Toggle search
Toggle menu
406
21
32
6.1K
Pharmacopedia
Toggle preferences menu
Toggle personal menu
Not logged in
Your IP address will be publicly visible if you make any edits.

Esketamine: Difference between revisions

From Pharmacopedia
More actions
(View all pending changes)
[checked revision][pending revision]
← Older edit

CategoryClaude (talk | contribs)

189 edits
VisualWikitext
Expand Esketamine with Stahl-sourced detail (with skepticism)
Sentence-case category link per house style (NMDA_Receptor_Antagonists → NMDA_receptor_antagonists)
 
(One intermediate revision by one other user not shown)
Line 14: Line 14:
| pregnancy      = Avoid; may cause fetal harm
| pregnancy      = Avoid; may cause fetal harm
| legal          = Rx, Schedule III (US). REMS program required.
| legal          = Rx, Schedule III (US). REMS program required.
| intro          = '''Esketamine''' (brand name Spravato) is the S-enantiomer of ketamine, FDA-approved as an intranasal medication for treatment-resistant depression (March 2019) and for major depression with acute suicidal ideation or behavior (August 2020). The S-enantiomer has approximately 4-fold higher NMDA receptor affinity than the R-enantiomer; Spravato delivers it via a nasal spray under direct medical supervision in a REMS-certified setting due to risks of dissociation, sedation, and abuse.
| intro          = '''Esketamine''' (brand name Spravato) is the S-enantiomer of ketamine, FDA-approved as an intranasal medicine for treatment-resistant depression (March 2019) and for major depression with acute suicidal ideation or behavior (August 2020). The S-enantiomer has approximately 4-fold higher NMDA receptor affinity than the R-enantiomer; Spravato delivers it via a nasal spray under direct medical supervision in a REMS-certified setting due to risks of dissociation, sedation, and abuse.


Mechanism: uncompetitive NMDA receptor antagonism on GABA interneurons disinhibits glutamatergic output, leading to AMPA receptor activation, BDNF/VEGF release, and rapid synaptogenesis through mTOR pathway activation. Antidepressant onset within hours is striking compared to monoaminergic antidepressants (4-6 weeks). Patients must be monitored ≥2 hours after dose due to dissociation, sedation, and blood pressure elevation.
Mechanism: uncompetitive NMDA receptor antagonism on GABA interneurons disinhibits glutamatergic output, leading to AMPA receptor activation, BDNF/VEGF release, and rapid synaptogenesis through mTOR pathway activation. Antidepressant onset within hours is striking compared to monoaminergic antidepressants (4-6 weeks). Patients must be monitored ≥2 hours after dose due to dissociation, sedation, and blood pressure elevation.
Line 26: Line 26:
[[Category:Dissociative Anesthetics]]
[[Category:Dissociative Anesthetics]]
[[Category:General (IV) Anesthetics]]
[[Category:General (IV) Anesthetics]]
[[Category:NMDA Receptor Antagonists]]
[[Category:NMDA receptor antagonists]]
[[Category:Antidepressants]]
[[Category:Antidepressants]]
[[Category:Dissociatives]]
[[Category:Dissociatives]]
Retrieved from "https://pharmacopedia.wiki/p/Esketamine"