Ketamine and the glutamatergic system: A systematic review of NMDA receptor modulation

Authors

  • Pedro Santos-Pimenta Associate Laboratory i4HB - Institute for Health and Bioeconomy, University Institute of Health Sciences - CESPU, Gandra, Portugal; UCIBIO - Applied Molecular Biosciences Unit, Translational Toxicology Research Laboratory, University Institute of Health Sciences (1H-TOXRUN, IUCS-CESPU), Gandra, Portugal
  • Rita Azevedo Associate Laboratory i4HB - Institute for Health and Bioeconomy, University Institute of Health Sciences - CESPU, Gandra, Portugal; UCIBIO - Applied Molecular Biosciences Unit, Translational Toxicology Research Laboratory, University Institute of Health Sciences (1H-TOXRUN, IUCS-CESPU), Gandra, Portugal; Associate Laboratory i4HB - Institute for Health and Bioeconomy, Faculty of Pharmacy, University of Porto, Porto, Portugal; UCIBIO - Applied Molecular Biosciences Unit, Laboratory of Toxicology, Faculty of Pharmacy, University of Porto, Porto, Portugal
  • Daniel José Barbosa Associate Laboratory i4HB - Institute for Health and Bioeconomy, University Institute of Health Sciences - CESPU, Gandra, Portugal; UCIBIO - Applied Molecular Biosciences Unit, Translational Toxicology Research Laboratory, University Institute of Health Sciences (1H-TOXRUN, IUCS-CESPU), Gandra, Portugal https://orcid.org/0000-0002-1726-6011

DOI:

https://doi.org/10.48797/sl.2026.484

Keywords:

Poster

Abstract

Background: Ketamine was first synthesized in 1962 by Calvin Stevens as an alternative to phencyclidine. Its effects stem primarily from glutamatergic modulation, particularly from the antagonism of N-methyl-D-aspartate receptors (NMDAR) [1]. Objective: This study aims to systematically review the pharmacodynamics of ketamine, with particular attention to its effects on the glutamatergic system. Methods: The bibliographic search was conducted using books and scientific databases (PubMed and ScienceDirect), using the following terms: “ketamine”, “NMDA receptors”, “ketamine pharmacology”. Only articles published in English from 2000 to 2025 were considered. A total of 7 articles were included. Results: Both enantiomers of ketamine, (S)-ketamine and (R)-ketamine, are noncompetitive antagonists of NMDARs; however, (S)-ketamine has an affinity/potency for NMDARs that is approximately four times greater [2]. In Xenopus oocytes expressing recombinant NMDAR GluN2A–D subunits, in the absence of Mg²⁺, ketamine shows a higher affinity for NMDARs-GluN2B subtype [3]. However, the affinity depends not only on the subunits that constitute the receptor but also on Mg²⁺ levels and affinity for the receptor [4]. D-serine acts as a coagonist of ketamine by binding to the glycineB site of NMDARs. In PC-12 cells, ketamine influences intra- and extraneuronal levels of D-serine: (S)-ketamine increases intraneuronal levels and reduces extraneuronal levels, while (R)-ketamine decreases both. Furthermore, studies in rats have demonstrated that ketamine modulates the transcription of the gene encoding for serine racemase (Srr), increasing Srr mRNA levels in the striatum, hippocampus and cortex, but decreasing them in the forebrain [5]. Conclusions: The glutamatergic system plays a major role in short-term memory retention and consolidation, as well as in cognition [6]. Interference with this system leads to decreased memory retention, cognitive impairment, and dissociation [1]. Ketamine exerts both direct and indirect effects on the glutamatergic system, which explains the characteristic effects of its use. These effects underlie its use in recreational contexts [1] and as a facilitator drug in sexual assaults [7].

References

1. Dinis-Oliveira, R.J. Metabolism and metabolomics of ketamine: a toxicological approach. Forensic Sci Res 2017, 2, 2-10. doi:10.1080/20961790.2017.1285219.

2. Zanos, P. et al. Mechanisms of ketamine action as an antidepressant. Mol Psychiatry 2018, 23, 801-811. doi:10.1038/mp.2017.255.

3. Dravid, S.M. et al. Subunit-specific mechanisms and proton sensitivity of NMDA receptor channel block. J Physiol 2007, 581, 107-128. doi:10.1113/jphysiol.2006.124958.

4. Kotermanski, S.E. et al. Mg2+ imparts NMDA receptor subtype selectivity to the Alzheimer's drug memantine. J Neurosci 2009, 29, 2774-2779. doi:10.1523/JNEUROSCI.3703-08.2009.

5. Watanabe, M. et al. Subchronic administration of ketamine decreases the mRNA expression of serine racemase in rat brain. Tokai J Exp Clin Med 2010, 35, 137-143.

6. Santos, S.D. Glutamato. In Neurociências; Rego, A.C., Duarte, C.B., Oliveira, C.R., Eds Lidel: Lisbon, Portugal, 2017, pp. 85–102.

7. Lynam, M. et al. The prevalence of selected licit and illicit drugs in drug facilitated sexual assaults. Forensic Sci Inter Synerg 2024, 9, 100545. doi:10.1016/j.fsisyn.2024.100545.

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Published

2026-05-05

How to Cite

Santos-Pimenta, P., Azevedo, R., & Barbosa, D. J. (2026). Ketamine and the glutamatergic system: A systematic review of NMDA receptor modulation. Scientific Letters, 1(Sup 1). https://doi.org/10.48797/sl.2026.484

Issue

Vol. 1 No. Sup 1 (2026)

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Copyright (c) 2026 Pedro Santos-Pimenta, Rita Azevedo, Daniel José Barbosa

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