â– LECTURE OVERVIEW: Lithium carbonate is a highly effective mood stabilizer utilized for bipolar disorder, but it carries a narrow therapeutic index.
â– PHARMACOLOGICAL KINETICS & RENAL FILTERS:
1. Narrow Window: The safe therapeutic index for lithium is narrow: 0.6 to 1.2 mEq/L, with toxic manifestations developing above 1.5 mEq/L.
2. Renal Clearance: Lithium is not metabolized; it is excreted 100% unchanged by the kidneys, handled similarly to sodium.
3. Proximal tubule reabsorption: It is freely filtered by the glomerulus, and approximately 80% is reabsorbed in the proximal convoluted tubule (PCT) alongside sodium.
4. Toxicity Triggers: Any state that reduces glomerular filtration rate or increases proximal sodium and water reabsorption will cause a dangerous accumulation of serum lithium, precipitating toxic levels.
â– PHARMACOKINETIC & PHARMACODYNAMIC ATTRIBUTES:
Absorption and steady-state kinetics display high variability based on plasma protein binding levels, tissue volume of distribution (Vd), and hepatic CYP450 microsomal enzymatic clearance indices.
â– SURGICAL COMPASS & ANATOMICAL CORRELATION:
Dissection lines must respect established fascial boundaries to prevent neurovascular traction injuries and secure excellent diagnostic margins.
[HY-BOARD-1192]
🌟 Dynamic Clinical Key:
Toxicity triggers include dehydration, low-sodium diets, and three classic drug classes: NSAIDs (which block renal prostaglandins to restrict GFR), Thiazide Diuretics (which deplete sodium, driving compensatory PCT reabsorption), and ACE Inhibitors/ARBs. Toxicity presents with severe coarse tremors, ataxia, vomiting, and confusion. Closely monitor serum plasma concentrations if drugs display a narrow therapeutic window to mitigate toxic peaks. Verify landmarks dynamically with gentle palpation and specialized intraoperative markers.