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Ventilator-Associated Pneumonia

Ventilator-Associated Pneumonia

Ventilator-Associated Pneumonia

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VAP: Definition & Epidemiology - Lungs Under Siege

  • Pneumonia developing >48 hours after endotracheal intubation.
  • Most frequent ICU-acquired infection in mechanically ventilated (MV) patients.
  • Affects 9-27% of intubated individuals; ↑ morbidity & mortality.
  • Types based on onset:
    • Early-onset VAP (EOVAP): <5 days of intubation.
      • Usually antibiotic-sensitive bacteria (e.g., S. pneumoniae, MSSA).
    • Late-onset VAP (LOVAP): ≥5 days of intubation.
      • Often MDR pathogens (e.g., P. aeruginosa, MRSA, Acinetobacter spp.).

⭐ LOVAP: ↑ risk of inadequate initial antibiotics & worse outcomes.

VAP: Pathogenesis & Etiology - How Bugs Sneak In

  • Pathogenesis:
    • Primary: Microaspiration of secretions (oropharyngeal, gastric) past ET tube cuff.
    • Biofilm formation on ET tube: Protects bacteria, promotes resistance.
    • Others: Contaminated aerosols, rarely hematogenous.
  • Etiology:

    Onset TypeTimingCommon Pathogens
    Early-onset VAP<5 daysS. pneumoniae, H. influenzae, MSSA, antibiotic-sensitive Enterobacteriaceae.
    Late-onset VAP5 daysP. aeruginosa, Acinetobacter spp., MRSA, ESBL-producing GNBs (often MDR).
  • Key Risk Factors: Prolonged ventilation, supine positioning, prior antibiotic use, advanced age, stress ulcer prophylaxis (PPIs/H2 blockers).

⭐ Biofilms on endotracheal tubes are a critical factor for VAP development, especially with MDR organisms in late-onset cases.

VAP: Diagnosis - Finding the Foe

  • New/progressive lung infiltrate on CXR + ≥2 clinical signs (fever >38°C, leukocytosis/leukopenia, purulent secretions).
  • Clinical Pulmonary Infection Score (CPIS): Score >6 suggests VAP.
    ComponentPoints
    Temperature0-2
    WBC Count0-2
    Tracheal Secretions0-2
    Oxygenation (PaO2/FiO2)0-2
    CXR Infiltrate0-2
    Tracheal Aspirate Culture0-2
  • Microbiological confirmation (quantitative cultures preferred):
    • Endotracheal Aspirate (ETA): ≥10⁵ CFU/mL
    • Bronchoalveolar Lavage (BAL): ≥10⁴ CFU/mL
    • Protected Specimen Brush (PSB): ≥10³ CFU/mL
  • Chest X-ray: Bilateral infiltrates in ventilated patient
  • Diagnostic Algorithm:
(*Fever, ↑WBC, Purulent Secretions)

⭐ Quantitative cultures of lower respiratory tract samples are preferred over qualitative cultures for VAP diagnosis to reduce inappropriate antibiotic use.

VAP: Management - Fighting Back Smart

  • Initiate empiric antibiotics promptly (within 1 hour of suspicion).
  • Base choice on MDR risk factors & local antibiogram.
  • De-escalate therapy based on culture results.
  • Typical duration: 7 days.

⭐ Quantitative cultures (e.g., BAL >10,000 CFU/mL, PSB >1,000 CFU/mL) preferred to guide VAP therapy.

VAP: Prevention - Keeping Lungs Clear

VAP prevention focuses on meticulous care bundles. Key elements:

  • Head of bed (HOB) elevation: 30-45 degrees continuously.
  • Daily sedation interruption ("sedation vacation") & readiness-to-extubate assessment.
  • Thorough oral care with chlorhexidine (e.g., 0.12% solution q6-12h).
  • Stress ulcer (PUD) prophylaxis.
  • Venous thromboembolism (DVT) prophylaxis.
  • Maintain endotracheal tube cuff pressure at 20-30 $cm H_2O$.
  • Use subglottic secretion drainage (SSD) tubes where possible. VAP prevention bundle strategies and impact on incidence

⭐ Consistent application of VAP bundles can decrease VAP rates by over 50%.

High‑Yield Points - ⚡ Biggest Takeaways

  • VAP: Pneumonia developing >48 hours post-intubation and mechanical ventilation.
  • Common pathogens: P. aeruginosa, Acinetobacter, MRSA, ESBL-producing Enterobacteriaceae.
  • Late-onset VAP (≥5 days) strongly associated with MDR organisms.
  • Diagnosis: New radiographic infiltrate with clinical signs (fever, purulent sputum) & microbiology.
  • Prevention: Key is the VAP bundle (head elevation 30-45°, oral chlorhexidine, sedation holds).
  • Treatment: Empiric broad-spectrum antibiotics, then de-escalate based on cultures.

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