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ASTHMA

ASTHMA. Pediatric Critical Care Medicine Emory University Children’s Healthcare of Atlanta. Asthma. Episodes of increased breathlessness, cough, wheezing, chest tightness. Exacerbations may be abrupt or progressive

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ASTHMA

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  1. ASTHMA Pediatric Critical Care Medicine Emory University Children’s Healthcare of Atlanta

  2. Asthma • Episodes of increased breathlessness, cough, wheezing, chest tightness. • Exacerbations may be abrupt or progressive • Always related to decreases in expiratory (also in inspiratory in severe cases) airflows • Hallmarks: airway inflammation, smooth muscle constriction and mucous plugs

  3. Epidemiology • Most common chronic disease in the world: varies between regions • More prevalent in westernized countries but more severe in developing countries • Yr of cost 2005 >$11.5 billion per year • 35/100.000 fatality, mostly pre-hospital & older pop • Seasonal exacerbation pattern but ICU admission remains constant • <10% life threatening exacerbation: 2-20% with ICU admission; 4% intubation • Reduction in mortality (63%) in the 1980’s due to inhaled steroids

  4. Asthma Prevalence

  5. Pathophysiology • Airway inflammation, smooth muscle constriction, and airway obstruction • VQ mismatch (<0.1)- decrease vent with normal perfusion • Intrapulmonary shunt is prevented due to collateral ventilation, hypoxic pulmonary vasoconstriction, rarely functionally complete obstruction  mild hypoxemia • Worsening of hypercapnea is indicative of impending respiratory failure in combination of lactic acidosis • Worsening of hypoxemia after beta-agonist is common due to removal of hypoxic induced pulmonary vasoconstriction

  6. Asthma

  7. Histamine Tryptase PGD2 LTC4 IL-4 IL-5 IL-6 TNF-α IL-3 IL-4 IL-5 GM-CSF Eosinophilic cationic proteins Major basic proteins Platelet activating factor LTC4, LTD4, LTE4

  8. Pathophysiology • Lactic acidosis: • Changes in glycolysis due to high dose beta agosist; • Increased wob, anaerobic metabolism • Coexisting profound tissue hypoxia • Over production of lactic acid by the lungs • Decrease lactate clearance due to hypoperfusion

  9. Pathophysiology • Significantly reduced: FEV1; FEV1/FVC, Peak expiratory flow; maximal expiratory flow at 75%, 50% and 25%, and maximal exiratory flow between 25% and 75% of the FVC • Abnormally high airway resistance: 5-15x normal due to shortening of airway smooth muscle, airway edema and inflammation, excessive luminal secretions.

  10. Pathophysiology • Dynamic hyperinflation: Auto PEEP (intrinsic positive end expiratory pressuse PEEPi): directly proportional to minute ventilation and the degree of obstruction • Shifts tidal breathing to the less compliant part of the respiratory system pressure volume curve • Flatten diaphragm  reduces the generation of force • Increase dead space  increase minute ventilation for adequate ventilation • “Silent chest”: lower inspiratory flow due to dynamic hyperinflation • Asthma increases all three components of respiratory system load: resistance, elastance and minute volume • Diaphragmatic blood flow is reduced  worsening of respiratory distress

  11. Pathophysiology • CV effects: “pulsus paradoxus” – decrease arterial systolic pressure in inspiration) >12mmHg • Expiration: increase in venous return, rapid RV filling  shifting of interventricular septum causing LV diastolic dysfunction • Large negative intrathoracic pressure: increase LV afterload by impairing systolic emptying. • Pulmonary pressure increases due to hyperinflation  increase RV afterload

  12. Clinical Presentation • Respiratory distress: sitting upright, dyspneic & communicate using short phrases • Severe obstruction: rapid, shallow breathing and use of accessory muscles • Life threatening: cyanosis, gasping, exhaustion, hypotension and decreased consciousness • PE: inspiratory & expiratory wheezes  silent chest • Intensity of wheezing is not a predictor of respiratory failure • Mild hypoxemia • Blood gas: hypoxemia, hypocapnea & respiratory alkalosis in mild asthma • Normocapnea & hypercapnea: impending respiratory failure

  13. Clinical Presentation • Baseline PEF and FEV1 are important • PEF 35-50% of predicted value: acute asthmatic exacerbation • Pre-treatment FEV1 or PEF <25% or post treatment <40% predicted: indication for hospitalization

  14. Treatment • Oxygen • β-agonists • Corticosteroids • Magnesium sulfate • Anticholinergics • Methylxanthines • Leukotriene modulators • Heliox • Mechanical ventilatory support

  15. Treatment • Oxygen: supplement to keep sat>90% • Severe hypoxemia is uncommon • Careful with 100% oxygen supplementation: may result in respiratory depression followed by carbon dioxide retention

  16. Treatment • β-agonists: albuterol, terbutaline; levalbuterol, epinephrine, terbutaline • Mediate respiratory smooth ms relaxation • Decrease vascular permeability • Increase mucocilliary clearance • Inhibit release of mast cell mediator • Onset is rapid, repetitive or continuous administration produces incremental bronchodilation • MDIs: with spacer device have similar effects to nebulizer • Aerolized: • Utilize adequate flow rate (10-12L/min): higher flow rate, smaller particles (0.8-3 μm are deposited in the small airway, smaller particles tend to be exhaled) • Continuous: more consistent delivery and allow deeper tissue penetration

  17. Treatment • β-agonists : • 1- Salbutamol (albuterol): racemic mixture equal R & S isomers • S-form has longer half life and pulm retention; pro-inflammatory properties • More accumulative SE • 2- Levosalbutamol (levalbuterol): R-salbutamol • Can be beneficial after S-form accumulate with SE • Can evoke 4x bronchodilation effects with 2x systemic SE • Genetic variations in β2-adrenergic receptors: may respond favourably to neb. epinephrine

  18. Treatment • β-agonists : • 3- Epinephrine: • Alpha 1 adrenergic receptor: microvascular constriction  decrease edema • Decreases parasympathetic tone  bronchodilator • Improves PaO2 • SQ epinephrine • SQ terbutaline: loose β2 effect, can cause decrease uterine blood flow and congenital malformations in pregnant patients • Side effects • CV: MI especially in IV isoprenaline (isoproterenol) • Hypokalemia • Tremor • Worsening of ventilation/perfusion mismatch

  19. Treatment • Corticosteroids: • Decrease inflammation • Increase the number and sensitivity of Beta-adrenergic receptors • Inhibit the migration and function of inflammatory cells (esp. eosinophils) • No inherent bronchodilator • Administer within 1 hr of onset: lower hospitalization rate, improve pulm functions • Onset of action: 2-6 hrs • Dose 40mg/day, limited evidence of additional efficacy of 60-80mg/day • SE: hyperglycemia, hypokalemia, mood alteration, hypertension, metabolic alkalosis, peripheral edema

  20. Treatment • Magnesium sulfate: direct smooth ms relaxation and anti-inflammation • Controversies in inhaled mag. sulfate • 40mg/kg/dose Q6, max 2gm in adults • Anticholinergics: ipratropium bromide • selective for muscarinic airway (proximal airway), absence of systemic effects • Slow onset of action: 60-90 min, less bronchodilation

  21. Treatment • Methylxanthines: theophyline and aminophyline • Mechanism of actions: phosphodiesterase inhibitor; stimulate endogenous catecholamine release; beta adrenergic receptor agonist and diuretic, augment diaphragmatic contractility; increase binding of cyclic adenosine monophosphate ; prostaglandins antagonist • No additional benefit in acute attack

  22. Treatment • Leukotriene modulators: • Potent lipid mediators derived from arachidonic acid with the 5-lipoxygenase pathway • 2 main groups: LTB4 and cysteinyl leukotrienes (CysLTs): LTC4, LTD4, LTE4 • Mediators in allergic airway disease • CysLTs: produce: bronchoconstriction, mucous hypersecretion, inflammatory cell recruitment, increased vascular permability, proliferation of airway smooth ms • Less potent in bronchodilation and anti-inflammatory than long acting beta agonist and steroids • Administration of single IV dose or PO doses showed improvement in acute attacks

  23. Treatment • Heliox: 60-80% blend • Laminar flow, increase ventilation, decrease wob, pulsus paradoxus and A-a gradient, delay onset of respiratory muscle fatigue • Controversies in benefits • In mechanical ventilated patients, heliox helps to lower peak inspiratory pressure, improve pH and PCO2 (Shamel et al. Helium-oxygen therapy for pediatric acute sever asthma requiring mechanical ventilation. Pediatr Crit Care Med 2003:(4))

  24. Treatment • Non invasive positive pressure ventilation • Decrease wob and auto-peep • Improve comfort, decrease need for sedation, decrease VAP and LOS • No benefits of positive pressure in delivering nebulized meds (Caroll, C. Noninvasive ventilation for the treatment o facute lower respiratory tract disease in children. Clin Ped Emerg Med) • Risks: aspiration, gastric distension, barotrauma • NIPPV + conventional managements associated with improved lung function and faster alleviation of the symptoms (Soroksy, A. et al. A pilot prospective, randomized, placebo-controlled trial of bilevel positive airway pressure in acute asthmatic attack. Chest 2003; 123:1018-25)

  25. Treatment • Mechanical ventilation • Avoid excessive airway pressure, min hyperinflation • Permissive hypercapnea, low TV, low rate, short I-time • Continuous sedation and NMB as needed • Low PEEP vs High PEEP (overcome the critical closing pressure facilitated exhalation)

  26. Treatment • Inhalational Anesthetics: Halothane, Isoflurane • Beta adrenergic receptor stimulation, increase in cAMP – ms relaxation; impede antigen-antibody mediated enzyme production and the release of histamine from leukocytes • Continuous administration: • SE: myocardial depression and arrhythmias (Vaschetto, R. et al. Inhalational Anesthetic in Acute Severe Asthma. Current Drug targets, 2009, 10, 826-32)

  27. Treatment • ECMO • When all treatment modalities failed • V-V ECMO: facilitates CO2 removal; CV stabilization; short run • Complications: brain death or CNS hemorrhage and cardiac arrest (Mikkelsen ME et al. Outcomes using extracorporeal life support for adult respiratory failure due to status asthmaticus. ASAIO J 2009; 55:47-52)

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