in eosinophilic
asthma.
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These agents are indicated for the treatment of severe persistent asthma in patients who are
poorly controlled with conventional therapy. Their use is limited by the high cost, route of
administration (IV for reslizumab and subcutaneous for others), and adverse effect profile.
Inhaled ipratropium [IP-ra-TROE-pee-um], is not recommended for the routine treatment of acute
bronchospasm in asthma, as its onset is much slower than that of inhaled SABAs.
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It may be useful in patients who are unable to tolerate a SABA or patients with asthma-COPD
overlap syndrome. lpratropium offers additional benefit when used with a SABA for treatment
of acute asthma exacerbations in the emergency department. Tiotropium [tye-oh-TROE-pee-um],
can be used as an add-on treatment in adult patients with severe asthma and a history of
exacerbations.
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27. IV. DRUGS USED TO TREAT CHRONIC OBSTRUCTIVE
PULMONARY DISEASE
Drug therapy for COPD is aimed at relief of symptoms and prevention of disease progression.
A. Bronchodilators
Inhaled bronchodilators, including the P2-adrenergic agonists and anticholinergic agents
(muscarinic antagonists), are the foundation of therapy for COPD (Figure 39.5). These drugs
increase airflow, alleviate symptoms, and decrease exacerbations. The long-acting
bronchodllators,
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LABAs and long-acting muscarinic antagonists (LAMAs), are preferred as first-line treatment
of COPD for all patients except those who are at low risk with less symptoms. LABAs include
oncedaily indacaterol, olodaterol, and vilanterol, as well as the twice-daily inhaled
formulations of arformoterol, formoterol, and salmeterol. Aclidinium, tiotropium,
glycopyrrolate, and umeclidinium are LAMAs.
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The combination of an anticholinergic and a f32 agonist may be helpful in patients who have
inadequate response to a single inhaled bronchodilator and are at risk of exacerbations.
B. Corticosteroids
The addition of an ICS to a long-acting bronchodilator may improve symptoms, lung function,
and quality of life in COPD patients with FEV1 of less than 60% predicted or patients with
symptoms of both asthma and COPD.
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However, ICS treatment in COPD should be restricted to these patients, since use is associated
with an increased risk of pneumonia. Although often used for acute exacerbations, oral
corticosteroids are not recommended for long-term treatment of COPD.
C. Other agents:
Rof/umi/ast[roe-FLUE-mi-last] is an oral phosphodiesterase-4 inhibitor used to reduce
exacerbations in patients with severe chronic bronchitis.
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31. DRUGS USED TO TREAT ALLERGIC RHINITIS
The mast cells release mediators, such as histamine, leukotrienes, and chemotactic factors that
promote bronchiolar spasm and mucosal thickness.
A. Antihistamines
Oral antihistamine have a fast onset of action and are useful for the management of symptoms
of allergic rhinitis caused by histamine release, such as sneezing, watery rhinorrhea, and itchy
eyes/nose from edema and cellular infiltration.
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B. Corticosteroids
Intranasal corticosteroids, such as bec/omethasone, budesonide, fluticasone, cic/esonide,
mometasone, and triamcinolone, are themost effective medications for treatment of allergic
rhinitis. With anonset of action that ranges from 3 to 36 hours after first dose, intranasal
corticosteroids improve sneezing, itching, rhinorrhea, and nasal congestion.
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C. a-Adrenergic agonists
Short-acting a-adrenergic agonists ("nasal decongestants"), such as phenylephrine, constrict
dilated arterioles in the nasal mucosa and reduce airway resistance. When administered
intranasally, these drugs have a rapid onset of action and show few systemic effects.
Administration of oral a-adrenergic agonists results in a longer duration of action but also
increased systemic effects, such as increased blood pressure and heart rate.
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D. Other agents
Intranasal cromolyn may be useful in allergic rhinitis, particularly when administered before
contact with an allergen. To optimize the therapeutic effect, dosing should begin at least 1 to 2
weeks prior to allergen exposure. Although potentially inferior to other treatments, some
leukotriene receptor antagonists are effective for allergic rhinitis as monotherapy or in
combination with other agents.
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35. VII. DRUGS USED TO TREAT COUGH
A. Opioids
Codeine [KOE-deen], an opioid, decreases the sensitivity of cough centers in the central
nervous system to peripheral stimuli and decreases mucosal secretion. These therapeutic effects
occur at doses lower than those required for analgeIn addition, codeine has addictive potential,
which limits its use. Dextromethorphan [dex-troe-meth-OR-fan] is a synthetic derivative of
morphine that has no analgesic effects in antitussive doses.
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dextromethorphan has a low addictive profile. However, it is also a potential drug of abuse.
Guaifenesin [gwye-FENe- sin], an expectorant, is available as a single-ingredient formulation
and is commonly found in combination cough products with codeine or dextromethorphan.
B. Benzonatate
Suppresses the cough reflex through peripheral action. It anesthetizes the stretch receptors
located in the respiratory passages, lungs, and pleura.
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