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Respiratory problems in premature infants

Respiratory problems in premature infants. Dr. Rozin Ilya Department of Neonatology Kaplan Medical Center. Respiratory problems. Respiratory Distress Syndrome (RDS) or Hyaline Membrane Diseases (HMD) Broncho-Pulmonary Dysplasia (BPD). Respiratory Distress Syndrome. Definition.

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Respiratory problems in premature infants

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  1. Respiratory problems in premature infants Dr. Rozin Ilya Department of Neonatology Kaplan Medical Center

  2. Respiratory problems • Respiratory Distress Syndrome (RDS) or Hyaline Membrane Diseases (HMD) • Broncho-Pulmonary Dysplasia (BPD)

  3. Respiratory Distress Syndrome

  4. Definition • Also known as hyaline membrane disease • Deficiency of pulmonary surfactant in an immature lung • Common respiratory disorder of premature infants • RDS can also be due to genetic problems with lung development

  5. Epidemiology • Major cause of morbidity and mortality in preterm infants • 20,000-30,000 newborn infants each year ( in US) • Incidence and severity of RDS are related inversely to gestational age of newborn infant (most case before 37 weeks) • 26-28 weeks gestation : 50% • 30-31 weeks gestation : <30%

  6. Epidemiology • Overall incidence in 501-1500 grams: 42% • 501-750 grams: 71% • 751-1000 grams: 54% • 1001-1250 grams: 36% • 1251-1500 grams: 22%

  7. Other risk factors for RDS Increased Risk Decreased Risk Chronic intra-uterine stress Prolonged rupture of membranes Maternal hypertension or toxemia IUGR/SGA Antenatal glucocorticoids Maternal use of narcotics/cocaine Tocolytic agents Hemolytic disease of the newborn • Prematurity • Male gender • Familial predisposition • Cesarean section without labor • Perinatal asphyxia • Caucasian race • Infant of diabetic mother • Chorioamnionitis • Non-Immune hydrops fetalis • Multiple pregnancy (twins or more)

  8. Phases of Lung Development

  9. Lung Development

  10. Surfactant • Complex lipoprotein • Composed of 6 phospholipids and 4 apoproteins • Surfactant contains • 70-80% phospholipids, • 8-10% protein, and • 10% neutral lipids

  11. Surfactant Metabolism

  12. Surfactant Metabolism

  13. 4 surfactant apoproteins • Surfactant protein B (SP-B) • Surfactant protein C (SP-C) for preventing atelectasis, and • Surfactant protein A (SP-A) - facilitates phagocytosis of pathogens by macrophages and their clearance from the airways • Surfactant protein D (SP-D) – if absent -increased surfactant lipid pools in the airspaces and emphysema in mice

  14. Assessment of Fetal Lung Maturity • Lecithin / sphingomyelin (L/S) ratio • Lamellar body counts • Phosphatidylglycerol • After 35 weeks gestation

  15. L/S Ratio

  16. Pathophysiology

  17. Etiology • Preterm delivery • Mutations in genes encoding surfactant proteins • SP-B • SP-C • ATP-binding cassette (ABC) transporter A3 (ABCA3) -is critical for proper formation of lamellar bodies and surfactant function and may also be important for lung function in other pulmonary diseases

  18. Lung Compliance

  19. Normal Lung

  20. Hyaline Membranes

  21. Surfactant Inactivation • Meconium and blood can inactivate surfactant activity (Full-term > Preterm) • Proteinaceous edema and inflammatory products increase conversion rate of surfactant into its inactive vesicular form • Oxidant and mechanical stress associated with mechanical ventilation that uses large TV

  22. Clinical Manifestations • Tachypnea • Nasal flaring • Grunting • Intercostal, sub xiphoid, and subcostal retractions • Cyanosis • Apnea

  23. Differential Diagnosis • TTN • MAS • Pneumonia • Cyanotic Congenital Heart Disease • Pneumomediastinum, pneumothorax • Hypoglycemia • Metabolic problems • Hematologic problems • Anemia, polycythemia • Congenital anomalies of the lungs

  24. Diagnosis • Onset of progressive respiratory failure shortly after birth • Characteristic chest radiograph • Laboratory tests – rule out infection • Analysis of blood gas: • Hypoxia • Hypercarbia

  25. Chest X Ray “ground glass”

  26. Prevention • Antenatal glucocorticoids • Enhances maturational changes in lung architecture and inducing enzymes • Stimulate phospholipid synthesis and release of surfactant • All pregnant mothers at risk for preterm delivery between 24 and 34 weeks gestation should receive ACS

  27. Treatment • Surfactant Therapy • Assisted Ventilation Techniques and Oxygen therapy (be careful) • Supportive Care • Thermoregulation • Fluid Management • Nutrition • Antibiotic therapy • Gentle handling

  28. Prognosis Acute complications of respiratory distress syndrome : • Alveolar rupture • Infection • Intracranial hemorrhage and periventricular leukomalacia • Patent Ductus Arteriosus (PDA) with increasing left-to-right shunt • Pulmonary hemorrhage • Necrotizing enterocolitis (NEC) and/or gastrointestinal (GI) perforation • Apnea of prematurity

  29. Prognosis • Chronic complications of respiratory distress syndrome : • Broncho pulmonary dysplasia (BPD) • Retinopathy of prematurity (ROP) • Neurologic impairment

  30. Bronchopulmonary dysplasia • Bronchopulmonary dysplasia (BPD) is a form of chronic lung disease that develops in preterm neonates treated with oxygen and positive-pressure ventilation (PPV). • The pathogenesis of this condition remains complex and poorly understood.

  31. Pathogenesis

  32. Definition • 1967, Northway et al. : premature infants with RDS, resaved prolonged ventilation, with high concentration of oxygen and high peak inspiratory pressure • All require oxygen at 28 days after birth and progressive change on chest x-ray

  33. Definition • 1979, Bancalari: same to Northway + tachypnea and crackles or retraction. • 1988, new criterion: oxygen supplementation at 36 weeks postmenstrual age (PMA) • - more accurately predicted abnormal pulmonary outcome at 2 years of age • - with medical care more infant with oxygen at 28 days

  34. Definition 2000, National Institute of Child Health and Human Development (NICHD)

  35. Definition • Because of absent specified in the consensus BPD definition, it was recommended that a physiologic test confirming the need for supplementation oxygen be performed

  36. Epidemiology • Incidence: • 42-46% (BW-501-750g) • 25-33% (BW=751-1000g) • 11-14% (BW=1001=1250g) • 5-6% (BW=1251-1500g) • Risk factors: • Prematurity, low BW • White boys • Genetic heritability

  37. Epidemiology • By the NICHD at 2010 from Neonatal Research Network • BW 401-1500 gr • GA 22 0/7 – 28 6/7 weeks • BPD of all diagnosis - 68% • Mild - 27% • Moderate – 23% • Severe – 18%

  38. Pathology • “Old” BPD: • Airway inflammation • Fibrosis • Smooth muscle hypertrophy • “New” BPD: • Lung development arrests before alveolarization: lung have larger but fewer alveoli than normal lung • Pulmonary vasculature to be dysmorphic

  39. Pathology • “Old BPD” (before surfactant and steroids) • Cystic changes, heterogeneous aeration • “New BPD” (after surfactant and steroids) • More uniform inflation and less fibrosis, absence of small and large airway epithelial metaplasia and smooth muscle hypertrophy • Some parenchymal opacities, but more homogenous aeration and less cystic areas • PATHOLOGIC HALLMARKS: larger simplified alveoli and dysmorphic pulmonary vasculature

  40. Pathology • Old BPD: • Airway injury, inflammation and parenchymal fibrosis due to mechanical ventilation and oxygen toxicity • New BPD: • Decreased septation and alveolar hypoplasia leading to fewer and larger alveoli, so less surface area for gas exchange • Dysregulation of vascular development leading to abnormal distribution of alveolar capillaries and thickened muscular layer of pulmonary arterioles

  41. Pathogenesis

  42. Pathogenesis • Chorioamnionitis – caused by an ascending infection, as possible cause • But histologic chorioamnionitisto be protective ( same umbilical vasculitis) – potential role of transcription factor nuclear factor kB and inflammation • Ureaplasma colonization • Bacterial sepsis

  43. Pathogenesis • Hemodynamic significantly PDA and surgery ligation • Mechanical ventilation (volutrauma and barotrauma) • Oxygen toxicity • High volume of fluids intake n the first few days after birth • Lower serum cortisol level (in VLBW) – early adrenal insufficiency

  44. Outcomes • Higher rate recurrent hospitalization in the first year after birth • Lung disease in adulthood: airway obstruction, reactive airways, emphysema • Affect growth • Cardiovascular sequelae: pulmonary artery hypertension, corpulmonale, systemic hypertension • Poor neurodevelopmental outcomes: language delay, increased fine and gross motor impairment

  45. Prevention and therapy • Antenatal: • corticosteroids administration • standard of care – 24 – 34 weeks • effect on the incidence of BPD controversial • in animals studies – arrest alveolarization and microvascular development

  46. Prevention and therapy • Postnatal: • postnatal corticosteroids therapy • decreased time to extubation • early use – poor neurodevelopmental outcomes (CP) • adverse effects: hyperglycemia, hypertension, GI bleeding, hypertrophic cardiomyopathy, infection

  47. Prevention and therapy • Azithromycin • macrolides antibiotic • anti-inflammatory effect • active against Ureaplasma infection • in a RCT no statistic significance (for 6 weeks of therapy)

  48. Prevention and therapy • Vitamin A: • regulation of lung development • injury repair • low level – increased risk to BPD • Vitamin E and Selenium: • study result have been mixed • selenium works synergistically with Vit E to prevent peroxide formation – not show to reduce risk to BPD

  49. Prevention and therapy • Caffeine: • significant reduce in BPD • Pentoxiphilline: • non specific phosphodiesterase inhibitor • decreased pulmonary inflammation • Cromolyn: • mast cell stabilizer • non protective effect

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