Asthma Flashcards
asthma
- quite prevalent
- can be associated with COPD
- reversible recurrent episodes of a/w obstr d/t:
- muscle hyperactivity -> bronchospasm to decrease inhalation of the trigger
- inflmtn -> exudate + swelling = compromised lumen of a/w
what type of inflammation do you have with asthma?
chronic infltm of the a/w
- known trigger, if encountered will cause bronchospasm and inflammation, but the pt will be hyperresponsive to other unknown triggers
- reversible, recurrent bronchospasm (a/w locks in a constricted state)
forms of asthma?
- Atopic (Extrinsic) Form
- atopy = genetic tendency to develop allergic diseases (ie. allergic asthma)
- typically associated with heightened IR to common allergens, esp inhaled and food allergens - Non-Atopic (Intrinsic) Form
- responses to triggers that are not genetically based
etiology
- complex trait, but has triggers that induce episodes; genetic and environmental factors
- hypersensitivity to certain stimuli = hyperresponsiveness
–> exercise, allergens, strong odours, a/w irritants
–> 2 categories of stimuli are inflmtry and
bronchospastic - T2H differentiation
- -> T2H responds to inhalation of allergens
patho
- you have chronic inflmtn so there’s always some WBCs present, but its not until the late phase that the WBCs enter the submucosa
- a/w becomes more hyperresponsive to other allergens/triggers = more bronchospasm and airflow limitation
- have either early or late phase, one doesn’t lead into the other
acute phase response
- can last up to 1 hr
i. inhaled allergen -> previously sensitized mast cell degranulates -> IgE mediated release of inflm mediators -> causes infiltration of inflm cells and bronchospasm (limits airflow) but inflm cells do not move into the submucosa
ii. prior sensitization to allergen (T1 HS)
iii. subsequent exposure -> IgE binds to sensitized mast cells -> mast cells on surface of submucosa release inflm mediators -> inflmtn
iv. intercellular junctions open -> allergens enter submucosa
v. increased capillary permb and mucous hypersecretion -> edema of the a/w d/t exudate from inflmtn
vi. bronchospasm (via PNS) = reflex resulting in dyspnea and wheezing; person will have a response to irritants but compromise their breathing
vii. bronchoconstriction = attempt at compensation, but is not beneficial
late phase response
- can last up to days, self-sustaining cycle
- 1/2 of people with asthma will experience this
i. infmtn of a/w is worsened -> edema, inflm damage, and hypersecrection of mucous resulting in decreased mucociliary fx -> limits airflow even further
ii. T1H, but response is delayed post-exposure (peaks 4-8 hours)
iii. pt. becomes hyperresponsive to new triggers
iv. causes an influx of inflm cells
- inflm damage to epithelial cells
- compromises mucociliary blanket (decreased
defense = increased susceptibility to infection)
- frequent, severe triggers
v. beta adrenergic receptors = bronchodilation to increase breathing for fight or flight response
- asthmatics lack B-receptor stimulation
(bronchodilation doesn’t occur when its required)
vi. alpha adrenergic receptors = bronchoconstriction
- binding to both of these receptors is mediated by cAMP
manifestations
- wide range of intensity (ie. immobilization)
- dyspnea, wheezing, cough
- increased resp effort and compromised breathing
- abnormal ABG profile (increased PaCO2)
diagnosis
- Hx, Px
- labs (CBC, ABGs)
- pulmonary fx tests
- inhalation challenge tests
inhalation challenge tests
assess a/w responsiveness to different substances; gold standard for dx asthma
treatment
- shift from episodic to chronic management
- prophylactic management (smoking cessation, avoid allergens and irritants)
- drugs
explain what drugs you would use for treatment of asthma
i. short acting b-agonist (bronchodilator) inhaled prn
ii. add inhaled steroid (decrease inflmtn) -> local not systemic
iii. add long-acting bronchodilator (inhaled) to steroid
iv. short course of PO steroids to deal with acute flare-ups + add a 3rd drug (leukotriene receptor antagonist or theophylline)
leukotriene receptor antagonist
inflm mediator and involved in allergic response, so drug inhibits both of these actions
