Role of ketamine in treatment-resistant depression
Joanna Dmochowska, Marcin Ciechański, Joanna Cieszkowska, Julia Czerwik, Marta Czubala, Patrycja Felisiak, Wiktor Gąska, Karol Kanon, Edyta Witkowska
Journal of Education Health and Sport April 5, 2025 Peer reviewed DOI: 10.12775/jehs.2025.80.58492 via OpenAlex
Summary
Ketamine has shown rapid antidepressant effects in treating treatment-resistant depression (TRD), reducing depressive symptoms and suicidal thoughts within hours, unlike traditional antidepressants that take weeks. It works by modulating the glutamatergic system and enhancing synaptic plasticity. However, its potential for addiction and side effects like dissociative symptoms necessitate careful monitoring. Variations in administration route and patient age also affect its efficacy.
Study at a glance
| Population | patients with treatment-resistant depression |
|---|---|
| Key finding | Ketamine is effective in reducing depressive symptoms and suicidal ideation within hours in patients with treatment-resistant depression. |
Abstract
Introduction: Depression, affecting 350 million people globally, is a leading cause of disability. Common symptoms include low mood, sadness, guilt, anxiety, and suicidalthoughts. Current treatments, mostly monoamine-based antidepressants, have limitations such as delayed effects and low efficacy, with over 60% of patients not achieving lasting remission. Ketamine, an NMDA antagonist, has shown rapid antidepressant effects, and research suggests glutamatergic dysfunction plays a role in TRD, highlighting the need for faster, more effective treatments. Current state of knowledge: Ketamine, an NMDA receptor antagonist, has gained attention for its rapid antidepressant effects, particularly in treatment-resistant depression. It works by modulating the glutamatergic system, enhancing synaptic plasticity, and involving other systems like GABA and 5-HT. Clinical trials have shown ketamine's efficacy in reducing depressive symptoms and suicidal ideation within hours, contrasting with traditional antidepressants that take weeks. The intravenous route is most effective, with lower bioavailability in other forms. While ketamine shows promise, its potential for addiction and side effects necessitate careful monitoring. Conclusion: Evidence supports ketamine for treating refractory depression, enhancing neuroplasticity and regulating affective symptoms through anti-inflammatory effects. Variations exist in administration route, bioavailability, and patient age. Common adverse effects include dissociative symptoms and cardiovascular issues, requiring careful monitoring and management.