Antidepressants

Selective Serotonin Reuptake Inhibitors (SSRIs)

Cause discontinuation symptoms† if stopped abruptly (less likely with fluoxetine)Cause discontinuation symptoms† if stopped abruptly (less likely with fluoxetine)

CitalopramCitalopram

Lower potential for drug interactions because it has less effect on CYP450 isoenzymes

Risk of QT-interval prolongation that limits doses to ≤ 40 mg/day

EscitalopramEscitalopram

Lower potential for drug interactions because it has less effect on CYP450 isoenzymes

FluoxetineFluoxetine

Has very long half-life

Less likely to cause discontinuation symptoms†

The only antidepressant proven effective in children

FluvoxamineFluvoxamine

Can cause clinically significant elevation of theophylline, warfarin, and clozapine blood levelsCan cause clinically significant elevation of theophylline, warfarin, and clozapine blood levels

Has potential for interactions between its active metabolites and HCAs, carbamazepine, antipsychotics, or type 1C antiarrhythmicsHas potential for interactions between its active metabolites and HCAs, carbamazepine, antipsychotics, or type 1C antiarrhythmics

Has CYP450 profile similar to fluoxetineHas CYP450 profile similar to fluoxetine

ParoxetineParoxetine

Has potential for interactions between its active metabolites and HCAs, carbamazepine, antipsychotics, or type 1C antiarrhythmicsHas potential for interactions between its active metabolites and HCAs, carbamazepine, antipsychotics, or type 1C antiarrhythmics

Has CYP450 profile similar to fluoxetineHas CYP450 profile similar to fluoxetine

Of SSRIs, may cause the most weight gain

SertralineSertraline

Of SSRIs, has highest incidence of loose stools

VilazodoneVilazodone

May increase risk of bleeding if taken with aspirin, other NSAIDs, or other drugs that affect coagulationMay increase risk of bleeding if taken with aspirin, other NSAIDs, or other drugs that affect coagulation

Should not be stopped abruptly; reduce dose gradually

Serotonin modulators (5-HT₂ blockers)

Cause discontinuation symptoms† if stopped abruptly

MirtazapineMirtazapine

Causes weight gain and sedation

Has fewer sexual adverse effects than SSRIs and SNRIs

TrazodoneTrazodone

May cause priapism and sedation

May cause orthostatic hypotension

Serotonin-norepinephrine reuptake inhibitors (SNRIs)

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DesvenlafaxineDesvenlafaxine

May increase BP or HR (control BP before initiating the medication and monitor BP and HR while patients are on it)

DuloxetineDuloxetine

Modest dose-dependent increase in systolic and diastolic BP

May cause mild urinary hesitancy in males

Less potential for drug interactions because it has less effect on CYP450 isoenzymes

LevomilnacipranLevomilnacipran

May increase BP or HR (control BP before initiating the medication and monitor BP and HR while patients are on it)

May increase risk of bleeding if it is taken with aspirin, other NSAIDs, or anticoagulantsMay increase risk of bleeding if it is taken with aspirin, other NSAIDs, or anticoagulants

Can affect urinary hesitation or retention (caution required in patients with obstructive urinary disorders; stop it if symptoms develop)

VenlafaxineVenlafaxine

Modest dose-dependent increase in diastolic BP

Dual norepinephrine and 5-HT reuptake effect at about 150 mg

Rarely, increase in systolic BP (not dose-dependent)

If stopped, should be tapered slowly

Less potential for drug interactions because it has less effect on CYP450 isoenzymes

VortioxetineVortioxetine

May increase risk of bleeding if taken with aspirin, other NSAIDs, or other medications that affect coagulation or bleedingMay increase risk of bleeding if taken with aspirin, other NSAIDs, or other medications that affect coagulation or bleeding

Norepinephrine-dopamine reuptake inhibitor

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BupropionBupropion

Contraindicated in patients who have bulimia or who are seizure-prone

May interact with HCAs, increasing the risk of seizures

May cause dose-dependent recent memory loss

Heterocyclics

Contraindicated in patients with coronary artery disease, certain arrhythmias, angle-closure glaucoma, benign prostatic hyperplasia, or esophageal hiatus hernia

Can cause orthostatic hypotension leading to falls and fractures, potentiate the effect of alcohol, and raise the blood level of antipsychotics

Cause discontinuation symptoms† if stopped abruptly

With significant overdose, potentially lethal

AmitriptylineAmitriptyline

Causes weight gain

AmoxapineAmoxapine

Can have extrapyramidal adverse effects

ClomipramineClomipramine

Lowers seizure threshold at doses of > 250 mg/day

DesipramineDesipramine

Metabolized only via CYP2D6 isoenzyme: Medications that inhibit this enzyme markedly increase plasma levels

DoxepinDoxepin

Causes weight gain

ImipramineImipramine

May cause excessive sweating and nightmares

MaprotilineMaprotiline

Increased risk of seizures with rapid dose escalation at high doses

NortriptylineNortriptyline

Has long half-life (74 hours)

ProtriptylineProtriptyline

Has long half-life (74 hours)

TrimipramineTrimipramine

Causes weight gain

Monoamine Oxidase (MAO) Inhibitors

Serotonin syndrome possible when taken with an SSRI

Hypertensive crisis possible when taken with other antidepressants, sympathomimetic or other selected medications, or certain foods and beverages

With significant overdose, potentially lethal

IsocarboxazidIsocarboxazid

Causes orthostatic hypotension

PhenelzinePhenelzine

Causes orthostatic hypotension

Selegiline, transdermalSelegiline, transdermal

Can cause application site reactions and insomnia

TranylcypromineTranylcypromine

Causes orthostatic hypotension

Has amphetamine-type stimulant effects and modest abuse potentialHas amphetamine-type stimulant effects and modest abuse potential

Melatonergic antidepressant

Agomelatine (5-HT_2C receptor antagonist)

Should be stopped immediately if symptoms or signs of potential liver injury develop or if serum aminotransferases increase to> 3 times the upper limit of normal