| Structure/Class |
- Monovalent cation
|
| Pharmacodynamics |
- Functions by inhibiting IP3 and GSK-3, which is a multifunctional protein kinase.
- Overall acts to reduce α-adrenergic and muscarinic transmission.
- Also inhibits adenylyl cyclase and second messenger systems, therefore causing hypothyroidism and Nephrogenic DI.
|
| Absorption/administration |
- PO
- Absorption is virtually complete in 6-8 hours.
|
| Distribution |
- Initially distributed in TBW, with Vd ~0.5L/kg, rising to 0.7 to 0.9L/kg.
- No protein binding, but some sequestration in bone.
|
| Metabolism |
- Nil
|
| Excretion |
- Virtually entirely in urine. Clearance is ~20% of creatinine clearance.
- Long T ½ – about 20 hours.
|
| Indications |
- Bipolar affective disorder (especially manic phase)
- Depressive disorders
- Schizophrenia
|
| Contraindications |
|
| Special precautions |
- Pregnancy – renal clearance increases during pregnancy and clearance decreases post-partum.
|
| Interactions |
- Thiazide diuretics reduce clearance of lithium by 25%.
- Clearance also reduced by NSAIDs.
- Use of anti-psychotics may produce more severe extrapyramidal symptoms with lithium.
|
| Adverse events |
- Neurological
- Very common. Tremor, ataxia and dysarthria are common. May also cause new psychiatric disturbances (mental confusion)
- Endocrinology
- Renal
- Nephrogenic DI à causes polyuria and polydipsia
- Cardiac
- Depresses SA node (CI in SSS and tachy-brady syndrome)
- Pregnancy and post-partum
- Lithium causes Ebstein’s anomaly
- May also cross breast milk – results in lethargy, poor suck and poor reflexes.
- Idiosyncratic
|
| Dosing/administration |
|
| Toxicology |
- Therapeutic ODs are more common than intentional/accidental OD, due to changes in the patient’s status (that is ,decreased serum Na, increased diuretic use or fluctuating renal function)
- Treatment is dialysis or supportive care.
|
| Withdrawal syndrome |
|
| Special notes |
|
