pharm agents in pulmonary med II Flashcards

1
Q

anticholinergics summary. MOA, use, and comparison with beta agonists

A

competitive antagonist at muscarinic ACh receptors.
quaternary nitrogen compounds are better tolerated b/c they have less access to the CNS
slower onset than SABAs
helps with COPD chronically and with acute exacerbations of asthma and COPD
esp. important in COPD populations who can’t tolerate the heart side effects of beta agonists

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2
Q

evidence for use of anti-cholinergics in asthma maintenance

A

LABAs and anti-cholinergics help more in pts with uncontrolled asthma than doubling the corticosteroid dose. MAy also lead to a better change in FEV1 and fewer severe exacerbations than standard combo therapy.

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3
Q

Name of anticholinergic I should know

A

tiotropium

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4
Q

evidence for anti-cholinergic use in COPD

A

compared with salmeterol (LABA), see fewer COPD exacerbations

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5
Q

methylxanthines. primary agent

A

theophylline

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6
Q

MOA of theophylline

A

inhibits phosphodiesterase in a non-selective manner to increase cAMP (PDE breaks down cAMP). this leads to bronchodilation

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7
Q

effects of theophylline

A

bronchodilation. Also it is an adenosine antagonist (adenosine is a bronchoconstrictior0, has anti-inflammatory effects, and increases mucociliary clearance.

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8
Q

theophilline limitations

A

very narrow therapeutic rance with non-linear phmacokinetics and variable clearance
may lead to nausea, vomiting, tachycardia, arrhythmias, anxiety, CNS excitation, seizures and death. therefore 4th line treatment

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9
Q

effects of mast cell stabilizers

A

inhibit release of mediators from mast cells after activation (primary mechanism)
also decrease chemotaxis of PMNs, lymphocytes, eosinophils to inhibito bronchospasm and airway inflammation

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10
Q

mast cell stabilizers names

A

cromolyn and nedocromil

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11
Q

advantages and disadvantages of mast cell stabilizers

A

advantages: few side effects, could help with both acute and late onset response
but doesn’t work as well as corticosteroids, so they are second line controller agents and second line for exercised induced bronchospasm (first line is beta agonists)

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12
Q

leukotriene modifiers: 2 approaches and names

A

CysLT1 receptor antagonists: montelukast and zafirlukast

lipo-oxyegenase inhbitor: zileuton

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13
Q

what does the cyst LT receptor do

A

when activated, it promotes mucus production, broncho constriction, edema and eosinophilia. Not responsible for granulocyte chemotaxis

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14
Q

advantages and disadvantages of leukotriene modifiers. include side effects

A

advantages: few side effects, rapid onset, can be taken orally
disadvantages: inconsistent response, rare churg struass. both zafirlukast and zileuton interact with many other drugs. zileuton also can cause hepatic problems.

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15
Q

Role for leukotriene modifiers

A

2nd line for asthma. no role in COPD

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16
Q

Omalizumab

A

anti-IgE Ab that prevents its binding to mast cell membrane to decrease release of mediators when exposed to antigen.

17
Q

Omalizumab disadvantages and use

A

problems: must be administered every 2-4 weeks and is expensive. also may cause anaphylaxis, malignancy, injection site irritation. used for 5-6 level asthma. No use in COPD

18
Q

Roflumilast

A

PDE4 (phosphodiesterase) inhibito. increase cAMP and decrese PMNs. better FEV1. reduces COPD exacerbations in COPD patients with a history of chronic bronchits and exacerbations

19
Q

problems with foflumilast

A

weight loss, GI intolerabuility, increased suicidality, drug interaction potential. not a big impact on quality of life or symptoms

20
Q

role of antibiotics in COPD

A

macrolids like azithromycin may decrease COPD exacerbations