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Pediatric Respiratory Emergencies Mohammed Al Faifi, MD. Director, Emergency Out-Reach Program King Faisal Specialist Hospital & Research Centre Riyadh, KSA Kuwait, Oct. 2011 Pediatric Respiratory Emergencies Part 1 Emergency Management of Asthma QUALITY OF CARE OF ED RESPIRATORY ILNESS Data on visits to EDs by children – 1 -19 years of age with moderate/severe asthma – 3 months to 2 years of age with bronchiolitis – 3 months to 3 years of age with croup Knapp et al. Pediatrics 2008 Results Corticosteroids 69% of the 405,000 visits for moderate/ severe asthma Antibiotics 53% of the estimated 228,000 annual visits for bronchiolitis Radiographs 72% of bronchiolitis visits 32% of croup visits 31% of the estimated 317,000 annual croup visits Knapp et al. Pediatrics 2008 Conclusions Physicians treating children with Asthma, bronchiolitis and croup In USA Emergency Departments are under using known effective treatments and overusing ineffective or unproven therapies and diagnostic tests. Knapp et al. Pediatrics 2008 Pediatric Respiratory Emergencies Part 1 Emergency Management of Asthma Introduction Asthma is the most common chronic disease seen in children Emergency department (ED) visits by children with acute asthma are a common occurrence The overall goal of asthma care in the ED is to integrate with home, outpatient, and inpatient care whenever possible Recognition of high-risk patients with acute asthma is essential. History Initial history is brief, focused • Duration of symptoms • Severity of symptoms • Medication use More comprehensive history follows • Triggers • Fever • Systemic Review Past Medical History Previous wheezing Prior admissions for wheezing Prior admissions to ICU Chronic lung disease Physical Examination Level of consciousness Vital signs Degree and symmetry of wheezing Inspiratory and expiratory ratio Accessory muscle use Differential Diagnosis Bronchiolitis Foreign body aspiration Gastroesophageal reflux Cystic fibrosis Anaphylaxis Pulmonary Index Score* Score R.R* 0 < 30 1 Wheezing† I/E Ratio Acc.Muscle use O2 Sat. None 2:1 None 99-100 31 - 45 End expiration 1:1 + 96 -98 2 46 - 60 Entire expiration 1:2 ++ 93- 95 3 > 60 Inspiration and expiration without stethoscope 1:3 +++ < 93 * For patients aged 6 or older: through 20, score 0; 21 through 35, score 1; 36 through 50, score 2; > 50, score 3. † If no wheezing due to minimal air entry, score 3. Pulse Oximetry Noninvasive and inexpensive Can help to predict the need for hospitalization Obtain for moderately to severely ill children Supplement with oxygen if SaO2 < 92% CXRs CXRs for First Time Wheezers 371 children > age 1 94% CXRs normal 20/21 abnormal films would have been identified by: • RR > 60 • HR> 160 • Fever • Focal exam Gerschel, N Engl J Med 1983 Chest Radiographs Focal findings Fever Severe disease Treatment Options Beta2-agonists • Inhaled (nebulizer vs. metered-dose inhaler) • Subcutaneously • Intravenously Corticosteroids • • • • Orally Nebulized Intramuscularly Intravenously Ipratropium bromide Magnesium sulfate Beta2-Agonist Delivery Beta2-agonists remain the standard of care for treatment of acute asthma They should be administered every 20 mins, in the first hour of care Delivery by SVN or MDI with holding chamber are each reasonable options Steps should be taken to insure optimal drug delivery Beta2-Agonist Optimizing Delivery Small particles Mouthpiece Low inspiratory flow rate Breath-holding Ipratropium Bromide An anticholinergic Low lipid solubility Less than 1% absorbed Safe, inexpensive Most studies show that IB plus a Beta2 agonist is superior to Beta2 agonist alone Ipratropium Bromide Group 1 A, P A, P A, P Group 2 A, I A, P A, P Group 3 A, I A, I A, I 0 20 40 Time (mins.) Schuh, et al. J.Pediatrics 1995;126:639-645 Ipratropium Bromide Ipratropium plus Beta2 agonist is superior to Beta2 agonist alone Multi-dose ipratropium is superior to single dose Safe, inexpensive Peak effects are in 40-60 minutes Schuh, et al. J.Pediatrics 1995;126:639-645 Ipratropium Bromide Recommendations For children with a moderate or moderate-to-severe exacerbation or for those already receiving Beta2 agonist therapy : • 250-500 ug of ipratropium bromide by nebulization to be administered concurrently with the albuterol treatments Scarfone, et al, Pediatrics 1993; 92: 513-518 Randomized, double-blind, placebo 75 children in the ED with a moderate to severe asthma attack 2mg/kg oral prednisone vs. placebo Conclusions: Scarfone, et al Oral Corticosteroids: Decreases hospitalization rate Effective within 4 hours Augments Beta2-agonists therapy Oral vs IV Steroid Randomized, double-blinded, placebo 49 Children in ED with moderate to severe acute asthma 2mg/kg methylprednisolone: Oral vs IV Barnett, et al. Ann Emerg Med, 1997; 29 :212-217 Barnett, et al. •Results After 4 hours, there were no differences between the two groups with respect to: • Hospitalization rate • FEV1 • Pulmonary index score • Oxygen saturation • Respiratory rate Oral Prednisone vs. Oral Dexamethasone 533 children in ED with mild, moderate, or severe asthma All got q 20 min RA and IB, in first hour Prednisone - 2 mg/kg in ED - 1 mg/kg for 4 days Dexamethasone - 0.6 mg/kg in ED - 0.6 mg/kg for 1 dose, on day 2 Qureshi F .J Pediatrics 2001 Oral Prednisone vs Oral Dexamethasone Pred. Dex. Admit, from ED 12% 11% Relapse 7% 7% Admit, after relapse 17% 20% Symptoms at 10 days 21% 22% Vomited in ED 3% 0.3 Noncompilance 4% 0.4 Qureshi F .J Pediatrics 2001 Moderate Asthma Treatment Recommendations Beta2 agonists may be delivered by SVNs or MDIs with holding chambers Ipratropium bromide should be given as a single dose or concurrently with first 3 Beta2 agonist treatments Prednisone should be given early ASAP -If emesis • Methylprednisolone IV • Dexamethasone: orally or IM Management of Moderate Asthma Albuterol nebulization or MDI Prednisone1 O2 If Pulse Ox < 92% Albuterol q20-30 mins. Ipiatropium with albuterol No improvement Hospitalize Marked Improvement Slightly improved Discharge home Continue albuterol q30 mins. Disposition Disposition Discharge : PEF > 70% predicted, Symptoms are minimal or absent, Sufficient medications can be prescribed and maintained Outpatient care can be established within a severaldays time frame EDUCATION.. Disposition Observed for 30 to 60 minutes for symptom recurrence hospitalization : prior history of a sudden, severe exacerbation prior intubation or ICU Admission ≥ two hospitalizations in the past year current steroid use or recent wean from steroids medical or psychiatric comorbidity low socioeconomic status or urban residence POST EMERGENCY DEPARTMENT CARE Short-term Medications - Beta-agonist Therapy - Corticosteroids - Inhaled steroids Education Pulmonary Index Score* Score R.R* 0 < 30 1 Wheezing† I/E Ratio Acc.Muscle use O2 Sat. None 2:1 None 99-100 31 - 45 End expiration 1:1 + 96 -98 2 46 - 60 Entire expiration 1:2 ++ 93- 95 3 > 60 Inspiration and expiration without stethoscope 1:3 +++ < 93 * For patients aged 6 or older: through 20, score 0; 21 through 35, score 1; 36 through 50, score 2; > 50, score 3. † If no wheezing due to minimal air entry, score 3. Severe Asthma No wheezing 3 Unable to speak Dyspnea Markedly prolonged expiratory phase 3 Significant work of breathing with Retractions 2 Requires oxygen 3 2 Severe Asthma Initial management Oxygen (consider non-rebreather) Inhaled beta2-agonist Inhaled ipratropium bromide Intravenous corticosteroids ASAP Oxygen Simple face mask • An oxygen flow rate of 6-10 L/min should provide an oxygen concentration of 35-60% • Limitations: open exhalation ports allow for the inspiration of room air and exhaled carbon dioxide is rebreathed. Oxygen Non. re-breathing face mask Modifications allow for greater oxygen delivery to the patient. These include: Exhalation ports serving as one-way valves. A reservoir bag with a one-way valve that diverts oxygen-poor exhaled gases thereby maintaining a mix of almost pure oxygen. With flow of 10-12 L/min and proper fitting mask, oxygen concentrations > 90% can usually be achieved. Subcutaneous Terbutaline Uncooperative, anxious young children Very poor inspiratory flow or aeration Poor response to initial nebulized albuterol Continuously Nebulized Albuterol Advantages: • Easier to adhere to • Less respiratory therapy time • Safe • May benefit sicker patients Disadvantages: • Patients may go unobserved • Claustrophobic mask Corticosteroids IV Methylprednisolone ASAP Magnesium Sulfate Is It Safe • Mild side effects during infusion: Facial flushing, nausea, dry mouth, malaise • Significant adverse effects have not been reported • Hypotension and cardiac conduction disturbances are seen only with serum magnesium levels > 8 mg/dl Magnesium Sulfate Conclusions • The routine administration of magnesium to moderately to severely ill asthmatic children as an adjunct to initial treatment with albuterol and corticosteroids was not efficacious. • Future studies will be needed to determine the optimal dose of magnesium, the optimal duration of infusion, and the subgroup of asthmatic children most likely to benefit from magnesium. • Severely ill asthmatics experience the greatest benefit from magnesium IV Beta2 Agonists Recommendations: • Not recommended as a first-line agent even for severely ill children • For severely ill who are poorly responsive to initial measures IV Terbutaline 10 ug/kg over 10 minutes; infusion 0.5 ug/kg/min Increase by 0.2 ug/kg/min to max of 5ug/kg/min Largely empiric Expect side effects at therapeutic doses titrate to effect Decrease infusion rate by 50% if patient is receiving theophylline IV Beta2 Agonists Potential Toxicities Tachycardia Hyperglycemia Dysrhythmia Hypokalemia Hypertension Rhabdomyolysis Myocardial ischemia Lactic acidosis Severe Asthma Other Considerations Arterial blood gas Heliox Intubation -ketamine -Decompress stomache -Beware of barotrauma -Permissive hypercapnia -Low tidal volumes and peak pressures -Slow rate, no PEEP, I/E ratio=1/3 Inhaled nitic oxide Nakagawa et al, J Pediatr 2000 Severe Status Asthmaticus Vital Signs & oxygen saturation Supplemental Oxygen 0.15mg/kg albuterol by nebulization 250-500 micgm Ipratropium Bromide Poor response Good response 0.01cc/kg of subcutaneous terbutaline Continue with approach to moderately ill patient 2mg/kg IV Methylprednisolone Continuously nebulized albuterol 75mg/kg IV Magnesium sulfate IV Terbutaline infusion Clinical Role of MDI’s When used with a (mask) spacer device, multiple pediatric studies show MDI effectiveness comparable to nebulization therapy • Chou et al. Arch Pediatr Adolesc Med 1995 • Williams et al. Pediatr Emerg Care 1996 • Leversha et al. J Pediatr 2000 • Delgado et al. Arch Pediatr Adolesc Med 2003 MDI / Spacer Tips • 10 puffs or detergent wash to eliminate electrostatic charge of new spacer – Avoids initial 70% delivery reduction • Shake MDI before each puff, administer 1 puff at a time one minute apart, 5 tidal breaths per puff – 6 puffs / rx for acute exacerbation (Q 20” x 3) – 2 puffs / rx for maintenance (Q 3-6 hours) • Count total puffs per MDI (200 std.) – “shake” or “float” tests unreliable Dexamethasone in Asthma • Random, non-blinded, 3-16 years, N = 42 • IM dexamthasone, 0.3 mg/kg (up to 15 mg), effective as 3 day course of oral prednisone, 2 mg/kg/day • Oral dexamethsone 0.6 mg/kg (up to 16 mg) x 2 days vs. pred x 5 days. Similar efficacy fewer side effects. Klig et al. J Asthma 1997 and Qureshi et al. J Pediatr 2001 Magnesium Sulfate • Bronchodilation through smooth muscle relaxation • Inhibits cellular calcium uptake • Inhibits histamine release Mg IV vs. Placebo • RCT (double blind), placebo, 1-18 yrs, N=54 • Mg 75 mg/kg IV over 20 minutes vs. placebo after 1st albuterol • No different in PFTs or admit rate • No adverse effects or BP changes with Mg Scarfone et al. Ann Emerg Med 2000 IV Magnesium Sulfate in Asthma • Meta-analysis of 5 RCTs (with placebo) • 182 pediatric patients with moderate to severe asthma • Received beta agonists and steroids • Mg prevents hospitalization (NNT = 4) • Short term PFTs and clinical scores improved • ? Dose, 25-75 mg/kg over 20 minutes Cheuk et al. Arch Dis Child 2005 PICU Case Reports • 3 children in status asthmaticus • Maximized traditional therapy • Failure to improve after 2-3 hours • BiPAP delivered an average of 12-17 hours • Resolution of hypercarbia, and improved clinical state • 2/3 used continuous IV ketamine as adjunct Olugbenga A, et al. Pediatr Crit Care Med 2002 Factors Associated with Long Asthma Therapy • Previous ICU admit • Baseline sat ≤ 92% • Higher ( 6 / 9 ) clinical asthma score at four hours • 4 hour sat ≤ 92% • 4 hour albuterol more often than q1 hour • If none, 82% chance short therapy only • ≥ 3 predictors 92% chance long therapy Keogh et al. J Pediatr 2001