Prematurity (Raf) Flashcards

1
Q

What are epidemiologic risk factors for RDS?

A
  • GA
  • gender (males worse than females)
  • ethnicity (worse for whites than african American)
  • antenatal steroids (which have decreased incidence and severity of RDS)
  • maternal insulin
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2
Q

What is the typical clinical presentation of RDS?

A

Early onset respiratory distress by 4 hours, worst at 24-36 hours, improved at 36-48 hours
(endogenous surfactant production starts at 24 hours)

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3
Q

What are the CXR manifestations of RDS?

A
  • Low lung volumes
  • Diffuse ground glass (reticulonodular)
  • Air bronchograms
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4
Q

Pathologic features of new BPD?

A
  • Fewer, larger and simplified alveoli
  • Fewer arteries, but dysmorphic
  • Less regional heterogeneity
  • Rare airway epithelial lesions
  • Mild airway smooth muscle thickening
  • rare fibroproliferative changes
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5
Q

Pathologic features of old BPD?

A
  • heterogeneous: alternating atelectasis with hyperinflation
  • severe airway epithelial lesions
  • market airway smooth muscle hyperplasia
  • extensive diffuse fibroproliferation
  • hypertensive remodelling of pulmonary arteries
  • decreased alveolarization and surface area
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6
Q

Definition for BPD?

A
  • Need for oxygen >21% for at least 28 days
  • Time point for assessment:
    <32 weeks: assess at 36 weeks or discharge, whichever is sooner
  • > 32 weeks: assess at 56 days or discharge, whichever is sooner
    (need to go with sooner since the patient will be discharge, so need to classify before discharge)
  • Mild: no oxygen
  • Moderate: <30% fiO2
  • Severe: >30% fiO2 +/- PPV/CPAP
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7
Q

Why are old and new BPD different?

A

Old BPD: infants were born in late saccular stage. Lung injury was due to hyperoxia, ventilator induced lung injury, inflammation, infection
New BPD: mid to late cannalicular stage, mainly due to aberrant lung development. With antenatal steroids, surfactant and gentl ventilation, less old BPD.

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8
Q

Properties of chyle?

A
  • Chylothorax = accumulation of lymphatic fluid in the pleura
  • Lymph generally drains into thoracic duct
  • Sudan IIIn stain positive for fat globules
  • Triglycerides >1.1 mmol/L
  • High lymphocyte content (>80%)
  • sterile
  • fat content higher than plasma
  • electrolytes, BUN, glucose similar to plasma
  • meets the criteria for an exudate
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9
Q

Differential diagnosis of neonatal chylothorax?

A
  • congenital: Down’s, Noonan, Turner
  • Hydrops fetalis
  • Injury to thoracic duct - either congenital (eg. birth trauma), post operative
  • congenital lymphatic abnormality - eg. lymphangiectasis, lymphangioma
  • Increased central venous pressure pressure - eg. post fontan, thrombosis of SVC
  • Chylothorax in general: lymphoma, teratoma, neuroblastoma, TB, histoplasmosis, sarcoid
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10
Q

If neonatal chylothorax is not improving with conservative management, what are next investigations?

A
  • Lymphangiography to localize a site of lymphatic leak
  • CT scan - may see thickened interlobular septa with lymphangiectasia, but can’t visualize lymphatics on CT scn (I’m not sure if this finding is specific to lymphangiectasia)
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11
Q

Lymphangioma versus lymphangiomatosis versus lymphangiectasia?

A

Lymphangioma: abnormal proliferation of lymphatic vessels, forming a cyst
Lymphangiomatosis: multiple lymphangiomas, which can be in lung, liver, spleen, mediastinum
Lymphangiectasia: dilated lymphatic channels, which impair drainage. Can be primary or secondary (due to increased venous back pressure such as in heart failure or portal hypertension

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