â– LECTURE OVERVIEW: Delirium Tremens (DTs) is the most severe and life-threatening manifestation of the alcohol withdrawal syndrome.
â– HYPEREXCITABLE NEURAL MECHANISMS:
1. Chronic GABA Drive: Chronic alcohol use continuously stimulates inhibitory GABA-A receptors, prompting down-regulation of these receptors, and continually blocks excitatory NMDA glutamate receptors, prompting up-regulation of NMDA receptors.
2. Abrupt Cessation: When alcohol is abruptly discontinued, the sudden loss of inhibitory GABA stimulation paired with an unregulated glutamatergic drive causes severe, systemic central nervous system hyperexcitability.
3. Autonomic Storm: Drives a severe sympathetic storm, characterized by extreme hypertension, hyperthermia, tachycardic arrhythmias, and psychomotor agitation.
â– ETIOLOGICAL PROFILE & RISK FACTORS:
Major etiological drivers include genetic predispositions (autosomal patterns and chromosomal translocations) and environmental triggers like toxic chemical exposure, mechanical stress, or chronic viral infections.
â– ACUTE TOXICOLOGICAL PROFILE:
High cumulative chemical exposure or accidental overdose triggers systemic receptor overload, cellular injury, and metabolic acidosis.
[HY-BOARD-1163]
🌟 Dynamic Clinical Key:
DTs typically begins 48-96 hours after the last drink, presenting with altered sensorium, disorientation, and vivid visual/tactile hallucinations (e.g., crawling insects). First-line treatment is aggressive intravenous Benzodiazepines (e.g., Diazepam, Lorazepam) to restore GABAergic inhibition and prevent status epilepticus. Assess family history and genetic screens to identify high-risk patients before symptoms present. Immediate administration of physiological charcoal or specific receptor antagonists is lifesaving.