Table 1.
Main classes of antidepressants with their date of approval, contributions, and disadvantages
|
Product
|
Date of FDA1 approval
|
Contributions
|
Disadvantages
|
|
| MAOI 2 | Iproniazid | 1958 | Confirmed the role of monoaminergic transmission in depression | Drug interactions, dietary restrictions |
| Led to a new search methodologies to develop new antidepressants | Hepatotoxicity and hypertensive crises | |||
| TC 3 | Imipramine | 1959 | Efficacy in patients with more severe symptoms of MDD | Cardiovascular toxicity and anticholinergic side effects. Risk of lethal toxicity from overdoses |
| Desipramine | ||||
| Nortriptyline | 1992 | |||
| Amitriptyline | 1961 | |||
| Clomipramine | Not approved | |||
| First tetracyclicmaprotiline | ||||
| SSRI 4 | Fluoxetine | 1987 | Improved tolerability | Several minor side effects (sexual dysfunction, loss of appetite, vomiting, nausea, irritability, anxiety, insomnia, and headache). Paroxetine had the highest rate of sexual dysfunction. Fluvoxamine is associated with the most overall adverse events |
| Citalopram | 1998 | |||
| Fluvoxamine | 2007 | |||
| Paroxetine | 1992 | |||
| Escitalopram | 2002 | |||
| Sertraline | 1999 | |||
| SNRI 5 | Venlafaxine | 2008 | Commonly recommended for patients who do not respond to SSRIs | No improvement in efficacy. Lower tolerability (highest rates of nausea, vomiting, and sexual dysfunction) |
| Duloxetine | 2004 | |||
| Reboxetine | Not approved | |||
| Other antidepressants | Trazodone | 1981 | Comparable efficacy to SSRIs | High rate of somnolence |
| Nefazodone | 2003 | Rare but fatal hepatotoxicity | ||
| Bupropion | 2003 | A better tolerability profile (minimal weight gain or even weight loss). Likely to improve symptoms of fatigue and sleepiness | May increase risk for seizures (low evidence) | |
| Vortioxetine | 2013 | Efficacy in elderly patients. Supposed cognitive-enhancing properties. Safety profile is similar to SSRIs | The most commonly reported adverse effect was nausea | |
| Vilazodone | 2011 | Less sexual dysfunction (low evidence). Safety profile is similar to SSRIs | The most commonly reported adverse effects were diarrhea and nausea | |
| Mirtazapine | 1997 | Comparable efficacy to SSRIs. Low risk of sexual dysfunction | Weight gain | |
| Ketamine and related drugs | Ketamine | Not approved | Rapid effects on resistant depression and acute suicidal ideation | Short antidepressant effect. Possible neurotoxicity and drug dependence |
| Esketamine | 2019 | Treatment-resistant depression. Greater affinity for NMDA receptor than ketamine | Potential risk of abuse. Lack of hindsight | |
1
United States Food and Drug Administration.
2
Monoamine oxidase inhibitors.
3
Tricyclic antidepressant.
4
Selective serotonin reuptake inhibitors.
5
Serotonin-norepinephrine reuptake inhibitors.
NMDA: N-methyl-D-aspartate; SSRI: DSelective serotonin reuptake inhibitors; MDD: Major depressive disorder; MAOI: Monoamine oxidase inhibitor.