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– THERAPEUTIC TARGETS & MANAGEMENT:
Primary pharmacological intervention aims to restore physiological homeostatic balance. This is achieved by either competitively blocking receptor sites, allosterically inhibiting enzymes, or supplementing missing metabolic products.
â– GERIATRIC PHYSIOLOGIC ADJUSTMENTS:
Older patients display reduced physiological reserves, altered muscle-to-fat distributions, and distinct renal filtration profiles.
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🌟 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. Absolute contraindications include pregnancy, renal insufficiency, or concurrent use of metabolic inhibitors. Always adjust therapeutic doses based on age-related glomerular filtration clearance.