Norketotifen

Norketotifen is a pharmaceutical medication which is not yet approved for use and is undergoing clinical trials. It is a biologically active demethylated metabolite of ketotifen and has a similar potency as ketotifen as an antihistamine H₁ medication and a mast cell stabilizer, yet is devoid of severe sedative effects of ketotifen, potentially allowing for higher doses to be administered without sedation as a limiting factor.^[1] Norketotifen is researched for its potential anti-inflammatory activity caused by dose-dependent inhibition of the release of the pro-inflammatory cytokine TNF-α,^[1] and for its other potential properties.^[2]

Norketotifen

Identifiers
CAS Number	34580-20-6
3D model (JSmol)	Interactive image
PubChem CID	9904236
SMILES C1CNCCC1=C2C3=C(C(=O)CC4=CC=CC=C42)SC=C3
Properties
Chemical formula	C18H17NOS
Molar mass	295.4
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa). Infobox references

Pharmaceutical properties

A prodrug of norketotifen is ketotifen which was patented in 1970 by Sandoz Pharmaceuticals (currently a part of Novartis), a Swiss company,^[3][4][5] and came into medical use in 1976.^[5] Ketotifen can be considered a sedating prodrug that is converted to norketotifen, a nonsedating metabolite with anti-inflammatory properties, when used as an anti-inflammatory medication.^[5]

Research directions

Influenza

The potential future applications of norketotifen, including a treatment for non-complicated influenza are researched by Emergo Therapeutics, a US company.^{[6][7][8][9][10]}

Malaria

Norketotifen, the de-methylated metabolite of ketotifen, has shown promising potential as an antimalarial drug, but the research is in the very early stage.^[2] Norketotifen has been found to be a more potent antimalarial in vitro compared to ketotifen, and it exhibited equivalent activity in vivo against asexual blood and developing liver-stage parasites.^[2] After ketotifen dosing, norketotifen levels were much higher than ketotifen relative to the IC50s of the compounds against Plasmodium falciparum in vitro.^[2] This suggests that the antimalarial activity of ketotifen in mice is mediated through norketotifen.^[2] Given these findings, future research could focus on further understanding the pharmacokinetics and metabolism of norketotifen, as well as its mechanism of action against Plasmodium falciparum.^[2] It would also be beneficial to investigate the drug's efficacy against other strains of Plasmodium and in different animal models.^[2] If norketotifen continues to show promising results in future studies, it could potentially be developed into a new antimalarial drug. This could be particularly valuable given the increasing resistance of malaria parasites to existing drugs.^[2]

Sedation

Both ketotifen and its active metabolite norketotifen exist as optically active atropisomers. They both have antihistaminic and anti-inflammatory properties. However, the S-atropisomer of norketotifen (SN) causes less sedation than ketotifen and the R-atropisomer of norketotifen (RN) in rodents. The lower sedative effect of SN in rodents is probably due to a combination of a lower uptake of norketotifen than ketotifen into the brain and less affinity of SN for histamine H₁ receptors in the central nervous system. This research direction could potentially lead to the development of antihistamines with reduced sedative effects.^[11]

References

1. Aberg AK, Arulnesan N, Bolger GT, Ciofalo VB, Pucaj K, Walle K, et al. (April 2022). "Ketotifen is a Prodrug. Norketotifen is the active metabolite". Drug Development Research. 83 (2): 362–367. doi:10.1002/ddr.21865. PMID 34410005. S2CID 237216445.
2. Milner E, Sousa J, Pybus B, Auschwitz J, Caridha D, Gardner S, et al. (March 2012). "Ketotifen is an antimalarial prodrug of norketotifen with blood schizonticidal and liver-stage efficacy". Eur J Drug Metab Pharmacokinet. 37 (1): 17–22. doi:10.1007/s13318-012-0080-2. PMID 22314893.
3. "Ketotifen". Drugbank. April 12, 2024. Archived from the original on August 6, 2019. Retrieved November 16, 2023.
4. "Ketotifen Fumarate". Inxight Drugs. Bethesda MD, US: National Center for Advancing Translational Sciences (NCATS). April 12, 2024. Archived from the original on April 13, 2024. Retrieved April 13, 2024.
5. MacDonald G (1982). "An Overview of Ketotifen". Chest. 82 (1 Suppl): 30s–32s. doi:10.1378/chest.82.1.30S. PMID 6806019. Archived from the original on April 13, 2024. Retrieved April 13, 2024.
6. "A Phase 2b Double-blind, Randomized, Placebo-controlled, Parallel-group Study of the Efficacy and Safety of Norketotifen (NKT) in the Treatment of Acute Uncomplicated Influenza-like Illness (ILI)". January 25, 2023. Archived from the original on April 13, 2024. Retrieved April 13, 2024.
7. "Efficacy and Safety of Norketotifen in Uncomplicated Influenza-like Illness: Influenza Clinical". January 30, 2023. Archived from the original on April 13, 2024. Retrieved April 13, 2024.
8. "Efficacy and Safety of Norketotifen in Uncomplicated Influenza-like Illness". January 25, 2023. Archived from the original on April 20, 2024. Retrieved April 13, 2024.
9. "Emergo finds midstage success in developing flu-fighter norketotifen + | Bioworld | BioWorld". Archived from the original on April 13, 2024. Retrieved April 13, 2024.
10. "Norketotifen in Influenza -Like Illness - Clinical Trials Registry - ICH GCP". Archived from the original on April 13, 2024. Retrieved April 13, 2024.
11. Feng F, Fawcett JP, Zhang H, Tucker IG (April 2020). "Cell-based, animal and H1 receptor binding studies relative to the sedative effects of ketotifen and norketotifen atropisomers". J Pharm Pharmacol. 72 (4): 507–518. doi:10.1111/jphp.13220. PMID 32030755.

External links

 

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