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Oxygen Toxicity

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Oxygen Toxicity - Basics & Breath Woes

Oxygen toxicity refers to the adverse physiological effects resulting from breathing molecular oxygen ($O_2$) at elevated partial pressures ($P_{O_2}$), leading to hyperoxia-induced cellular damage.

  • Types & Thresholds:
    • CNS Toxicity (Paul Bert Effect): Acute. $P_{O_2}$ > 1.6 ATA.
    • Pulmonary Toxicity (Lorrain Smith Effect): Chronic. Prolonged $P_{O_2}$ > 0.5 ATA.

⭐ The two main forms of oxygen toxicity are CNS toxicity (Paul Bert effect), occurring rapidly at $P_{O_2}$ > 1.6 ATA, and pulmonary toxicity (Lorrain Smith effect), developing over longer exposures at $P_{O_2}$ > 0.5 ATA.

  • Pathophysiology:
    • ↑ $P_{O_2}$ → ↑ Reactive Oxygen Species (ROS): $O_2^-$, $H_2O_2$, $OH^•$.
    • ROS overwhelm antioxidant defenses → oxidative stress.
    • Effects:
      • Lipid peroxidation (membrane damage).
      • Enzyme inactivation.
      • ↓ Surfactant (pulmonary toxicity) → atelectasis.

Oxygen Toxicity - Signs & Symptoms Spotlight

  • CNS Toxicity (Paul Bert Effect): Acute, occurs at >2-3 ATA $O_2$.
    • Symptoms: 📌 CONVENTID
      • Convulsions
      • Visual disturbances (tunnel vision)
      • Ear (tinnitus)
      • Nausea
      • Twitching (esp. facial, lips)
      • Irritability/Anxiety
      • Dizziness/Vertigo
    • Prodromal symptoms (e.g., anxiety, twitching, nausea) often precede seizures.
  • Pulmonary Toxicity (Lorrain Smith Effect): Chronic, with prolonged exposure to >0.5 ATA $O_2$ (typically >24-48 hours).
    • Early: Substernal discomfort/pain, dry cough, dyspnea on exertion.
    • Progressive: Dyspnea at rest, ↓ vital capacity, tracheobronchitis.
    • Late: ARDS-like picture, pulmonary edema, fibrosis.

⭐ The 📌 CONVENTID mnemonic (Convulsions, Visual changes, Ear ringing, Nausea, Twitching, Irritability, Dizziness) is key for recalling CNS oxygen toxicity symptoms, which often precede seizures.

Oxygen Toxicity - Danger Zones & Defenses

  • Risk Factors: High inspired $P_{O_2}$, ↑exposure duration, $CO_2$ retention, exercise, fever, hyperthyroidism, individual susceptibility.
  • Prevention:
    • Limit $P_{O_2}$ & duration (e.g., Oxygen Tolerance Units - OTU, UPTD).
    • Use 'air breaks' during hyperbaric oxygen therapy (HBOT) and prolonged normobaric hyperoxia.
    • Antioxidants (experimental).
  • Management Overview:

⭐ Intermittent 'air breaks' (breathing normal air for 5-10 minutes every 20-30 minutes) significantly reduce risk of CNS & pulmonary oxygen toxicity during HBOT or prolonged high inspired oxygen fraction.

High‑Yield Points - ⚡ Biggest Takeaways

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