Drug Txs:
1. Lithium
Narrow therapeutic range and renal toxicity therefore ❌ needed, range 0.6 - 0.75 mmol/L. Wide variation in dose required, initially ❌ daily od or bd. 80% reduced risk of ❌, possibly by decreasing impulsive-aggressive behavior. Possible MoAs: modulates ❌ proteins, affects ❌ transduction via inhibition of ❌, interferes with ❌ signal transduction cascades.
2. Valproic acid
Effective for the ❌ phase of bipolar disorder and may prevent recurrence. Not an established treatment for preventing depression but effective for some. MoA: interferes with voltage-sensitive ❌ channels by increasing inhibitory actions of ❌ and regulating downstream signal transduction cascades. Also interacts with other ion channels e.g. voltage sensitive ❌ channels, and indirectly blocks ❌.
2. Carbamazepine
Very good for acute ❌ and maintenance treatment, but is a potent ❌ inducer so generally 2nd/3rd line. MoA: Binds to ❌ subunit of voltage-sensitive sodium channels and perhaps has additional effects at calcium and potassium ion channels, to enhance the ❌ effects GABA.
3. Lamotrigine
Useful for bipolar ❌ but unlicensed - increasingly popular. Similar effects to carbamazepine on sodium channels, blocks the α subunit. Also ❌ glutamate release, which is unique. Comparatively ❌ tolerated, excluding the
propensity to cause ❌ – minimize by ❌ dose increases.
4. Atypical antipsychotics
For mania:
Established for psychotic and nonpsychotic mania. In particular, ❌. Antagonism or partial agonism of ❌, and antagonism of ❌ receptors indirectly reduces ❌, may be MoA.
For depression:
Effects ❌ receptors - indirectly disinhibits ❌ theoretically improving mood and cognition. Mood improved by blocking NA and 5-HT reuptake.
Adjunctive treatment options - ❌ for agitation; topiramate or zonisamide for weight
loss; and ❌ for anxiety, sleep, or pain
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