Amoxapine is FDA approved drug belonging to the class of second-generation tricyclic dibenzoxazepine antidepressants.[1][2] It is generally reserved for second or third-line treatment after selective serotonin reuptake inhibitors (SSRIs) or serotonin-norepinephrine reuptake inhibitors (SNRI) have failed to control the depression.[1] Thus, it is indicated for treatment-resistant depression, after the first and second-line medication has failed to improve symptoms.

Indications for this medication also include use in cases of depression with other psychiatric issues, such as anxiety, agitation, psychosis as well as neurotic or recurrent depression.[2] Amoxapine may either be taken as a single oral tablet daily or divided into two daily doses.[3] Research (in mice) has revealed that amoxapine also decreases the production of amyloid-beta chains in Alzheimer disease by acting of the serotonin-6 (HTR-6, 5-HT-6) receptor.[4] In various studies, amoxapine also reduced the incidence of diarrhea in patients undergoing chemotherapy, specifically with irinotecan.[5][6] Additionally, research showed this drug to improve the prognosis of neuropathic pain.[7]

Amoxapine is a second-generation tricyclic dibenzoxazepine antidepressant; therefore, it works primarily by inhibiting the reuptake of norephedrine in the neuronal synapses.[2][8][9] It appears to have the minimal effect of serotonin receptors, asides from the serotonin-6 receptor (HTR-6, 5-HT-6).[2][4] Amoxapine has a minimal impact on the histamine H1 receptor.[10]

Amoxapine is primarily metabolized into two active metabolites by the liver through aromatic hydroxylation. The active metabolites are 7-hydroxyamoxapine and 8-hydroxyamoxapine, which reduce the incidence of diarrhea in patients after the administration of irinotecan chemotherapy.[2][6] The research revealed that these metabolites decreased tumor growth in such individuals.[6] The half-life of the active metabolite, 8-hydroxyamoxapine, is found to be 30 hours, while the half-life of the drug itself is 8 hours.[2] The primary method of excretion of the drug from the body is through the urine, with a small portion eliminated in the feces.[2]

Amoxapine is administered orally, starting at 100 mg, with the potential to titrate the dosage up to 300 mg.[11][12][13][2] The drug can be administered as one dose daily or divided into two tablets daily.[3] However, due to the long half-life of the active metabolites of the drug, it was found to be more beneficial to have one single dose compared to two divided doses.[11] The antidepressant effects of amoxapine are observable in as little as seven days.[8]

The most common side effects of amoxapine therapy include, but are not limited to, insomnia, palpitations, tachycardia, hypotension, and constipation.[14][15][2] Researchers found that amoxapine induces hypomanic states in patients with underlying bipolar disorder.[14] Amoxapine also induces noradrenaline contraction of the urethra in guinea pigs and rats in various laboratory studies, resulting in increased urethral resistance.[16][17] The drug also correlated with some incidences of painful ejaculations, relieved by the administration of tamsulosin.[18] Furthermore, tricyclic antidepressants, such as amoxapine, are associated with an increased risk of seizures in patients with epilepsy and the elderly population.[19][20] it is recommended to use selective serotonin reuptake inhibitors (SSRIs) or serotonin-norepinephrine reuptake inhibitors (SNRIs) in patients with a history of epilepsy and seizures.

Also, since amoxapine imparts, although minimal, effects on the histamine H1 receptor, antihistamine side effects must be taken into account, especially in the elderly population consisting of patients above the age of 65. These effects include sedation, insomnia, dry mouth, delirium, and Parkinsonism symptoms.[21] It was also found, in a few patient cases, to prolong the QTc interval.[22]

The primary mechanism of action of amoxapine is through inhibition of presynaptic reuptake of norepinephrine; patients should not take it alongside other antidepressant or drugs which impart similar effects, such as MAO inhibitors. Patients should not take the drug within 14 days of other antidepressants, allowing time for the previous antidepressant to leave the system entirely before initiating amoxapine, or any other TCA.

Furthermore, due to the QTc prolongation effect of the drug, patients with increased QTc intervals or acute myocardial infarction should not be prescribed this medication to avoid exacerbating their symptoms.[22] Tricyclic antidepressants are also contraindicated in patients with a history of epilepsy or seizures, and the recommendation is, instead, to utilize SSRIs or SNRIs in such patients, as research has shown it to slightly increase the risk of seizures.[20] Additionally, as the drug is metabolized in the liver, patients with liver disease should not be prescribed amoxapine.