| Indication |
For the treatment of depression. |
| Pharmacodynamics |
Nefazodone, an antidepressant synthetically derived
phenylpiperazine, is used to treat major depression. Although it is
structurally similar to trazodone, nefazodone has a mechanism of action
different from other antidepressants and, hence, lacks the risk for
major cardiovascular toxicity seen with tricyclics and insomnia and
inhibition of REM sleep seen with the selective serotonin reuptake
inhibitors. |
| Mechanism of action |
Within the serotonergic system, nefazodone acts as an antagonist at type 2 serotonin (5-HT2)
post-synaptic receptors and, like fluoxetine-type antidepressants,
inhibits pre-synaptic serotonin (5-HT) reuptake. These mechanisms
increase the amount of serotonin available to interact with 5-HT
receptors. Within the noradrenergic system, nefazodone inhibits
norepinephrine uptake minimally. Nefazodone also antagonizes
alpha(1)-adrenergic receptors, producing sedation, muscle relaxation,
and a variety of cardiovascular effects. Nefazodone's affinity for
benzodiazepine, cholinergic, dopaminergic, histaminic, and beta or
alpha(2)-adrenergic receptors is not significant. |
| Absorption |
Nefazodone is rapidly and completely absorbed. Its absolute bioavailability is low (about 20%). |
| Volume of distribution |
|
| Protein binding |
Greater than 99% (in vitro, human plasma proteins). |
| Metabolism |
Hepatic. |
| Route of elimination |
Nefazodone is extensively metabolized after oral administration by
n-dealkylation and aliphatic and aromatic hydroxylation, and less than
1% of administered nefazodone is excreted unchanged in urine. |
| Half life |
2-4 hours |
| Clearance |
Not Available |
| Toxicity |
Cases of life-threatening hepatic failure have been reported in patients treated
with nefazodone. |
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