Bronchopulmonary Dysplasia- Prevention and Management.ppt
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1、Bronchopulmonary Dysplasia: Prevention and Management,Namasivayam Ambalavanan M.D. Assistant Professor, Division of Neonatology, Department of Pediatrics, University of Alabama at Birmingham Feb 2003,Overview of presentation,Bronchopulmonary dysplasia: a moving target? Pathogenesis Strategies for pr
2、evention of BPD Strategies for management of BPD Outcome Appendix,BPD vs. CLD,Initially labeled “bronchopulmonary dysplasia” BPD Later called “neonatal chronic lung disease” or “chronic lung disease of infancy” CLD Many experts now believe the term “bronchopulmonary dysplasia” is more accurate in de
3、scribing the pathogenesis and that CLD is not a specific diagnosis or description,Introduction,Northway, Rosan, and Porter (1967) :BPD :premature infants who developed RDS, required prolonged mechanical ventilation with high pressures and FiO2. Classic clinical and radiographic course had four stage
4、s: I: RDS, II: dense parenchymal opacification, III: bubble-like pattern, IV: hyperlucency of bases with strands of radiodensity in upper lobes. Currently, a milder form of BPD is more commonly seen in tiny premies who have only mild pulmonary disease not requiring high ventilatory support,Introduct
5、ion,Definitions: 1980s: Oxygen dependence for 28 days or more after birth (Tooley WH. J Pediatr 95: 851-8, 1979) 1990s: Oxygen dependence at 36 wks corrected age (Shennan et al. Pediatrics 82:527-32, 1988) More correlated with abnormal pulmonary outcome at 2 years (63% PPV) vs. 28 d definition (38%
6、PPV). 21st century: New physiologic definition of BPD,Physiologic definition of BPD,Problem with previous definitions: The decision to administer oxygen is not uniform and the definition of acceptable saturation (85-98%) varies. Development of a “room air test” to document the need for oxygen by the
7、 NICHD Neonatal Research Network What is O2 requirement (failure in test)? Saturation 88% for 5 continuous minutes Any saturation 80% on an accurate pulse oximeter reading,Study Design,Baseline phase x 5 min Oxygen reduction phase as per protocol every 10 min with continuous monitoring,O2 reduction
8、phase,Rapid Pass (15 min in RA96%),Rapid Fail (80-88% for 5 min (or) 80% immediate fail,Intermediate: 88-96% in first 15 min. Monitor for total 60 min.,No BPDBPDSome BPD Some No BPD,Incidence,Varies by definition, selection bias, survival Developed countries: NICHD Neonatal Network for 2001 BPD-36 U
9、AB All centers 401-1500g 11% (n=297) 23% (n=3589) 401-1000g 19% (n=154) 39% (n=1517) Developing countries: PGI: BPD-28: 1000g: 50% ; 1000-1249g: 8%; 1250-1499g: 2.3% (Indian Pediatrics Feb 2002),Incidence,UAB statistics (1998-1999) of all live births 34 w (excluding 10 deaths before admission)401-10
10、00 g (2001; n=154): 82% IMV, 73% surf, 16% steroids for BPD,Pathogenesis,Increased Airway Compliance,Pressure/ flow inhomogeneity,Immature cells,surfactant deficiency,DIFFUSE ALVEOLAR DAMAGE,BRONCHOPULMONARY DYSPLASIA,Barotrauma,Infection / Inflammation,RECOVERY,Barotrauma,Infection / Inflammation,P
11、DA O2 Toxicity,Protein leak,Retained fluid,PULMONARY IMMATURITY,Respiratory Distress Syndrome,Prevention of BPD,Ventilatory Strategies Selective intubation / Avoid IMV (Prophylactic IMV bad) Early CPAP Minimal (gentle”) ventilation Early extubation Pharmacologic Strategies Antenatal steroids Vitamin
12、 A supplementation Others Other management: PDA, Infection,Conservative Indication For CV and BPD,Intubation,BPD,Adapted from Poets and Sens*, Gitterman et al., and Lindner et al, de Klerk and de Klerk*.,*and/or mortality,Percent (%),Non-ventilatory strategies for BPD prevention,Antenatal steroids V
13、itamin A supplementation (Tyson et al. NEJM 340:1962, 1999) Avoidance of infections Closure of PDA (but TIPP trial did not show a difference in BPD despite a decrease in PDA from 50 to 24%. Schmidt et al. NEJM 344:1966-72, 2001) Optimal fluid and electrolyte management: moderate water and sodium res
14、triction in first week of life (Tammela et al. Acta Paediatr 81:207-12,1992; Costarino et al. J Pediatr 120: 99-106, 1992; Hartnoll et al 82: F19-23, 2000),BPD Management,Treatment is directed towards major pathophysiology: Pulmonary edema = Diuretics Bronchoconstriction and airway hyperreactivity =
15、 Bronchodilators Airway inflammation = Steroids Cor pulmonale = Vasodilators Chronic lung injury and repair =Antioxidants, nutrition, prevention of infections,Management - Diuretics,DIURETICS: Furosemide + Thiazides When to consider :Babies 1-2 wks w/ mod-severe lung disease on ventilatorBPD w/ volu
16、me overload“Stalled” BPDBPD w/ inadequate nutrition due to fluid restriction,Management - Diuretics,How? Therapeutic trial (Lasix): Give 1 mg/kg iv or 2 mg/kg po/og x 4-5 doses. If no improvement, increase dose. If improvement, give long term. If no improvement, no long term. Eval weekly. Monitor fo
17、r side effects: Fluid-electrolyte balance/ alkalosis/ osteopenia / ototoxic / gall stones. Alternate day Rx may decrease side effects. No evidence to support any long-term benefit (Brion et al. Cochrane Database Syst Rev (1):CD001817, 2002),Management - Bronchodilators,Types of Bronchodilators: Meth
18、ylxanthines ( Theophylline, caffeine ) Bronchodilator, diuretic, resp stimulant weak bronchodilator, increased side effects b-adrenergic agonists ( mainly b2, less b1 ) mainly smooth muscle relaxation, also enhance mucociliary transport, redistribute pulmonary blood flow Anticholinergics - Atropine,
19、 Ipratropium,Management - Bronchodilators,Results: Bronchodilators improve pulmonary function in the short-term. No studies on long-term efficacy Inhaled salbutamol did not prevent BPD in a RCT (Denjean et al. Eur J Pediatr 157:926-31, Nov 1998) Long term safety ? - b receptors in the brain. Is bron
20、choconstriction protective ? Focal bronchoconstriction may have protective action by limiting lung injury to distal units May maintain airway wall rigidity,Management - Vasodilators,VASODILATORS WHY ? Alveolar hypoxia leads to pulmonary vasoconstriction and structural remodeling of the pulmonary vas
21、cular bed. Oxygen a potent vasodilator, main vasodilator used in BPD. Keep PO2 60-80, SpO2 92-95%. Hydralazine, Diltiazem, Nifedipine used in very small trials showed hemodynamic improvement. Nitric Oxide (NO) improves oxygenation in some infants (Pilot study by Banks et al. Pediatrics 103:610-8, Ma
22、r 1999),Management - Steroids,STEROIDS - Widespread use, different regimens HIGH RISK: Use is not recommended WHY ? Anti-inflammatory properties (early) Modulate lung repair (late) HOW ? Early vs Late use Short-term vs Long-term course PO/IV vs Inhaled route,AAP/CPS statement Pediatrics 109: 330-8 F
23、eb 2002,“The routine use of systemic dexamethasone for the prevention or treatment of chronic lung disease in infants with very low birth weight is not recommended” “Outside the context of a randomized, controlled trial, the use of corticosteroids should be limited to exceptional clinical circumstan
24、ces (eg, an infant on maximal ventilatory and oxygen support).”,Summary of systemic dexamethasone for BPD,BPD and BPD/Death are decreased by steroids However, short-term risks are significant No improvement in survival Long-term neurodevelopment is worse in infants treated with steroids (about a 2-f
25、old increase in CP) Alternatives: Low doses of hydrocortisone ? Inhaled steroids ? Other steroids eg. Methylprednisolone ?,RCT OF VITAMIN A IN ELBW INFANTS,CLD or DeathCLD in SurvivorsHospital-acquired sepsisGrade 3/4 IVHDeath, 3/4 IVH, or PVL,Decreased Risk Increased Risk,0.6 0.7 0.8 0.9 1.0 1.1 1.
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